Jump to content

Malaria

This is a good article. Click here for more information.
From Wikipedia, the free encyclopedia
(Redirected from Tertian fever)

Malaria
Malaria parasite connecting to a red blood cell
Pronunciation
SpecialtyInfectious disease
SymptomsFever, vomiting, headache, yellow skin[1]
Complicationsseizures, coma,[1] organ failure, anemia, cerebral malaria[2]
Usual onset10–15 days post exposure[3]
CausesPlasmodium transmitted to humans by Anopheles mosquitoes[1][4]
Diagnostic methodExamination of the blood, antigen detection tests[1]
PreventionMosquito nets, insect repellent, mosquito control, medications[1]
MedicationAntimalarial medication[3]
Frequency249 million (2022)[5]
Deaths608,000 (2022)[5]

Malaria is a mosquito-borne infectious disease that affects vertebrates and Anopheles mosquitoes.[6][7][3] Human malaria causes symptoms that typically include fever, fatigue, vomiting, and headaches.[1][8] In severe cases, it can cause jaundice, seizures, coma, or death.[1][9] Symptoms usually begin 10 to 15 days after being bitten by an infected Anopheles mosquito.[10][4] If not properly treated, people may have recurrences of the disease months later.[3] In those who have recently survived an infection, reinfection usually causes milder symptoms.[1] This partial resistance disappears over months to years if the person has no continuing exposure to malaria.[1] The mosquito vector is itself harmed by Plasmodium infections, causing reduced lifespan.[11]

Human malaria is caused by single-celled microorganisms of the Plasmodium group.[10] It is spread exclusively through bites of infected female Anopheles mosquitoes.[10][12] The mosquito bite introduces the parasites from the mosquito's saliva into a person's blood.[3] The parasites travel to the liver, where they mature and reproduce.[1] Five species of Plasmodium commonly infect humans.[10] The three species associated with more severe cases are P. falciparum (which is responsible for the vast majority of malaria deaths), P. vivax, and P. knowlesi (a simian malaria that spills over into thousands of people a year).[13][14] P. ovale and P. malariae generally cause a milder form of malaria.[1][10] Malaria is typically diagnosed by the microscopic examination of blood using blood films, or with antigen-based rapid diagnostic tests.[1] Methods that use the polymerase chain reaction to detect the parasite's DNA have been developed, but they are not widely used in areas where malaria is common, due to their cost and complexity.[15]

The risk of disease can be reduced by preventing mosquito bites through the use of mosquito nets and insect repellents or with mosquito-control measures such as spraying insecticides and draining standing water.[1] Several medications are available to prevent malaria for travellers in areas where the disease is common.[3] Occasional doses of the combination medication sulfadoxine/pyrimethamine are recommended in infants and after the first trimester of pregnancy in areas with high rates of malaria.[3] As of 2023, two malaria vaccines have been endorsed by the World Health Organization.[16] The recommended treatment for malaria is a combination of antimalarial medications that includes artemisinin.[17][18][1][3] The second medication may be either mefloquine, lumefantrine, or sulfadoxine/pyrimethamine.[19] Quinine, along with doxycycline, may be used if artemisinin is not available.[19] In areas where the disease is common, malaria should be confirmed if possible before treatment is started due to concerns of increasing drug resistance.[3] Resistance among the parasites has developed to several antimalarial medications; for example, chloroquine-resistant P. falciparum has spread to most malarial areas, and resistance to artemisinin has become a problem in some parts of Southeast Asia.[3]

The disease is widespread in the tropical and subtropical regions that exist in a broad band around the equator.[20][1] This includes much of sub-Saharan Africa, Asia, and Latin America.[3] In 2022, some 249 million cases of malaria worldwide resulted in an estimated 608,000 deaths, with 80 percent being five years old or less.[21] Around 95% of the cases and deaths occurred in sub-Saharan Africa. Rates of disease decreased from 2010 to 2014, but increased from 2015 to 2021.[18] According to UNICEF, nearly every minute, a child under five died of malaria in 2021,[22] and "many of these deaths are preventable and treatable".[23] Malaria is commonly associated with poverty and has a significant negative effect on economic development.[24][25] In Africa, it is estimated to result in losses of US$12 billion a year due to increased healthcare costs, lost ability to work, and adverse effects on tourism.[26]

Video summary (script)

Etymology

[edit]

The term malaria originates from Medieval Italian: mala aria 'bad air', a part of miasma theory; the disease was formerly called ague or marsh fever due to its association with swamps and marshland.[27] The term appeared in English at least as early as 1768.[28] Malaria was once common in most of Europe and North America,[29] where it is no longer endemic,[30] though imported cases do occur.[31]

Signs and symptoms

[edit]
Main symptoms of malaria[32]

Adults with malaria tend to experience chills and fever—classically in periodic intense bouts lasting around six hours, followed by a period of sweating and fever relief—as well as headache, fatigue, abdominal discomfort, and muscle pain.[33] Children tend to have more general symptoms: fever, cough, vomiting, and diarrhea.[33]

Initial manifestations of the disease—common to all malaria species—are similar to flu-like symptoms,[34] and can resemble other conditions such as sepsis, gastroenteritis, and viral diseases.[15] The presentation may include headache, fever, shivering, joint pain, vomiting, hemolytic anemia, jaundice, hemoglobin in the urine, retinal damage, and convulsions.[35]

The classic symptom of malaria is paroxysm—a cyclical occurrence of sudden coldness followed by shivering and then fever and sweating, occurring every two days (tertian fever) in P. vivax and P. ovale infections, and every three days (quartan fever) for P. malariae. P. falciparum infection can cause recurrent fever every 36–48 hours, or a less pronounced and almost continuous fever.[36]

Symptoms typically begin 10–15 days after the initial mosquito bite, but can occur as late as several months after infection with some P. vivax strains.[33] Travellers taking preventative malaria medications may develop symptoms once they stop taking the drugs.[33]

Severe malaria is usually caused by P. falciparum (often referred to as falciparum malaria). Symptoms of falciparum malaria arise 9–30 days after infection.[34] Individuals with cerebral malaria frequently exhibit neurological symptoms, including abnormal posturing, nystagmus, conjugate gaze palsy (failure of the eyes to turn together in the same direction), opisthotonus, seizures, or coma.[34]

Diagnosis based on skin odor profiles

Humans emanate a large range of smells. Studies have been conducted on how to detect human malaria infections through volatile compounds from the skin - suggesting that volatile biomarkers may be a reliable source for the detection of infection, including those asymptomatic. Using skin body odor profiles can be efficient in diagnosing global populations, and the screening and monitoring of infection to officially eradicate malaria. Research findings have predominantly relied on chemical explanations to explain the differences in attractiveness among humans based on distinct odor profiles. The existence of volatile compounds, like fatty acids, and lactic acid is an essential reason on why some individuals are more appealing to mosquitos than others.

Volatile compounds

Kanika Khanna, a postdoctoral scholar at the University of California, Berkeley studying the structural basis of membrane manipulation and cell-cell fusion by bacterial pathogens, discusses studies that determine how odor profiles can be used to diagnose the disease. Within the study, samples of volatile compounds from around 400 children within schools in Western Kenya were collected - to identify asymptomatic infections. These biomarkers have been established as a non-invasive way to detect malarial infections. In addition, these volatile compounds were heavily detected by mosquito antennae as an attractant, making the children more vulnerable to the bite of the mosquitos.[37]

Fatty acids

Fatty acids have been identified as an attractive compound for mosquitoes, they are typically found in volatile emissions from the skin. These fatty acids that produce body odor profiles originate from the metabolism of glycerol, lactic acid, amino acids, and lipids - through the action of bacteria found within the skin. They create a “chemical signature” for the mosquitoes to locate a potential host, humans in particular.[38]

Lactic acid

Lactic acid, a naturally produced levorotatory isomer, has been titled an attractant of mosquitoes for a long time. Lactic acid is predominantly produced by eccrine-sweat glands, creating a large amount of sweat on the surface of the skin. Due to the high levels of lactic acid released from the human body, it has been hypothesized to represent a specific human host-recognition cue for anthropophilic (attracted to humans) mosquitoes.

Pungent foot odor

Most studies use human odors as stimuli to attract host seeking mosquitoes and have reported a strong and significant attractive effect. The studies have found human odor samples very effective in attracting mosquitoes. Foot odors have been demonstrated to have the highest attractiveness to anthropophilic mosquitoes. Some of these studies have included traps that had been baited with nylon socks previously worn by human participants and were deemed efficient in catching adult mosquitos. Foot odors have high numbers of volatile compounds, which in turn elicit an olfactory response from mosquitoes.[38]

Complications

[edit]

Malaria has several serious complications, including the development of respiratory distress, which occurs in up to 25% of adults and 40% of children with severe P. falciparum malaria. Possible causes include respiratory compensation of metabolic acidosis, noncardiogenic pulmonary oedema, concomitant pneumonia, and severe anaemia. Although rare in young children with severe malaria, acute respiratory distress syndrome occurs in 5–25% of adults and up to 29% of pregnant women.[39] Coinfection of HIV with malaria increases mortality.[40] Kidney failure is a feature of blackwater fever, where haemoglobin from lysed red blood cells leaks into the urine.[34]

Infection with P. falciparum may result in cerebral malaria, a form of severe malaria that involves encephalopathy. It is associated with retinal whitening, which may be a useful clinical sign in distinguishing malaria from other causes of fever.[41] An enlarged spleen, enlarged liver or both of these, severe headache, low blood sugar, and haemoglobin in the urine with kidney failure may occur.[34] Complications may include spontaneous bleeding, coagulopathy, and shock.[42]

Malaria during pregnancy can cause stillbirths, infant mortality, miscarriage, and low birth weight,[43] particularly in P. falciparum infection, but also with P. vivax.[44]

Cause

[edit]
The life cycle of malaria parasites: Sporozoites are introduced by a mosquito bite. When they reach the liver, they multiply into thousands of merozoites. The merozoites infect red blood cells and replicate, infecting more and more red blood cells. Some parasites form gametocytes, which are taken up by a mosquito, continuing the life cycle.

Malaria is caused by infection with parasites in the genus Plasmodium.[45] In humans, malaria is caused by six Plasmodium species: P. falciparum, P. malariae, P. ovale curtisi, P. ovale wallikeri, P. vivax and P. knowlesi.[46] Among those infected, P. falciparum is the most common species identified (~75%) followed by P. vivax (~20%).[15] Although P. falciparum traditionally accounts for the majority of deaths,[47] recent evidence suggests that P. vivax malaria is associated with potentially life-threatening conditions about as often as with a diagnosis of P. falciparum infection.[48] P. vivax proportionally is more common outside Africa.[49] Some cases have been documented of human infections with several species of Plasmodium from higher apes, but except for P. knowlesi—a zoonotic species that causes malaria in macaques[50]—these are mostly of limited public health importance.[51]

The Anopheles mosquitos initially get infected by Plasmodium by taking a blood meal from a previously Plasmodium infected person or animal.[52][53] Parasites are then typically introduced by the bite of an infected Anopheles mosquito. Some of these inoculated parasites, called "sporozoites", probably remain in the skin,[54] but others travel in the bloodstream to the liver, where they invade hepatocytes.[55] They grow and divide in the liver for 2–10 days, with each infected hepatocyte eventually harboring up to 40,000 parasites.[55] The infected hepatocytes break down, releasing these invasive Plasmodium cells, called "merozoites", into the bloodstream. In the blood, the merozoites rapidly invade individual red blood cells, replicating over 24–72 hours to form 16–32 new merozoites.[55] The infected red blood cell lyses, and the new merozoites infect new red blood cells, resulting in a cycle that continuously amplifies the number of parasites in an infected person.[55] Over rounds of this infection cycle, a small portion of parasites do not replicate, but instead develop into early sexual stage parasites called male and female "gametocytes". These gametocytes develop in the bone marrow for 11 days, then return to the blood circulation to await uptake by the bite of another mosquito.[55] Once inside a mosquito, the gametocytes undergo sexual reproduction, and eventually form daughter sporozoites that migrate to the mosquito's salivary glands to be injected into a new host when the mosquito bites.[55]

The liver infection causes no symptoms; all symptoms of malaria result from the infection of red blood cells.[46] Symptoms develop once there are more than around 100,000 parasites per milliliter of blood.[46] Many of the symptoms associated with severe malaria are caused by the tendency of P. falciparum to bind to blood vessel walls, resulting in damage to the affected vessels and surrounding tissue. Parasites sequestered in the blood vessels of the lung contribute to respiratory failure. In the brain, they contribute to coma. In the placenta they contribute to low birthweight and preterm labor, and increase the risk of abortion and stillbirth.[46] The destruction of red blood cells during infection often results in anemia, exacerbated by reduced production of new red blood cells during infection.[46]

Only female mosquitoes feed on blood; male mosquitoes feed on plant nectar and do not transmit the disease. Females of the mosquito genus Anopheles prefer to feed at night. They usually start searching for a meal at dusk, and continue through the night until they succeed.[56] However, in Africa, due to the extensive use of bed nets, they began to bite earlier, before bed-net time.[57] Malaria parasites can also be transmitted by blood transfusions, although this is rare.[58]

Recurrent malaria

[edit]

Symptoms of malaria can recur after varying symptom-free periods. Depending upon the cause, recurrence can be classified as either recrudescence, relapse, or reinfection. Recrudescence is when symptoms return after a symptom-free period due to failure to remove blood-stage parasites by adequate treatment.[59] Relapse is when symptoms reappear after the parasites have been eliminated from the blood but have persisted as dormant hypnozoites[60] in liver cells. Relapse commonly occurs between 8 and 24 weeks after the initial symptoms and is often seen in P. vivax and P. ovale infections.[15] P. vivax malaria cases in temperate areas often involve overwintering by hypnozoites, with relapses beginning the year after the mosquito bite.[61] Reinfection means that parasites were eliminated from the entire body but new parasites were then introduced. Reinfection cannot readily be distinguished from relapse and recrudescence, although recurrence of infection within two weeks of treatment ending is typically attributed to treatment failure.[62] People may develop some immunity when exposed to frequent infections.[63]

Pathophysiology

[edit]
Micrograph of a placenta from a stillbirth due to maternal malaria. H&E stain. Red blood cells are anuclear; blue/black staining in bright red structures (red blood cells) indicate foreign nuclei from the parasites.
Electron micrograph of a Plasmodium falciparum-infected red blood cell (center), illustrating adhesion protein "knobs"

Malaria infection develops via two phases: one that involves the liver (exoerythrocytic phase), and one that involves red blood cells, or erythrocytes (erythrocytic phase). When an infected mosquito pierces a person's skin to take a blood meal, sporozoites in the mosquito's saliva enter the bloodstream and migrate to the liver where they infect hepatocytes, multiplying asexually and asymptomatically for a period of 8–30 days.[64]

After a potential dormant period in the liver, these organisms differentiate to yield thousands of merozoites, which, following rupture of their host cells, escape into the blood and infect red blood cells to begin the erythrocytic stage of the life cycle.[64] The parasite escapes from the liver undetected by wrapping itself in the cell membrane of the infected host liver cell.[65]

Within the red blood cells, the parasites multiply further, again asexually, periodically breaking out of their host cells to invade fresh red blood cells. Several such amplification cycles occur. Thus, classical descriptions of waves of fever arise from simultaneous waves of merozoites escaping and infecting red blood cells.[64]

Some P. vivax sporozoites do not immediately develop into exoerythrocytic-phase merozoites, but instead, produce hypnozoites that remain dormant for periods ranging from several months (7–10 months is typical) to several years.[61] After a period of dormancy, they reactivate and produce merozoites. Hypnozoites are responsible for long incubation and late relapses in P. vivax infections,[61] although their existence in P. ovale is uncertain.[66]

The parasite is relatively protected from attack by the body's immune system because for most of its human life cycle it resides within the liver and blood cells and is relatively invisible to immune surveillance. However, circulating infected blood cells are destroyed in the spleen. To avoid this fate, the P. falciparum parasite displays adhesive proteins on the surface of the infected blood cells, causing the blood cells to stick to the walls of small blood vessels, thereby sequestering the parasite from passage through the general circulation and the spleen.[67] The blockage of the microvasculature causes symptoms such as those in placental malaria.[68] Sequestered red blood cells can breach the blood–brain barrier and cause cerebral malaria.[69]

Genetic resistance

[edit]

Due to the high levels of mortality and morbidity caused by malaria—especially the P. falciparum species—it has placed the greatest selective pressure on the human genome in recent history. Several genetic factors provide some resistance to it including sickle cell trait, thalassaemia traits, glucose-6-phosphate dehydrogenase deficiency, and the absence of Duffy antigens on red blood cells.[70][71][72]

The impact of sickle cell trait on malaria immunity illustrates some evolutionary trade-offs that have occurred because of endemic malaria. Sickle cell trait causes a change in the haemoglobin molecule in the blood. Normally, red blood cells have a very flexible, biconcave shape that allows them to move through narrow capillaries; however, when the modified haemoglobin S molecules are exposed to low amounts of oxygen, or crowd together due to dehydration, they can stick together forming strands that cause the cell to distort into a curved sickle shape. In these strands, the molecule is not as effective in taking or releasing oxygen, and the cell is not flexible enough to circulate freely. In the early stages of malaria, the parasite can cause infected red cells to sickle, and so they are removed from circulation sooner. This reduces the frequency with which malaria parasites complete their life cycle in the cell. Individuals who are homozygous (with two copies of the abnormal haemoglobin beta allele) have sickle-cell anaemia, while those who are heterozygous (with one abnormal allele and one normal allele) experience resistance to malaria without severe anaemia. Although the shorter life expectancy for those with the homozygous condition would tend to disfavour the trait's survival, the trait is preserved in malaria-prone regions because of the benefits provided by the heterozygous form.[72][73]

Liver dysfunction

[edit]

Liver dysfunction as a result of malaria is uncommon and usually only occurs in those with another liver condition such as viral hepatitis or chronic liver disease. The syndrome is sometimes called malarial hepatitis.[74] While it has been considered a rare occurrence, malarial hepatopathy has seen an increase, particularly in Southeast Asia and India. Liver compromise in people with malaria correlates with a greater likelihood of complications and death.[74]

Effects on vaccine response

[edit]

Malaria infection affects the immune responses following vaccination for various diseases. For example, malaria suppresses immune responses to polysaccharide vaccines. A potential solution is to give curative treatment before vaccination in areas where malaria is present.[75]

Diagnosis

[edit]
The blood film is the gold standard for malaria diagnosis.
Ring-forms and gametocytes of Plasmodium falciparum in human blood

Due to the non-specific nature of malaria symptoms, diagnosis is typically suspected based on symptoms and travel history, then confirmed with a laboratory test to detect the presence of the parasite in the blood (parasitological test). In areas where malaria is common, the World Health Organization (WHO) recommends clinicians suspect malaria in any person who reports having fevers, or who has a current temperature above 37.5 °C without any other obvious cause.[76] Malaria should be suspected in children with signs of anemia: pale palms or a laboratory test showing hemoglobin levels below 8 grams per deciliter of blood.[76] In areas of the world with little to no malaria, the WHO recommends only testing people with possible exposure to malaria (typically travel to a malaria-endemic area) and unexplained fever.[76]

In sub-Saharan Africa, testing is low, with only about one in four (28%) of children with a fever receiving medical advice or a rapid diagnostic test in 2021. There was a 10-percentage point gap in testing between the richest and the poorest children (33% vs 23%). Additionally, a greater proportion of children in Eastern and Southern Africa (36%) were tested than in West and Central Africa (21%).[22] According to UNICEF, 61% of children with a fever were taken for advice or treatment from a health facility or provider in 2021. Disparities are also observed by wealth, with an 18 percentage point difference in care-seeking behaviour between children in the richest (71%) and the poorest (53%) households.[22]

Malaria is usually confirmed by the microscopic examination of blood films or by antigen-based rapid diagnostic tests (RDT). Microscopy—i.e. examining Giemsa-stained blood with a light microscope—is the gold standard for malaria diagnosis.[46] Microscopists typically examine both a "thick film" of blood, allowing them to scan many blood cells in a short time, and a "thin film" of blood, allowing them to clearly see individual parasites and identify the infecting Plasmodium species.[46] Under typical field laboratory conditions, a microscopist can detect parasites when there are at least 100 parasites per microliter of blood, which is around the lower range of symptomatic infection.[76] Microscopic diagnosis is relatively resource intensive, requiring trained personnel, specific equipment, electricity, and a consistent supply of microscopy slides and stains.[76]

In places where microscopy is unavailable, malaria is diagnosed with RDTs, rapid antigen tests that detect parasite proteins in a fingerstick blood sample.[76] A variety of RDTs are commercially available, targeting the parasite proteins histidine rich protein 2 (HRP2, detects P. falciparum only), lactate dehydrogenase, or aldolase.[76] The HRP2 test is widely used in Africa, where P. falciparum predominates.[46] However, since HRP2 persists in the blood for up to five weeks after an infection is treated, an HRP2 test sometimes cannot distinguish whether someone currently has malaria or previously had it.[76] Additionally, some P. falciparum parasites in the Amazon region lack the HRP2 gene, complicating detection.[76] RDTs are fast and easily deployed to places without full diagnostic laboratories.[76] However they give considerably less information than microscopy, and sometimes vary in quality from producer to producer and lot to lot.[76]

Serological tests to detect antibodies against Plasmodium from the blood have been developed, but are not used for malaria diagnosis due to their relatively poor sensitivity and specificity. Highly sensitive nucleic acid amplification tests have been developed, but are not used clinically due to their relatively high cost, and poor specificity for active infections.[76]

Classification

[edit]

Malaria is classified into either "severe" or "uncomplicated" by the World Health Organization (WHO).[15] It is deemed severe when any of the following criteria are present, otherwise it is considered uncomplicated.[77]

Cerebral malaria is defined as a severe P. falciparum-malaria presenting with neurological symptoms, including coma (with a Glasgow coma scale less than 11, or a Blantyre coma scale less than 3), or with a coma that lasts longer than 30 minutes after a seizure.[78]

Prevention

[edit]
An Anopheles stephensi mosquito shortly after obtaining blood from a human (the droplet of blood is expelled as a surplus). This mosquito is a vector of malaria, and mosquito control is an effective way of reducing its incidence.

Methods used to prevent malaria include medications, mosquito elimination and the prevention of bites. As of 2023, there are two malaria vaccines, approved for use in children by the WHO: RTS,S and R21.[16][79] The presence of malaria in an area requires a combination of high human population density, high Anopheles mosquito population density and high rates of transmission from humans to mosquitoes and from mosquitoes to humans. If any of these is lowered sufficiently, the parasite eventually disappears from that area, as happened in North America, Europe, and parts of the Middle East. However, unless the parasite is eliminated from the whole world, it could re-establish if conditions revert to a combination that favors the parasite's reproduction. Furthermore, the cost per person of eliminating anopheles mosquitoes rises with decreasing population density, making it economically unfeasible in some areas.[80]

Prevention of malaria may be more cost-effective than treatment of the disease in the long run, but the initial costs required are out of reach of many of the world's poorest people. There is a wide difference in the costs of control (i.e. maintenance of low endemicity) and elimination programs between countries. For example, in China—whose government in 2010 announced a strategy to pursue malaria elimination in the Chinese provinces—the required investment is a small proportion of public expenditure on health. In contrast, a similar programme in Tanzania would cost an estimated one-fifth of the public health budget.[81] In 2021, the World Health Organization confirmed that China has eliminated malaria.[82] In 2023, the World Health Organization confirmed that Azerbaijan, Tajikistan, and Belize have eliminated malaria.[83]

In areas where malaria is common, children under five years old often have anaemia, which is sometimes due to malaria. Giving children with anaemia in these areas preventive antimalarial medication improves red blood cell levels slightly but does not affect the risk of death or need for hospitalisation.[84]

Mosquito control

[edit]
Man spraying kerosene oil in standing water, Panama Canal Zone, 1912

Vector control refers to methods used to decrease malaria by reducing the levels of transmission by mosquitoes. For individual protection, the most effective insect repellents are based on DEET or picaridin.[85] However, there is insufficient evidence that mosquito repellents can prevent malaria infection.[86] Insecticide-treated nets (ITNs) and indoor residual spraying (IRS) are effective, have been commonly used to prevent malaria, and their use has contributed significantly to the decrease in malaria in the 21st century.[87][88][89] ITNs and IRS may not be sufficient to eliminate the disease, as these interventions depend on how many people use nets, how many gaps in insecticide there are (low coverage areas), if people are not protected when outside of the home, and an increase in mosquitoes that are resistant to insecticides.[87] Modifications to people's houses to prevent mosquito exposure may be an important long term prevention measure.[87]

Insecticide-treated nets

[edit]
A mosquito net in use

Mosquito nets help keep mosquitoes away from people and reduce infection rates and transmission of malaria. Nets are not a perfect barrier and are often treated with an insecticide designed to kill the mosquito before it has time to find a way past the net. Insecticide-treated nets (ITNs) are estimated to be twice as effective as untreated nets and offer greater than 70% protection compared with no net.[90] Between 2000 and 2008, the use of ITNs saved the lives of an estimated 250,000 infants in Sub-Saharan Africa.[91] According to UNICEF, only 36% of households had sufficient ITNs for all household members in 2019.[92] In 2000, 1.7 million (1.8%) African children living in areas of the world where malaria is common were protected by an ITN. That number increased to 20.3 million (18.5%) African children using ITNs in 2007, leaving 89.6 million children unprotected[93] and to 68% African children using mosquito nets in 2015.[94] The percentage of children sleeping under ITNs in sub-Saharan Africa increased from less than 40% in 2011 to over 50% in 2021.[22] Most nets are impregnated with pyrethroids, a class of insecticides with low toxicity. They are most effective when used from dusk to dawn.[95] It is recommended to hang a large "bed net" above the center of a bed and either tuck the edges under the mattress or make sure it is large enough such that it touches the ground.[96] ITNs are beneficial towards pregnancy outcomes in malaria-endemic regions in Africa but more data is needed in Asia and Latin America.[97]

In areas of high malaria resistance, piperonyl butoxide (PBO) combined with pyrethroids in mosquito netting is effective in reducing malaria infection rates.[98] Questions remain concerning the durability of PBO on nets as the impact on mosquito mortality was not sustained after twenty washes in experimental trials.[98]

UNICEF notes that the use of insecticide-treated nets has been increased since 2000 through accelerated production, procurement and delivery, stating that "over 2.5 billion ITNs have been distributed globally since 2004, with 87% (2.2 billion) distributed in sub-Saharan Africa. In 2021, manufacturers delivered about 220 million ITNs to malaria endemic countries, a decrease of 9 million ITNs compared with 2020 and 33 million less than were delivered in 2019".[23] As of 2021, 66% of households in sub-Saharan Africa had ITNs, with figures "ranging from 31 per cent in Angola in 2016 to approximately 97 per cent in Guinea-Bissau in 2019".[23] Slightly more than half of the households with an ITN had enough of them to protect all members of the household, however.[23]

Indoor residual spraying

[edit]
Walls where indoor residual spraying of DDT has been applied. The dead mosquitoes remain on the wall, eventually falling to the floor.

Indoor residual spraying is the spraying of insecticides on the walls inside a home. After feeding, many mosquitoes rest on a nearby surface while digesting the bloodmeal, so if the walls of houses have been coated with insecticides, the resting mosquitoes can be killed before they can bite another person and transfer the malaria parasite.[99] As of 2006, the World Health Organization recommends 12 insecticides in IRS operations, including DDT and the pyrethroids cyfluthrin and deltamethrin.[100] This public health use of small amounts of DDT is permitted under the Stockholm Convention, which prohibits its agricultural use.[101] One problem with all forms of IRS is insecticide resistance. Mosquitoes affected by IRS tend to rest and live indoors, and due to the irritation caused by spraying, their descendants tend to rest and live outdoors, meaning that they are less affected by the IRS.[102] Communities using insecticide treated nets, in addition to indoor residual spraying with 'non-pyrethroid-like' insecticides found associated reductions in malaria.[103] Additionally, the use of 'pyrethroid-like' insecticides in addition to indoor residual spraying did not result in a detectable additional benefit in communities using insecticide treated nets.[103]

Housing modifications

[edit]

Housing is a risk factor for malaria and modifying the house as a prevention measure may be a sustainable strategy that does not rely on the effectiveness of insecticides such as pyrethroids.[87][104] The physical environment inside and outside the home that may improve the density of mosquitoes are considerations. Examples of potential modifications include how close the home is to mosquito breeding sites, drainage and water supply near the home, availability of mosquito resting sites (vegetation around the home), the proximity to live stock and domestic animals, and physical improvements or modifications to the design of the home to prevent mosquitoes from entering,[87] such as window screens.

In addition to installing window screens, house screening measures include screening ceilings, doors, and eaves. In 2021, the World Health Organization's (WHO) Guideline Development Group conditionally recommended screening houses in this manner to reduce malaria transmission.[105] However, the WHO does point out that there are local considerations that need to be addressed when incorporating these techniques. These considerations include the delivery method, maintenance, house design, feasibility, resource needs, and scalability.[105]

Several studies have suggested that screening houses can have a significant impact on malaria transmission. Beyond the protective barrier screening provides, it also does not call for daily behavioral changes in the household.[106] Screening eaves can also have a community-level protective effect, ultimately reducing mosquito-biting densities in neighboring houses that do not have this intervention in place.[106]

In some cases, studies have used insecticide-treated (e.g., transfluthrin) or untreated netting to deter mosquito entry.[106] One widely used intervention is the In2Care BV EaveTube. In 2021, In2Care BV received funding from the United States Agency for International Development to develop a ventilation tube that would be installed in housing walls.[107] When mosquitoes approach households, the goal is for them to encounter these EaveTubes instead. Inside these EaveTubes is insecticide-treated netting that is lethal to insecticide-resistant mosquitoes.[107] This approach to mosquito control is called the Lethal House Lure method. The WHO is currently evaluating the efficacy of this product for widespread use.[108]

Mass drug administration

[edit]

Mass drug administration (MDA) involves the administration of drugs to the entire population of an area regardless of disease status.[109] A 2021 Cochrane review on the use of community administration of ivermectin found that, to date, low quality evidence shows no significant impact on reducing incidence of malaria transmission from the community administration of ivermectin.[110]

Mosquito-targeted drug delivery

[edit]

One potential way to reduce the burden of malaria is to target the infection in mosquitoes, before it enters the mammalian host (during sporogeny).[111] Drugs may be used for this purpose which have unacceptable toxicity profiles in humans. For example, aminoquinoline derivates show toxicity in humans,[13] but this has not been shown in mosquitoes. Primaquine is particularly effective against Plasmodium gametocytes. Likewise, pyrroloquinazolinediamines show unacceptable toxicity in mammals,[112] but it is unknown whether this is the case in mosquitoes. Pyronaridine, thiostrepton, and pyrimethamine have been shown to dramatically reduce ookinete formation in P. berghei, while artefenomel, NPC-1161B, and tert-butyl isoquine reduce exflagellation in P. Falciparum.[113]

Other mosquito control methods

[edit]

People have tried a number of other methods to reduce mosquito bites and slow the spread of malaria. Efforts to decrease mosquito larvae by decreasing the availability of open water where they develop, or by adding substances to decrease their development, are effective in some locations.[114] Electronic mosquito repellent devices, which make very high-frequency sounds that are supposed to keep female mosquitoes away, have no supporting evidence of effectiveness.[115] There is a low certainty evidence that fogging may have an effect on malaria transmission.[116] Larviciding by hand delivery of chemical or microbial insecticides into water bodies containing low larval distribution may reduce malarial transmission.[117] There is insufficient evidence to determine whether larvivorous fish can decrease mosquito density and transmission in the area.[118]

Medications

[edit]

There are a number of medications that can help prevent or interrupt malaria in travellers to places where infection is common. Many of these medications are also used in treatment. In places where Plasmodium is resistant to one or more medications, three medications—mefloquine, doxycycline, or the combination of atovaquone/proguanil (Malarone)—are frequently used for prevention.[119] Doxycycline and the atovaquone/proguanil are better tolerated while mefloquine is taken once a week.[119] Areas of the world with chloroquine-sensitive malaria are uncommon.[120] Antimalarial mass drug administration to an entire population at the same time may reduce the risk of contracting malaria in the population, however the effectiveness of mass drug administration may vary depending on the prevalence of malaria in the area.[121] Other factors such as drug administration plus other protective measures such as mosquito control, the proportion of people treated in the area, and the risk of reinfection with malaria may play a role in the effectiveness of mass drug treatment approaches.[121]

The protective effect does not begin immediately, and people visiting areas where malaria exists usually start taking the drugs one to two weeks before they arrive, and continue taking them for four weeks after leaving (except for atovaquone/proguanil, which only needs to be started two days before and continued for seven days afterward).[122] The use of preventive drugs is often not practical for those who live in areas where malaria exists, and their use is usually given only to pregnant women and short-term visitors. This is due to the cost of the drugs, side effects from long-term use, and the difficulty in obtaining antimalarial drugs outside of wealthy nations.[123] During pregnancy, medication to prevent malaria has been found to improve the weight of the baby at birth and decrease the risk of anaemia in the mother.[124] The use of preventive drugs where malaria-bearing mosquitoes are present may encourage the development of partial resistance.[125]

Giving antimalarial drugs to infants through intermittent preventive therapy can reduce the risk of having malaria infection, hospital admission, and anaemia.[126]

Mefloquine is more effective than sulfadoxine-pyrimethamine in preventing malaria for HIV-negative pregnant women. Cotrimoxazole is effective in preventing malaria infection and reduce the risk of getting anaemia in HIV-positive women.[127] Giving sulfadoxine-pyrimethamine for three or more doses as intermittent preventive therapy is superior than two doses for HIV-positive women living in malaria-endemic areas.[128][needs update]

Prompt treatment of confirmed cases with artemisinin-based combination therapies (ACTs) may also reduce transmission.[129]

Research on malaria vaccines

[edit]

Malaria vaccines have been another goal of research. The first promising studies demonstrating the potential for a malaria vaccine were performed in 1967 by immunising mice with live, radiation-attenuated sporozoites, which provided significant protection to the mice upon subsequent injection with normal, viable sporozoites. Since the 1970s, there has been considerable progress in developing similar vaccination strategies for humans.[130]

In 2013, WHO and the malaria vaccine funders group set a goal to develop vaccines designed to interrupt malaria transmission with malaria eradication's long-term goal.[131] The first vaccine, called RTS,S, was approved by European regulators in 2015.[132] As of 2023, two malaria vaccines have been licensed for use.[16] Other approaches to combat malaria may require investing more in research and greater primary health care.[133] Continuing surveillance will also be important to prevent the return of malaria in countries where the disease has been eliminated.[134]

As of 2019 it is undergoing pilot trials in 3 sub-Saharan African countries—Ghana, Kenya and Malawi—as part of the WHO's Malaria Vaccine Implementation Programme (MVIP).[135]

Immunity (or, more accurately, tolerance) to P. falciparum malaria does occur naturally, but only in response to years of repeated infection.[63][136] An individual can be protected from a P. falciparum infection if they receive about a thousand bites from mosquitoes that carry a version of the parasite rendered non-infective by a dose of X-ray irradiation.[137] The highly polymorphic nature of many P. falciparum proteins results in significant challenges to vaccine design. Vaccine candidates that target antigens on gametes, zygotes, or ookinetes in the mosquito midgut aim to block the transmission of malaria. These transmission-blocking vaccines induce antibodies in the human blood; when a mosquito takes a blood meal from a protected individual, these antibodies prevent the parasite from completing its development in the mosquito.[138] Other vaccine candidates, targeting the blood-stage of the parasite's life cycle, have been inadequate on their own.[139] For example, SPf66 was tested extensively in areas where the disease was common in the 1990s, but trials showed it to be insufficiently effective.[140]

As of 2020, the RTS,S vaccine has been shown to reduce the risk of malaria by about 40% in children in Africa.[79][141] A preprint study of the R21 vaccine has shown 77% vaccine efficacy.[needs update][142]

In 2021, researchers from the University of Oxford reported findings from a Phase IIb trial of a candidate malaria vaccine, R21/Matrix-M, which demonstrated efficacy of 77% over 12-months of follow-up. This vaccine is the first to meet the World Health Organization's Malaria Vaccine Technology Roadmap goal of a vaccine with at least 75% efficacy.[143]

Germany-based BioNTECH SE is developing an mRNA-based malaria vaccine BN165 [144] which has recently initiated a Phase 1 study [clinicaltrials.gov identifier: NCT05581641] in December 2022. The vaccine, based on the circumsporozite protein (CSP) is being tested in adults aged 18–55 yrs at 3 dose levels to select a safe and tolerable dose of a three-dose schedule. Unlike GSK's RTS,S (AS01) and Serum Institute of India's R21/MatrixM, BNT-165 is being studied in adult age groups meaning it could be developed for Western travelers as well as those living in endemic countries. For the travelers profile, a recent commercial assessment forecast potential gross revenues of BNT-165 at $479m (2030) 5-yrs post launch, POS-adjusted revenues.[145]

Others

[edit]

Community participation and health education strategies promoting awareness of malaria and the importance of control measures have been successfully used to reduce the incidence of malaria in some areas of the developing world.[146] Recognising the disease in the early stages can prevent it from becoming fatal. Education can also inform people to cover over areas of stagnant, still water, such as water tanks that are ideal breeding grounds for the parasite and mosquito, thus cutting down the risk of the transmission between people. This is generally used in urban areas where there are large centers of population in a confined space and transmission would be most likely in these areas.[147] Intermittent preventive therapy is another intervention that has been used successfully to control malaria in pregnant women and infants,[148] and in preschool children where transmission is seasonal.[149]

Treatment

[edit]
Advertisement entitled "The Mosquito Danger". Includes 6 panel cartoon:#1 breadwinner has malaria, family starving; #2 wife selling ornaments; #3 doctor administers quinine; #4 patient recovers; #5 doctor indicating that quinine can be obtained from post office if needed again; #6 man who refused quinine, dead on stretcher.
An advertisement for quinine as a malaria treatment from 1927.

Malaria is treated with antimalarial medications; the ones used depend on the type and severity of the disease.[150] While medications against fever are commonly used, their effects on outcomes are not clear.[151][152] Providing free antimalarial drugs to households may reduce childhood deaths when used appropriately. Programmes which presumptively treat all causes of fever with antimalarial drugs may lead to overuse of antimalarials and undertreat other causes of fever. Nevertheless, the use of malaria rapid-diagnostic kits can help to reduce over-usage of antimalarials.[153][154]

Uncomplicated malaria

[edit]

Simple or uncomplicated malaria may be treated with oral medications. Artemisinin drugs are effective and safe in treating uncomplicated malaria.[155] Artemisinin in combination with other antimalarials (known as artemisinin-combination therapy, or ACT) is about 90% effective when used to treat uncomplicated malaria.[91] The most effective treatment for P. falciparum infection is the use of ACT, which decreases resistance to any single drug component.[156][157] Artemether-lumefantrine (six-dose regimen) is more effective than the artemether-lumefantrine (four-dose regimen) or other regimens not containing artemisinin derivatives in treating falciparum malaria.[158][159] Another recommended combination is dihydroartemisinin and piperaquine.[160][161][162] Artemisinin-naphthoquine combination therapy showed promising results in treating falciparum malaria but more research is needed to establish its efficacy as a reliable treatment.[163] Artesunate plus mefloquine performs better than mefloquine alone in treating uncomplicated falciparum malaria in low transmission settings.[164] Atovaquone-proguanil is effective against uncomplicated falciparum with a possible failure rate of 5% to 10%; the addition of artesunate may reduce failure rate.[165] Azithromycin monotherapy or combination therapy has not shown effectiveness in treating Plasmodium falciparum or Plasmodium vivax malaria.[166] Amodiaquine plus sulfadoxine-pyrimethamine may achieve less treatment failures when compared to sulfadoxine-pyrimethamine alone in uncomplicated falciparum malaria.[167] There is insufficient data on chlorproguanil-dapsone in treating uncomplicated falciparum malaria.[168][169] The addition of primaquine with artemisinin-based combination therapy for falciparum malaria reduces its transmission at day 3-4 and day 8 of infection.[170] Sulfadoxine-pyrimethamine plus artesunate is better than sulfadoxine-pyrimethamine plus amodiaquine in controlling treatment failure at day 28. However, the latter is better than the former in reducing gametocytes in blood at day 7.[171]

Infection with P. vivax, P. ovale or P. malariae usually does not require hospitalisation. Treatment of P. vivax malaria requires both elimination of the parasite in the blood with chloroquine or with artemisinin-based combination therapy and clearance of parasites from the liver with an 8-aminoquinoline agent such as primaquine or tafenoquine.[172][173] These two drugs act against blood stages as well, the extent to which they do so still being under investigation.[174]

To treat malaria during pregnancy, the WHO recommends the use of quinine plus clindamycin early in the pregnancy (1st trimester), and ACT in later stages (2nd and 3rd trimesters).[175][176] There is limited safety data on the antimalarial drugs in pregnancy.[177]

Severe and complicated malaria

[edit]

Cases of severe and complicated malaria are almost always caused by infection with P. falciparum. The other species usually cause only febrile disease.[178] Severe and complicated malaria cases are medical emergencies since mortality rates are high (10% to 50%).[179]

Recommended treatment for severe malaria is the intravenous use of antimalarial drugs. For severe malaria, parenteral artesunate was superior to quinine in both children and adults.[180][181] In another systematic review, artemisinin derivatives (artemether and arteether) were as efficacious as quinine in the treatment of cerebral malaria in children.[182] Treatment of severe malaria involves supportive measures that are best done in a critical care unit. This includes the management of high fevers and the seizures that may result from it. It also includes monitoring for poor breathing effort, low blood sugar, and low blood potassium.[47] Artemisinin derivatives have the same or better efficacy than quinolones in preventing deaths in severe or complicated malaria.[183] Quinine loading dose helps to shorten the duration of fever and increases parasite clearance from the body.[184] There is no difference in effectiveness when using intrarectal quinine compared to intravenous or intramuscular quinine in treating uncomplicated/complicated falciparum malaria.[185] There is insufficient evidence for intramuscular arteether to treat severe malaria.[186] The provision of rectal artesunate before transfer to hospital may reduce the rate of death for children with severe malaria.[187] In children with malaria and concomitant hypoglycaemia, sublingual administration of glucose appears to result in better increases in blood sugar after 20 minutes when compared to oral administration, based on very limited data.[188]

Cerebral malaria is the form of severe and complicated malaria with the worst neurological symptoms.[189] There is insufficient data on whether osmotic agents such as mannitol or urea are effective in treating cerebral malaria.[190] Routine phenobarbitone in cerebral malaria is associated with fewer convulsions but possibly more deaths.[191] There is no evidence that steroids would bring treatment benefits for cerebral malaria.[192]

Managing cerebral malaria Cerebral malaria usually makes a patient comatose. If the cause of the coma is in doubt, testing for other locally prevalent causes of encephalopathy (bacterial, viral or fungal infection) should be carried out. In areas where there is a high prevalence of malaria infection (e.g. tropical region) treatment can start without testing first.[45] To manage the cerebral malaria when confirmed the following can be done:

  • People who are in coma should be given meticulous nursing care ( monitor vital signs, turn patient every 2 hours, avoid lying the patient in a wet bed etc.)
  • A sterile urethral catheter should be inserted to help with urinating
  • To aspirate stomach content, a sterile nasogastric tube should be inserted.
  • In the occasion of convulsions, a slow intravenous injection of benzodiazepine is administered.[193]

There is insufficient evidence to show that blood transfusion is useful in either reducing deaths for children with severe anaemia or in improving their haematocrit in one month.[194] There is insufficient evidence that iron chelating agents such as deferoxamine and deferiprone improve outcomes of those with malaria falciparum infection.[195]

Monoclonal antibodies

[edit]

A 2022 clinical trial shows that a monoclonal antibody mAb L9LS offers protection against malaria. It binds the Plasmodium falciparum circumsporozoite protein (CSP-1), essential to disease, and makes it ineffective.[196]

Resistance

[edit]

Drug resistance poses a growing problem in 21st-century malaria treatment.[197] In the 2000s (decade), malaria with partial resistance to artemisins emerged in Southeast Asia.[198][199] Resistance is now common against all classes of antimalarial drugs apart from artemisinins. Treatment of resistant strains became increasingly dependent on this class of drugs. The cost of artemisinins limits their use in the developing world.[200] Malaria strains found on the Cambodia–Thailand border are resistant to combination therapies that include artemisinins, and may, therefore, be untreatable.[201] Exposure of the parasite population to artemisinin monotherapies in subtherapeutic doses for over 30 years and the availability of substandard artemisinins likely drove the selection of the resistant phenotype.[202] Resistance to artemisinin has been detected in Cambodia, Myanmar, Thailand, and Vietnam,[203] and there has been emerging resistance in Laos.[204][205] Resistance to the combination of artemisinin and piperaquine was first detected in 2013 in Cambodia, and by 2019 had spread across Cambodia and into Laos, Thailand and Vietnam (with up to 80 percent of malaria parasites resistant in some regions).[206]

There is insufficient evidence in unit packaged antimalarial drugs in preventing treatment failures of malaria infection. However, if supported by training of healthcare providers and patient information, there is improvement in compliance of those receiving treatment.[207]

Prognosis

[edit]
Disability-adjusted life year for malaria per 100,000 inhabitants in 2004
   no data
   <10
   0–100
   100–500
   500–1000
  1000–1500
  1500–2000
  2000–2500
  2500–2750
  2750–3000
  3000–3250
  3250–3500
   ≥3500

When properly treated, people with malaria can usually expect a complete recovery.[208] However, severe malaria can progress extremely rapidly and cause death within hours or days.[209] In the most severe cases of the disease, fatality rates can reach 20%, even with intensive care and treatment.[15] Over the longer term, developmental impairments have been documented in children who have had episodes of severe malaria.[210] Chronic infection without severe disease can occur in an immune-deficiency syndrome associated with a decreased responsiveness to Salmonella bacteria and the Epstein–Barr virus.[211]

During childhood, malaria causes anaemia during a period of rapid brain development, and also direct brain damage resulting from cerebral malaria.[210] Some survivors of cerebral malaria have an increased risk of neurological and cognitive deficits, behavioural disorders, and epilepsy.[212] Malaria prophylaxis was shown to improve cognitive function and school performance in clinical trials when compared to placebo groups.[210]

Epidemiology

[edit]
Deaths due to malaria per million persons in 2012
  0–0
  1–2
  3–54
  55–325
  326–679
  680–949
  950–1,358
Past and current malaria prevalence in 2009
Relative incidence of Plasmodium species by country of origin for imported cases to non-endemic countries[213]

The WHO estimates that in 2021 there were 247 million total cases of malaria resulting in 619,000 deaths.[18] Children under five years old are the most affected, accounting for 67% of malaria deaths worldwide in 2019.[214] About 125 million pregnant women are at risk of infection each year; in Sub-Saharan Africa, maternal malaria is associated with up to 200,000 estimated infant deaths yearly.[43] Since 2015, the WHO European Region has been free of malaria. The last country to report an indigenous malaria case was Tajikistan in 2014.[18] There are about 1300–1500 malaria cases per year in the United States.[39] The United States eradicated malaria as a major public health concern in 1951,[215] though small outbreaks persist.[216] Locally acquired mosquito-borne malaria occurred in the United States in 2003, when eight cases of locally acquired P. vivax malaria were identified in Florida, and again in May 2023, in four cases, as well as one case in Texas,[217] and in August in one case in Maryland.[218] About 900 people died from the disease in Europe between 1993 and 2003.[85] Both the global incidence of disease and resulting mortality have declined in recent years. According to the WHO and UNICEF, deaths attributable to malaria in 2015 were reduced by 60%[94] from a 2000 estimate of 985,000, largely due to the widespread use of insecticide-treated nets and artemisinin-based combination therapies.[91] Between 2000 and 2019, malaria mortality rates among all ages halved from about 30 to 13 per 100,000 population at risk. During this period, malaria deaths among children under five also declined by nearly half (47%) from 781,000 in 2000 to 416,000 in 2019.[92]

Malaria is presently endemic in a broad band around the equator, in areas of the Americas, many parts of Asia, and much of Africa; in Sub-Saharan Africa, 85–90% of malaria fatalities occur.[219] An estimate for 2009 reported that countries with the highest death rate per 100,000 of population were Ivory Coast (86.15), Angola (56.93) and Burkina Faso (50.66).[220] A 2010 estimate indicated the deadliest countries per population were Burkina Faso, Mozambique and Mali.[221] The Malaria Atlas Project aims to map global levels of malaria, providing a way to determine the global spatial limits of the disease and to assess disease burden.[222][223] This effort led to the publication of a map of P. falciparum endemicity in 2010 and an update in 2019.[224][225][226] As of 2021, 84 countries have endemic malaria.[18]

The geographic distribution of malaria within large regions is complex, and malaria-afflicted and malaria-free areas are often found close to each other.[227] Malaria is prevalent in tropical and subtropical regions because of rainfall, consistent high temperatures and high humidity, along with stagnant waters where mosquito larvae readily mature, providing them with the environment they need for continuous breeding.[228] In drier areas, outbreaks of malaria have been predicted with reasonable accuracy by mapping rainfall.[229] Malaria is more common in rural areas than in cities. For example, several cities in the Greater Mekong Subregion of Southeast Asia are essentially malaria-free, but the disease is prevalent in many rural regions, including along international borders and forest fringes.[230] In contrast, malaria in Africa is present in both rural and urban areas, though the risk is lower in the larger cities.[231]

Climate change

[edit]

Climate change is likely to affect malaria transmission, but the degree of effect and the areas affected is uncertain.[232] Greater rainfall in certain areas of India, and following an El Niño event is associated with increased mosquito numbers.[233]

Since 1900 there has been substantial change in temperature and rainfall over Africa.[234] However, factors that contribute to how rainfall results in water for mosquito breeding are complex, incorporating the extent to which it is absorbed into soil and vegetation for example, or rates of runoff and evaporation.[235] Recent research has provided a more in-depth picture of conditions across Africa, combining a malaria climatic suitability model with a continental-scale model representing real-world hydrological processes.[235]

History

[edit]
Ancient malaria oocysts preserved in Dominican amber

Although the parasite responsible for P. falciparum malaria has been in existence for 50,000–100,000 years, the population size of the parasite did not increase until about 10,000 years ago, concurrently with advances in agriculture[236] and the development of human settlements. Close relatives of the human malaria parasites remain common in chimpanzees. Some evidence suggests that the P. falciparum malaria may have originated in gorillas.[237]

References to the unique periodic fevers of malaria are found throughout history.[238] Ancient Indian physician Sushruta is believed to be among the first to attribute the disease to mosquitoes,[239] long before the Roman Columella associated the disease with insects from swamps.[240] Hippocrates described periodic fevers, labelling them tertian, quartan, subtertian and quotidian.[240] Malaria may have contributed to the decline of the Roman Empire,[241] and was so pervasive in Rome that it was known as the "Roman fever".[242] Several regions in ancient Rome were considered at-risk for the disease because of the favourable conditions present for malaria vectors. This included areas such as southern Italy, the island of Sardinia, the Pontine Marshes, the lower regions of coastal Etruria and the city of Rome along the Tiber. The presence of stagnant water in these places was preferred by mosquitoes for breeding grounds. Irrigated gardens, swamp-like grounds, run-off from agriculture, and drainage problems from road construction led to the increase of standing water.[243]

British doctor Ronald Ross received the Nobel Prize for Physiology or Medicine in 1902 for his work on malaria.

Malaria is not referenced in the medical books of the Mayans or Aztecs. Despite this, antibodies against malaria have been detected in some South American mummies, indicating that some malaria strains in the Americas might have a pre-Columbian origin.[244] European settlers and the West Africans they enslaved likely brought malaria to the Americas starting in the 16th century.[245][246]

Scientific studies on malaria made their first significant advance in 1880, when Charles Louis Alphonse Laveran—a French army doctor working in the military hospital of Constantine in Algeria—observed parasites inside the red blood cells of infected people for the first time.[247] He, therefore, proposed that malaria is caused by this organism, the first time a protist was identified as causing disease.[248] For this and later discoveries, he was awarded the 1907 Nobel Prize for Physiology or Medicine. A year later, Carlos Finlay, a Cuban doctor treating people with yellow fever in Havana, provided strong evidence that mosquitoes were transmitting disease to and from humans.[249] This work followed earlier suggestions by Josiah C. Nott,[250] and work by Sir Patrick Manson, the "father of tropical medicine", on the transmission of filariasis.[251]

Chinese medical researcher Tu Youyou received the Nobel Prize for Physiology or Medicine in 2015 for her work on the antimalarial drug artemisinin.

In April 1894, a Scottish physician, Sir Ronald Ross, visited Sir Patrick Manson at his house on Queen Anne Street, London. This visit was the start of four years of collaboration and fervent research that culminated in 1897 when Ross, who was working in the Presidency General Hospital in Calcutta, proved the complete life-cycle of the malaria parasite in mosquitoes.[252] He thus proved that the mosquito was the vector for malaria in humans by showing that certain mosquito species transmit malaria to birds. He isolated malaria parasites from the salivary glands of mosquitoes that had fed on infected birds.[252] For this work, Ross received the 1902 Nobel Prize in Medicine. After resigning from the Indian Medical Service, Ross worked at the newly established Liverpool School of Tropical Medicine and directed malaria-control efforts in Egypt, Panama, Greece and Mauritius.[253] The findings of Finlay and Ross were later confirmed by a medical board headed by Walter Reed in 1900. Its recommendations were implemented by William C. Gorgas in the health measures undertaken during construction of the Panama Canal. This public-health work saved the lives of thousands of workers and helped develop the methods used in future public-health campaigns against the disease.[254]

In 1896, Amico Bignami discussed the role of mosquitoes in malaria.[255] In 1898, Bignami, Giovanni Battista Grassi and Giuseppe Bastianelli succeeded in showing experimentally the transmission of malaria in humans, using infected mosquitoes to contract malaria themselves which they presented in November 1898 to the Accademia dei Lincei.[252]

Artemisia annua, source of the antimalarial drug artemisinin

The first effective treatment for malaria came from the bark of cinchona tree, which contains quinine. This tree grows on the slopes of the Andes, mainly in Peru. The indigenous peoples of Peru made a tincture of cinchona to control fever. Its effectiveness against malaria was found and the Jesuits introduced the treatment to Europe around 1640; by 1677, it was included in the London Pharmacopoeia as an antimalarial treatment.[256] It was not until 1820 that the active ingredient, quinine, was extracted from the bark, isolated and named by the French chemists Pierre Joseph Pelletier and Joseph Bienaimé Caventou.[257][258]

Quinine was the predominant malarial medication until the 1920s when other medications began to appear. In the 1940s, chloroquine replaced quinine as the treatment of both uncomplicated and severe malaria until resistance supervened, first in Southeast Asia and South America in the 1950s and then globally in the 1980s.[259]

The medicinal value of Artemisia annua has been used by Chinese herbalists in traditional Chinese medicines for 2,000 years.[260][261] In 1596, Li Shizhen recommended tea made from qinghao specifically to treat malaria symptoms in his "Compendium of Materia Medica", however the efficacy of tea, made with A. annua, for the treatment of malaria is dubious, and is discouraged by the World Health Organization (WHO).[262][263] Artemisinins, discovered by Chinese scientist Tu Youyou and colleagues in the 1970s from the plant Artemisia annua, became the recommended treatment for P. falciparum malaria, administered in severe cases in combination with other antimalarials.[264] Tu says she was influenced by a traditional Chinese herbal medicine source, The Handbook of Prescriptions for Emergency Treatments, written in 340 by Ge Hong.[265] For her work on malaria, Tu Youyou received the 2015 Nobel Prize in Physiology or Medicine.[266]

Plasmodium vivax was used between 1917 and the 1940s for malariotherapy—deliberate injection of malaria parasites to induce a fever to combat certain diseases such as tertiary syphilis. In 1927, the inventor of this technique, Julius Wagner-Jauregg, received the Nobel Prize in Physiology or Medicine for his discoveries. The technique was dangerous, killing about 15% of patients, so it is no longer in use.[267]

U.S. Marines with malaria in a field hospital on Guadalcanal, October 1942

The first pesticide used for indoor residual spraying was DDT.[268] Although it was initially used exclusively to combat malaria, its use quickly spread to agriculture. In time, pest control, rather than disease control, came to dominate DDT use, and this large-scale agricultural use led to the evolution of pesticide-resistant mosquitoes in many regions. The DDT resistance shown by Anopheles mosquitoes can be compared to antibiotic resistance shown by bacteria. During the 1960s, awareness of the negative consequences of its indiscriminate use increased, ultimately leading to bans on agricultural applications of DDT in many countries in the 1970s.[101] Before DDT, malaria was successfully eliminated or controlled in tropical areas like Brazil and Egypt by removing or poisoning the breeding grounds of the mosquitoes or the aquatic habitats of the larval stages, for example by applying the highly toxic arsenic compound Paris Green to places with standing water.[269]

Names

[edit]

Various types of malaria have been called by the names below:[citation needed]

Name Pathogen Notes
algid malaria Plasmodium falciparum severe malaria affecting the cardiovascular system and causing chills and circulatory shock
bilious malaria Plasmodium falciparum severe malaria affecting the liver and causing vomiting and jaundice
cerebral malaria Plasmodium falciparum severe malaria affecting the cerebrum
congenital malaria various plasmodia Plasmodium introduced from the mother via the fetal circulation
pernicious malaria Plasmodium falciparum severe malaria leading to grave illness
malignant malaria Plasmodium falciparum severe malaria leading to death
falciparum malaria, Plasmodium falciparum malaria, Plasmodium falciparum
ovale malaria, Plasmodium ovale malaria Plasmodium ovale
quartan malaria, malariae malaria, Plasmodium malariae malaria Plasmodium malariae paroxysms every fourth day (quartan), counting the day of occurrence as the first day
quotidian malaria Plasmodium falciparum, Plasmodium vivax, Plasmodium knowlesi paroxysms daily (quotidian)
tertian malaria Plasmodium falciparum, Plasmodium ovale, Plasmodium vivax paroxysms every third day (tertian), counting the day of occurrence as the first
transfusion malaria various plasmodia Plasmodium introduced by blood transfusion, needle sharing, or needlestick injury
vivax malaria, Plasmodium vivax malaria Plasmodium vivax

Eradication efforts

[edit]
Members of the Malaria Commission of the League of Nations collecting larvae on the Danube delta, 1929

Malaria has been successfully eliminated or significantly reduced in certain areas, but not globally. Malaria was once common in the United States, but the US eliminated malaria from most parts of the country in the early 20th century using vector control programs, which combined the monitoring and treatment of infected humans, draining of wetland breeding grounds for agriculture and other changes in water management practices, and advances in sanitation, including greater use of glass windows and screens in dwellings.[270] The use of the pesticide DDT and other means eliminated malaria from the remaining pockets in southern states of the US in the 1950s, as part of the National Malaria Eradication Program.[271] Most of Europe, North America, Australia, North Africa and the Caribbean, and parts of South America, Asia and Southern Africa have also eliminated malaria.[272] The WHO defines "elimination" (or "malaria-free") as having no domestic transmission (indigenous cases) for the past three years. They also define "pre-elimination" and "elimination" stages when a country has fewer than 5 or 1, respectively, cases per 1000 people at risk per year. In 2021, the total of international and national funding for malaria control and elimination was $3.5 billion—only half of what is estimated to be needed.[22] According to UNICEF, to achieve the goal of a malaria-free world, annual funding would need to more than double to reach the US$6.8 billion target.[22]

In parts of the world with rising living standards, the elimination of malaria was often a collateral benefit of the introduction of window screens and improved sanitation.[273] A variety of usually simultaneous interventions represents best practice. These include antimalarial drugs to prevent or treat infection; improvements in public health infrastructure to diagnose, sequester and treat infected individuals; bednets and other methods intended to keep mosquitoes from biting humans; and vector control strategies[274] such as larvaciding with insecticides, ecological controls such as draining mosquito breeding grounds or introducing fish to eat larvae and indoor residual spraying (IRS) with insecticides.

Initial WHO program (1955–1969)

[edit]
1962 Pakistani postage stamp promoting malaria eradication program

In 1955 the WHO launched the Global Malaria Eradication Program (GMEP).[275] The program relied largely on DDT for mosquito control and rapid diagnosis and treatment to break the transmission cycle.[276] The program eliminated the disease in "North America, Europe, the former Soviet Union",[277] and in "Taiwan, much of the Caribbean, the Balkans, parts of northern Africa, the northern region of Australia, and a large swath of the South Pacific"[273] and dramatically reduced mortality in Sri Lanka and India.[278]

However, failure to sustain the program, increasing mosquito tolerance to DDT, and increasing parasite tolerance led to a resurgence. In many areas early successes partially or completely reversed, and in some cases rates of transmission increased.[279] Experts tie malarial resurgence to multiple factors, including poor leadership, management and funding of malaria control programs; poverty; civil unrest; and increased irrigation. The evolution of resistance to first-generation drugs (e.g. chloroquine) and to insecticides exacerbated the situation.[280][281] The program succeeded in eliminating malaria only in areas with "high socio-economic status, well-organized healthcare systems, and relatively less intensive or seasonal malaria transmission".[277]

For example, in Sri Lanka, the program reduced cases from about one million per year before spraying to just 18 in 1963[282][283] and 29 in 1964. Thereafter the program was halted to save money and malaria rebounded to 600,000 cases in 1968 and the first quarter of 1969. The country resumed DDT vector control but the mosquitoes had evolved resistance in the interim, presumably because of continued agricultural use. The program switched to malathion, but despite initial successes, malaria continued its resurgence into the 1980s.[278][284]

Due to vector and parasite resistance and other factors, the feasibility of eradicating malaria with the strategy used at the time and resources available led to waning support for the program.[285] WHO suspended the program in 1969[275][285] and attention instead focused on controlling and treating the disease. Spraying programs (especially using DDT) were curtailed due to concerns over safety and environmental effects, as well as problems in administrative, managerial and financial implementation.[279] Efforts shifted from spraying to the use of bednets impregnated with insecticides and other interventions.[277][286]

After 1969

[edit]
Regions where malaria has been eliminated as of 2009

Target 6C of the Millennium Development Goals included reversal of the global increase in malaria incidence by 2015, with specific targets for children under five years old.[287] Since 2000, support for malaria eradication increased, although some actors in the global health community (including voices within the WHO) view malaria eradication as a premature goal and suggest that the establishment of strict deadlines for malaria eradication may be counterproductive as they are likely to be missed.[288] One of the targets of Goal 3 of the UN's Sustainable Development Goals is to end the malaria epidemic in all countries by 2030.

In 2006, the organization Malaria No More set a public goal of eliminating malaria from Africa by 2015, and the organization claimed they planned to dissolve if that goal was accomplished. In 2007, World Malaria Day was established by the 60th session of the World Health Assembly. As of 2018, they are still functioning.[289]

Video recording of a set of presentations given in 2010 about humanity's efforts towards malaria eradication

As of 2012, The Global Fund to Fight AIDS, Tuberculosis, and Malaria has distributed 230 million insecticide-treated nets intended to stop mosquito-borne transmission of malaria.[290] The U.S.-based Clinton Foundation has worked to manage demand and stabilize prices in the artemisinin market.[291] Other efforts, such as the Malaria Atlas Project, focus on analysing climate and weather information required to accurately predict malaria spread based on the availability of habitat of malaria-carrying parasites.[222] The Malaria Policy Advisory Committee (MPAC) of the World Health Organization (WHO) was formed in 2012, "to provide strategic advice and technical input to WHO on all aspects of malaria control and elimination".[292]

In 2015 the WHO targeted a 90% reduction in malaria deaths by 2030,[293] and Bill Gates said in 2016 that he thought global eradication would be possible by 2040.[294] According to the WHO's World Malaria Report 2015, the global mortality rate for malaria fell by 60% between 2000 and 2015. The WHO targeted a further 90% reduction between 2015 and 2030,[295] with a 40% reduction and eradication in 10 countries by 2020.[133] However, the 2020 goal was missed with a slight increase in cases compared to 2015.[296] Additionally, UNICEF reported that the number of malaria deaths for all ages increased by 10% between 2019 and 2020, in part due to service disruptions related to the COVID-19 pandemic, before experiencing a minor decline in 2021.[22]

Before 2016, the Global Fund against HIV/AIDS, Tuberculosis and Malaria had provided 659 million ITN (insecticide treated bed nets), organise support and education to prevents malaria. The challenges are high due to the lack of funds, the fragile health structure and the remote indigenous population that could be hard to reach and educate. Most of indigenous population rely on self-diagnosis, self-treatment, healer, and traditional medicine. The WHO applied for fund to the Gates Foundation which favour the action of malaria eradication in 2007.[297] Six countries, the United Arab Emirates, Morocco, Armenia, Turkmenistan, Kyrgyzstan, and Sri Lanka managed to have no endemic cases of malaria for three consecutive years and certified malaria-free by the WHO despite the stagnation of the funding in 2010.[287] The funding is essential to finance the cost of medication and hospitalisation cannot be supported by the poor countries where the disease is widely spread. The goal of eradication has not been met; nevertheless, the decrease rate of the disease is considerable.

While 31 out of 92 endemic countries were estimated to be on track with the WHO goals for 2020, 15 countries reported an increase of 40% or more between 2015 and 2020.[296] Between 2000 and 30 June 2021, twelve countries were certified by the WHO as being malaria-free. Argentina and Algeria were declared free of malaria in 2019.[296][298] El Salvador and China were declared malaria-free in the first half of 2021.[299][300]

Regional disparities were evident: Southeast Asia was on track to meet WHO's 2020 goals, while Africa, Americas, Eastern Mediterranean and West Pacific regions were off-track.[296] The six Greater Mekong Subregion countries aim for elimination of P. falciparum transmitted malaria by 2025 and elimination of all malaria by 2030, having achieved a 97% and 90% reduction of cases respectively since 2000.[296] Ahead of World Malaria Day, 25 April 2021, WHO named 25 countries in which it is working to eliminate malaria by 2025 as part of its E-2025 initiative.[301]

A major challenge to malaria elimination is the persistence of malaria in border regions, making international cooperation crucial.[302]

In 2018, WHO announced that Paraguay was free of malaria, after a national malaria eradication effort that began in 1950.[303]

In March 2023, the WHO certified Azerbaijan and Tajikistan as malaria-free,[304] and Belize in June 2023.[305] Cabo Verde, the latest country to eradicate Malaria, was certified in January 2024, bringing the total number of countries and territories certified malaria-free to 44.[306] In October 2024, the WHO certified Egypt to be malaria-free.[307]

Potential eradication of malaria by year 2050

[edit]

Experts say that malaria could be eliminated as wild disease of humans by the year 2050. World class experts (41 of them) in fields such as malariology, biomedicine, economics and health policy advocated more funding, a central data repository for dealing with local outbreaks of malaria, and training the workers needed to carry out the plan. Details are published in The Lancet. The report refers to current knowledge, recent research and financial matters to describe a respectable plan.[308]

The number of countries in which malaria was endemic was reduced from 200 to 86 in the years from 1900 to 2017. A further reduction by another 20 countries occurred by 2020. In light of the indication of possible practical accomplishment, countries and regions are planning further progress. Through the use of top notch diagnostic technique, effective treatment and vector reduction the world should be nearly free of malaria by 2050. This will require technical improvements in organizational efficiency and more monetary outlays.[309]

Society and culture

[edit]

Economic impact

[edit]
Malaria clinic in Tanzania

Malaria is not just a disease commonly associated with poverty; some evidence suggests that it is also a cause of poverty and a major hindrance to economic development.[24][25] Although tropical regions are most affected, malaria's furthest influence reaches into some temperate zones that have extreme seasonal changes. The disease has been associated with major negative economic effects on regions where it is widespread. During the late 19th and early 20th centuries, it was a major factor in the slow economic development of the American southern states.[310]

A comparison of average per capita GDP in 1995, adjusted for parity of purchasing power, between countries with malaria and countries without malaria gives a fivefold difference (US$1,526 versus US$8,268). In the period 1965 to 1990, countries where malaria was common had an average per capita GDP that increased only 0.4% per year, compared to 2.4% per year in other countries.[311]

Poverty can increase the risk of malaria since those in poverty do not have the financial capacities to prevent or treat the disease. In its entirety, the economic impact of malaria has been estimated to cost Africa US$12 billion every year. The economic impact includes costs of health care, working days lost due to sickness, days lost in education, decreased productivity due to brain damage from cerebral malaria, and loss of investment and tourism.[26] The disease has a heavy burden in some countries, where it may be responsible for 30–50% of hospital admissions, up to 50% of outpatient visits, and up to 40% of public health spending.[312]

Child with malaria in Ethiopia

Cerebral malaria is one of the leading causes of neurological disabilities in African children.[212] Studies comparing cognitive functions before and after treatment for severe malarial illness continued to show significantly impaired school performance and cognitive abilities even after recovery.[210] Consequently, severe and cerebral malaria have far-reaching socioeconomic consequences that extend beyond the immediate effects of the disease.[313]

Counterfeit and substandard drugs

[edit]

Sophisticated counterfeits have been found in several Asian countries such as Cambodia,[314] China,[315] Indonesia, Laos, Thailand, and Vietnam, and are a major cause of avoidable death in those countries.[316] The WHO said that studies indicate that up to 40% of artesunate-based malaria medications are counterfeit, especially in the Greater Mekong region. They have established a rapid alert system to rapidly report information about counterfeit drugs to relevant authorities in participating countries.[317] There is no reliable way for doctors or lay people to detect counterfeit drugs without help from a laboratory. Companies are attempting to combat the persistence of counterfeit drugs by using new technology to provide security from source to distribution.[318]

Another clinical and public health concern is the proliferation of substandard antimalarial medicines resulting from inappropriate concentration of ingredients, contamination with other drugs or toxic impurities, poor quality ingredients, poor stability and inadequate packaging.[319] A 2012 study demonstrated that roughly one-third of antimalarial medications in Southeast Asia and Sub-Saharan Africa failed chemical analysis, packaging analysis, or were falsified.[320]

War

[edit]
World War II poster

Throughout history, the contraction of malaria has played a prominent role in the fates of government rulers, nation-states, military personnel, and military actions.[321] In 1910, Nobel Prize in Medicine-winner Ronald Ross (himself a malaria survivor), published a book titled The Prevention of Malaria that included a chapter titled "The Prevention of Malaria in War". The chapter's author, Colonel C. H. Melville, Professor of Hygiene at Royal Army Medical College in London, addressed the prominent role that malaria has historically played during wars: "The history of malaria in war might almost be taken to be the history of war itself, certainly the history of war in the Christian era. ... It is probably the case that many of the so-called camp fevers, and probably also a considerable proportion of the camp dysentery, of the wars of the sixteenth, seventeenth and eighteenth centuries were malarial in origin."[322] In British-occupied India the cocktail gin and tonic may have come about as a way of taking quinine, known for its antimalarial properties.[323]

Malaria was the most significant health hazard encountered by U.S. troops in the South Pacific during World War II, where about 500,000 men were infected.[324] According to Joseph Patrick Byrne, "Sixty thousand American soldiers died of malaria during the African and South Pacific campaigns."[325]

Significant financial investments have been made to procure existing and create new antimalarial agents. During World War I and World War II, inconsistent supplies of the natural antimalaria drugs cinchona bark and quinine prompted substantial funding into research and development of other drugs and vaccines. American military organisations conducting such research initiatives include the Navy Medical Research Center, Walter Reed Army Institute of Research, and the U.S. Army Medical Research Institute of Infectious Diseases of the US Armed Forces.[326]

Additionally, initiatives have been founded such as Malaria Control in War Areas (MCWA), established in 1942, and its successor, the Communicable Disease Center (now known as the Centers for Disease Control and Prevention, or CDC) established in 1946. According to the CDC, MCWA "was established to control malaria around military training bases in the southern United States and its territories, where malaria was still problematic".[327]

Research

[edit]

The Malaria Eradication Research Agenda (malERA) initiative was a consultative process to identify which areas of research and development (R&D) must be addressed for worldwide eradication of malaria.[328][329]

Medications

[edit]

Malaria parasites contain apicoplasts, organelles related to the plastids found in plants, complete with their own genomes. These apicoplasts are thought to have originated through the endosymbiosis of algae and play a crucial role in various aspects of parasite metabolism, such as fatty acid biosynthesis. Over 400 proteins have been found to be produced by apicoplasts and these are now being investigated as possible targets for novel antimalarial drugs.[330]

With the onset of drug-resistant Plasmodium parasites, new strategies are being developed to combat the widespread disease. One such approach lies in the introduction of synthetic pyridoxal-amino acid adducts, which are taken up by the parasite and ultimately interfere with its ability to create several essential B vitamins.[331][332] Antimalarial drugs using synthetic metal-based complexes are attracting research interest.[333][334]

  • (+)-SJ733: Part of a wider class of experimental drugs called spiroindolone. It inhibits the ATP4 protein of infected red blood cells that cause the cells to shrink and become rigid like the aging cells. This triggers the immune system to eliminate the infected cells from the system as demonstrated in a mouse model. As of 2014, a Phase 1 clinical trial to assess the safety profile in human is planned by the Howard Hughes Medical Institute.[335]
  • NITD246 and NITD609: Also belonged to the class of spiroindolone and target the ATP4 protein.[335]

On the basis of molecular docking outcomes, compounds 3j, 4b, 4h, 4m were exhibited selectivity towards PfLDH. The post docking analysis displayed stable dynamic behavior of all the selected compounds compared to Chloroquine. The end state thermodynamics analysis stated 3j compound as a selective and potent PfLDH inhibitor.[336]

New targets

[edit]

Targeting Plasmodium liver-stage parasites selectively is emerging as an alternative strategy in the face of resistance to the latest frontline combination therapies against blood stages of the parasite.[337]

In research conducted in 2019, using experimental analysis with knockout (KO) mutants of Plasmodium berghei, the authors were able to identify genes that are potentially essential in the liver stage. Moreover, they generated a computational model to analyse pre–erytrocytic development and liver–stage metabolism. Combining both methods they identified seven metabolic subsystems that become essential compared to the blood stage. Some of these metabolic pathways are fatty acid synthesis and elongation, tricarboxylic acid, amino acid and heme metabolism among others.[337]

Specifically, they studied three subsystems: fatty acid synthesis and elongation, and amino sugar biosynthesis. For the first two pathways they demonstrated a clear dependence of the liver stage on its own fatty acid metabolism.[337]

They proved for the first time the critical role of amino sugar biosynthesis in the liver stage of P. berghei. The uptake of N–acetyl–glucosamine appears to be limited in the liver stage, being its synthesis needed for the parasite development.[337]

These findings and the computational model provide a basis for the design of antimalarial therapies targeting metabolic proteins.[337][338]

Genomic research

[edit]

The genome of Plasmodium falciparum was sequenced and published in the year 2002.[339]

A species of malaria plasmodium tends to have rather polymorphic antigens which can serve as immune system targets. Some searches of P. falciparum genes for hotspots of encoded variations found sections of genes that when tested proved to encode for antigens. When such antigens are use for vaccine targets a strain of plasmodium with a different allele for the antigen can sometimes escape the immune response stimulated by the vaccine.[340]

Two related viruses, MaRNAV-1 and MaRNAV-2 in Plasmodium vivax and in avian Leucocytozoon respectively, were found through RNA-Sequencing of blood. The finding of a virus infecting a human malaria plasmodium is a first discovery of its kind. It should lead to better understanding of malaria biology.[341]

Other

[edit]

A non-chemical vector control strategy involves genetic manipulation of malaria mosquitoes. Advances in genetic engineering technologies make it possible to introduce foreign DNA into the mosquito genome and either decrease the lifespan of the mosquito, or make it more resistant to the malaria parasite. Sterile insect technique is a genetic control method whereby large numbers of sterile male mosquitoes are reared and released. Mating with wild females reduces the wild population in the subsequent generation; repeated releases eventually eliminate the target population.[90]

Genomics is central to malaria research. With the sequencing of P. falciparum, one of its vectors Anopheles gambiae, and the human genome, the genetics of all three organisms in the malaria life cycle can be studied.[342] Another new application of genetic technology is the ability to produce genetically modified mosquitoes that do not transmit malaria, potentially allowing biological control of malaria transmission.[343]

In one study, a genetically modified strain of Anopheles stephensi was created that no longer supported malaria transmission, and this resistance was passed down to mosquito offspring.[344]

Gene drive is a technique for changing wild populations, for instance to combat or eliminate insects so they cannot transmit diseases (in particular mosquitoes in the cases of malaria,[345] zika,[346] dengue and yellow fever).[293]

In a study conducted in 2015, researchers observed a specific interaction between malaria and co-infection with the nematode Nippostrongylus brasiliensis, a pulmonary migrating helminth, in mice.[347] The co-infection was found to reduce the virulence of the Plasmodium parasite, the causative agent of malaria. This reduction was attributed to the nematode infection causing increased destruction of erythrocytes, or red blood cells. Given that Plasmodium has a predilection for older host erythrocytes, the increased erythrocyte destruction and ensuing erythropoiesis result in a predominantly younger erythrocyte population, which in turn leads to a decrease in Plasmodium population.[347] Notably, this effect appears to be largely independent of the host's immune control of Plasmodium.

Finally, a review article published in December 2020 noted a correlation between malaria-endemic regions and COVID-19 case fatality rates.[348] The study found that, on average, regions where malaria is endemic reported lower COVID-19 case fatality rates compared to regions without endemic malaria.

In 2017, a bacterial strain of the genus Serratia was genetically modified to prevent malaria in mosquitos[349][350] and in 2023, it has been reported that the bacterium Delftia tsuruhatensis naturally prevents the development of malaria by secreting a molecule called Harmane.[351][352][353]

Other avenue that can contribute to understanding of malaria transmission, is the source of meal for the vector when they have the parasites. Its known that plant sugars are the primary source of nutrients for survival of adult mosquitoes,[354] therefore utilising this link for management of the vector will contribute in mitigating malaria transmission.[355][356]

Other animals

[edit]

While none of the main four species of malaria parasite that cause human infections are known to have animal reservoirs,[357] P. knowlesi is known to regularly infect both humans and non-human primates.[50] Other non-human primate malarias (particularly P. cynomolgi and P. simium) have also been found to have spilled over into humans.[358] Nearly 200 Plasmodium species have been identified that infect birds, reptiles, and other mammals,[359] and about 30 of them naturally infect non-human primates.[360] Some malaria parasites of non-human primates (NHP) serve as model organisms for human malarial parasites, such as P. coatneyi (a model for P. falciparum) and P. cynomolgi (a model for P. vivax). Diagnostic techniques used to detect parasites in NHP are similar to those employed for humans.[361] Malaria parasites that infect rodents are widely used as models in research, such as P. berghei.[362] Avian malaria primarily affects species of the order Passeriformes, and poses a substantial threat to birds of Hawaii, the Galapagos, and other archipelagoes. The parasite P. relictum is known to play a role in limiting the distribution and abundance of endemic Hawaiian birds. Global warming is expected to increase the prevalence and global distribution of avian malaria, as elevated temperatures provide optimal conditions for parasite reproduction.[363]

References

[edit]
  1. ^ a b c d e f g h i j k l m n o Caraballo H, King K (May 2014). "Emergency department management of mosquito-borne illness: malaria, dengue, and West Nile virus". Emergency Medicine Practice. 16 (5): 1–23, quiz 23–24. PMID 25207355. S2CID 23716674. Archived from the original on 2016-08-01.
  2. ^ "Malaria". Mayo Clinic. Archived from the original on 2022-07-02. Retrieved 2022-06-04.
  3. ^ a b c d e f g h i j k "Malaria Fact sheet N°94". WHO. March 2014. Archived from the original on 3 September 2014. Retrieved 28 August 2014.
  4. ^ a b "CDC - Malaria - FAQs". 28 June 2023. Archived from the original on 13 May 2012. Retrieved 9 September 2017.
  5. ^ a b WHO (2023). World Malaria Report 2023. Switzerland: World Health Organization. ISBN 978-92-4-008617-3. Archived from the original on 2024-07-18. Retrieved 2024-07-22.
  6. ^ "Vector-borne diseases". www.who.int. Archived from the original on 2023-01-04. Retrieved 2022-04-24.
  7. ^ Dahalan FA, Churcher TS, Windbichler N, Lawniczak MK (November 2019). "The male mosquito contribution towards malaria transmission: Mating influences the Anopheles female midgut transcriptome and increases female susceptibility to human malaria parasites". PLOS Pathogens. 15 (11): e1008063. doi:10.1371/journal.ppat.1008063. PMC 6837289. PMID 31697788.
  8. ^ Basu S, Sahi PK (July 2017). "Malaria: An Update". Indian Journal of Pediatrics. 84 (7): 521–528. doi:10.1007/s12098-017-2332-2. PMID 28357581. S2CID 11461451.
  9. ^ "Fact sheet about malaria". www.who.int. Archived from the original on 2020-05-02. Retrieved 2024-05-10.
  10. ^ a b c d e "Fact sheet about malaria". www.who.int. Archived from the original on 2 May 2020. Retrieved 28 September 2023.
  11. ^ Dawes EJ, Churcher TS, Zhuang S, Sinden RE, Basáñez MG (October 2009). "Anopheles mortality is both age- and Plasmodium-density dependent: implications for malaria transmission". Malaria Journal. 8 (1): 228. doi:10.1186/1475-2875-8-228. PMC 2770541. PMID 19822012.
  12. ^ Walter K, John CC (February 2022). "Malaria". JAMA. 327 (6): 597. doi:10.1001/jama.2021.21468. PMID 35133414. S2CID 246651569.
  13. ^ a b "Fact sheet about malaria". www.who.int. Archived from the original on 2020-05-02. Retrieved 2024-02-19.
  14. ^ World Health Organization. "Global Technical Strategy for Malaria 2016-2030" (PDF). Archived (PDF) from the original on 2024-02-22. Retrieved 2024-02-19.
  15. ^ a b c d e f Nadjm B, Behrens RH (June 2012). "Malaria: an update for physicians". Infectious Disease Clinics of North America. 26 (2): 243–259. doi:10.1016/j.idc.2012.03.010. PMID 22632637.
  16. ^ a b c "WHO recommends R21/Matrix-M vaccine for malaria prevention in updated advice on immunization". 2 October 2023. Archived from the original on 3 October 2023. Retrieved 8 December 2023.
  17. ^ Rawat A, Roy M, Jyoti A, Kaushik S, Verma K, Srivastava VK (August 2021). "Cysteine proteases: Battling pathogenic parasitic protozoans with omnipresent enzymes". Microbiological Research. 249: 126784. doi:10.1016/j.micres.2021.126784. PMID 33989978. S2CID 234597200.
  18. ^ a b c d e WHO 2022, p. [page needed].
  19. ^ a b Guidelines for the treatment of malaria (2nd ed.). Geneva: World Health Organization. 2010. p. ix. ISBN 978-92-4-154792-5.
  20. ^ Baiden F, Malm KL, Binka F (2021). "Malaria". In Detels R, Karim QA, Baum F, Li L, Leyland AH (eds.). Oxford Textbook of Global Public Health. pp. 227–248. doi:10.1093/med/9780198816805.003.0073. ISBN 978-0-19-881680-5.
  21. ^ "World malaria report 2022". www.who.int. Archived from the original on 2024-01-30. Retrieved 2024-01-30.
  22. ^ a b c d e f g "Malaria in Africa". UNICEF DATA. Archived from the original on 2023-11-05. Retrieved 2023-11-02.
  23. ^ a b c d "Nearly every minute, a child under 5 dies of malaria". UNICEF. February 2023. Archived from the original on 2023-09-21. Retrieved 2023-09-10.
  24. ^ a b Gollin D, Zimmermann C (August 2007). Malaria: Disease Impacts and Long-Run Income Differences (PDF) (Report). Institute for the Study of Labor. Archived (PDF) from the original on 2016-03-18.
  25. ^ a b Worrall E, Basu S, Hanson K (October 2005). "Is malaria a disease of poverty? A review of the literature". Tropical Medicine & International Health. 10 (10): 1047–1059. doi:10.1111/j.1365-3156.2005.01476.x. PMID 16185240.
  26. ^ a b Greenwood BM, Bojang K, Whitty CJ, Targett GA (2005). "Malaria". The Lancet. 365 (9469): 1487–1498. doi:10.1016/S0140-6736(05)66420-3. PMID 15850634. S2CID 208987634.
  27. ^ Reiter P (1999). "From Shakespeare to Defoe: malaria in England in the Little Ice Age". Emerging Infectious Diseases. 6 (1): 1–11. doi:10.3201/eid0601.000101. PMC 2627969. PMID 10653562.
  28. ^ Sharpe S (1768). A view of the customs, manners, drama, &c. of Italy, as they are described in the Frusta letteraria; and in the Account of Italy in English, written by Mr. Baretti; compared with the Letters from Italy, written by Mr. Sharp. London: W. Nicoll.
  29. ^ Lindemann M (1999). Medicine and Society in Early Modern Europe. Cambridge University Press. p. 62. ISBN 978-0-521-42354-0. Archived from the original on 2023-01-13. Retrieved 2015-10-27.
  30. ^ Gratz NG (2006). The Vector- and Rodent-borne Diseases of Europe and North America: Their Distribution and Public Health Burden. Cambridge University Press. p. 33. ISBN 978-0-521-85447-4. Archived from the original on 2023-01-13. Retrieved 2015-10-27.
  31. ^ Webb 2008, p. [page needed].
  32. ^ Fairhurst RM, Wellems TE (2015). "Malaria (Plasmodium Species)". Mandell, Douglas, and Bennett's Principles and Practice of Infectious Diseases. pp. 3070–3090.e9. doi:10.1016/B978-1-4557-4801-3.00276-9. ISBN 978-1-4557-4801-3.
  33. ^ a b c d Despommier DD, Griffin DO, Gwadz RW, Hotez PJ, Knirsch CA (2019). "9. The Malarias". Parasitic Diseases (PDF) (7 ed.). New York: Parasites Without Borders. pp. 110–115. Archived (PDF) from the original on November 24, 2021. Retrieved November 24, 2021.
  34. ^ a b c d e Bartoloni A, Zammarchi L (2012). "Clinical aspects of uncomplicated and severe malaria". Mediterranean Journal of Hematology and Infectious Diseases. 4 (1): e2012026. doi:10.4084/MJHID.2012.026. PMC 3375727. PMID 22708041.
  35. ^ Beare NA, Taylor TE, Harding SP, Lewallen S, Molyneux ME (November 2006). "Malarial retinopathy: a newly established diagnostic sign in severe malaria". The American Journal of Tropical Medicine and Hygiene. 75 (5): 790–797. doi:10.4269/ajtmh.2006.75.790. PMC 2367432. PMID 17123967.
  36. ^ Ferri FF (2009). "Chapter 332. Protozoal infections". Ferri's Color Atlas and Text of Clinical Medicine. Elsevier Health Sciences. p. 1159. ISBN 978-1-4160-4919-7. Archived from the original on 2023-01-10. Retrieved 2015-10-27.
  37. ^ Khanna K (30 December 2021). "Microbial Origins of Body Odor". American Society for Microbiology.
  38. ^ a b Dormont L, Mulatier M, Carrasco D, Cohuet A (May 2021). "Mosquito Attractants". Journal of Chemical Ecology. 47 (4–5): 351–393. Bibcode:2021JCEco..47..351D. doi:10.1007/s10886-021-01261-2. PMID 33725235.
  39. ^ a b Taylor WR, Hanson J, Turner GD, White NJ, Dondorp AM (August 2012). "Respiratory manifestations of malaria". Chest. 142 (2): 492–505. doi:10.1378/chest.11-2655. PMID 22871759.
  40. ^ Korenromp EL, Williams BG, de Vlas SJ, Gouws E, Gilks CF, Ghys PD, et al. (September 2005). "Malaria attributable to the HIV-1 epidemic, sub-Saharan Africa". Emerging Infectious Diseases. 11 (9): 1410–1419. doi:10.3201/eid1109.050337. PMC 3310631. PMID 16229771.
  41. ^ Beare NA, Lewallen S, Taylor TE, Molyneux ME (March 2011). "Redefining cerebral malaria by including malaria retinopathy". Future Microbiology. 6 (3): 349–355. doi:10.2217/fmb.11.3. PMC 3139111. PMID 21449844.
  42. ^ Davidson's Principles and Practice of Medicine/21st/351
  43. ^ a b Hartman TK, Rogerson SJ, Fischer PR (2010). "The impact of maternal malaria on newborns". Annals of Tropical Paediatrics. 30 (4): 271–282. doi:10.1179/146532810X12858955921032. PMID 21118620. S2CID 25560090.
  44. ^ Rijken MJ, McGready R, Boel ME, Poespoprodjo R, Singh N, Syafruddin D, et al. (January 2012). "Malaria in pregnancy in the Asia-Pacific region". The Lancet Infectious Diseases. 12 (1): 75–88. doi:10.1016/S1473-3099(11)70315-2. PMID 22192132. Archived from the original on 2020-01-23. Retrieved 2019-07-05.
  45. ^ a b "Malaria - About Malaria - Disease". CDC-Centers for Disease Control and Prevention. 2022-03-22. Archived from the original on 2023-05-24. Retrieved 2022-04-28.
  46. ^ a b c d e f g h Ashley EA, Pyae Phyo A, Woodrow CJ (April 2018). "Malaria". The Lancet. 391 (10130): 1608–1621. doi:10.1016/S0140-6736(18)30324-6. PMID 29631781. S2CID 208791451.
  47. ^ a b Sarkar PK, Ahluwalia G, Vijayan VK, Talwar A (2009). "Critical care aspects of malaria". Journal of Intensive Care Medicine. 25 (2): 93–103. doi:10.1177/0885066609356052. PMID 20018606. S2CID 20941166.
  48. ^ Baird JK (January 2013). "Evidence and implications of mortality associated with acute Plasmodium vivax malaria". Clinical Microbiology Reviews. 26 (1): 36–57. doi:10.1128/CMR.00074-12. PMC 3553673. PMID 23297258.
  49. ^ Arnott A, Barry AE, Reeder JC (January 2012). "Understanding the population genetics of Plasmodium vivax is essential for malaria control and elimination". Malaria Journal. 11: 14. doi:10.1186/1475-2875-11-14. PMC 3298510. PMID 22233585.
  50. ^ a b Collins WE (2012). "Plasmodium knowlesi: a malaria parasite of monkeys and humans". Annual Review of Entomology. 57: 107–121. doi:10.1146/annurev-ento-121510-133540. PMID 22149265. Archived from the original on 2020-09-23. Retrieved 2019-07-05.
  51. ^ Collins WE, Barnwell JW (April 2009). "Plasmodium knowlesi: finally being recognized". The Journal of Infectious Diseases. 199 (8): 1107–1108. doi:10.1086/597415. PMID 19284287.
  52. ^ "CDC - Malaria - FAQs". www.cdc.gov. 2023-06-28. Archived from the original on 2012-05-13. Retrieved 2023-10-30. Only Anopheles mosquitoes can transmit malaria and they must have been infected through a previous blood meal taken from an infected person. When a mosquito bites an infected person, a small amount of blood is taken in which contains microscopic malaria parasites. About 1 week later, when the mosquito takes its next blood meal, these parasites mix with the mosquito's saliva and are injected into the person being bitten.
  53. ^ "CDC - Malaria - About Malaria - Biology". www.cdc.gov. 2020-07-16. Archived from the original on 2021-01-27. Retrieved 2023-10-30. Thus the infected mosquito carries the disease from one human to another (acting as a "vector"), while infected humans transmit the parasite to the mosquito, In contrast to the human host, the mosquito vector does not suffer from the presence of the parasites.
  54. ^ Ménard R, Tavares J, Cockburn I, Markus M, Zavala F, Amino R (October 2013). "Looking under the skin: the first steps in malarial infection and immunity". Nature Reviews. Microbiology. 11 (10): 701–712. doi:10.1038/nrmicro3111. PMID 24037451.
  55. ^ a b c d e f Cowman AF, Healer J, Marapana D, Marsh K (October 2016). "Malaria: Biology and Disease". Cell. 167 (3): 610–624. doi:10.1016/j.cell.2016.07.055. PMID 27768886. S2CID 2524633.
  56. ^ Arrow KJ, Panosian C, Gelband H (2004). Saving Lives, Buying Time: Economics of Malaria Drugs in an Age of Resistance. National Academies Press. p. 141. ISBN 978-0-309-09218-0.
  57. ^ Goldman JG. "Malaria Mosquitoes Are Biting before Bed-Net Time". Scientific American. Archived from the original on 2023-05-29. Retrieved 2023-05-29.
  58. ^ Owusu-Ofori AK, Parry C, Bates I (November 2010). "Transfusion-transmitted malaria in countries where malaria is endemic: a review of the literature from sub-Saharan Africa". Clinical Infectious Diseases. 51 (10): 1192–1198. doi:10.1086/656806. PMID 20929356.
  59. ^ WHO 2015, p. 4.
  60. ^ Markus MB (2011). "Malaria: origin of the term 'hypnozoite'". Journal of the History of Biology. 44 (4): 781–786. doi:10.1007/s10739-010-9239-3. PMID 20665090. S2CID 1727294.
  61. ^ a b c White NJ (October 2011). "Determinants of relapse periodicity in Plasmodium vivax malaria". Malaria Journal. 10: 297. doi:10.1186/1475-2875-10-297. PMC 3228849. PMID 21989376.
  62. ^ WHO 2015, p. 41.
  63. ^ a b Tran TM, Samal B, Kirkness E, Crompton PD (June 2012). "Systems immunology of human malaria". Trends in Parasitology. 28 (6): 248–257. doi:10.1016/j.pt.2012.03.006. PMC 3361535. PMID 22592005.
  64. ^ a b c Bledsoe GH (December 2005). "Malaria primer for clinicians in the United States". Southern Medical Journal. 98 (12): 1197–204, quiz 1205, 1230. doi:10.1097/01.smj.0000189904.50838.eb. PMID 16440920. S2CID 30660702.
  65. ^ Vaughan AM, Aly AS, Kappe SH (September 2008). "Malaria parasite pre-erythrocytic stage infection: gliding and hiding". Cell Host & Microbe. 4 (3): 209–218. doi:10.1016/j.chom.2008.08.010. PMC 2610487. PMID 18779047.
  66. ^ Richter J, Franken G, Mehlhorn H, Labisch A, Häussinger D (November 2010). "What is the evidence for the existence of Plasmodium ovale hypnozoites?". Parasitology Research. 107 (6): 1285–1290. doi:10.1007/s00436-010-2071-z. PMID 20922429. S2CID 2044783.
  67. ^ Tilley L, Dixon MW, Kirk K (June 2011). "The Plasmodium falciparum-infected red blood cell". The International Journal of Biochemistry & Cell Biology. 43 (6): 839–842. doi:10.1016/j.biocel.2011.03.012. PMID 21458590.
  68. ^ Mens PF, Bojtor EC, Schallig HD (October 2010). "Molecular interactions in the placenta during malaria infection". European Journal of Obstetrics, Gynecology, and Reproductive Biology. 152 (2): 126–132. doi:10.1016/j.ejogrb.2010.05.013. PMID 20933151.
  69. ^ Rénia L, Howland SW, Claser C, Charlotte Gruner A, Suwanarusk R, Hui Teo T, et al. (2012). "Cerebral malaria: mysteries at the blood-brain barrier". Virulence. 3 (2): 193–201. doi:10.4161/viru.19013. PMC 3396698. PMID 22460644.
  70. ^ Pierron D, Heiske M, Razafindrazaka H, Pereda-Loth V, Sanchez J, Alva O, et al. (March 2018). "Strong selection during the last millennium for African ancestry in the admixed population of Madagascar". Nature Communications. 9 (1): 932. Bibcode:2018NatCo...9..932P. doi:10.1038/s41467-018-03342-5. PMC 5834599. PMID 29500350.
  71. ^ Kwiatkowski DP (August 2005). "How malaria has affected the human genome and what human genetics can teach us about malaria". American Journal of Human Genetics. 77 (2): 171–192. doi:10.1086/432519. PMC 1224522. PMID 16001361.
  72. ^ a b Hedrick PW (October 2011). "Population genetics of malaria resistance in humans". Heredity. 107 (4): 283–304. doi:10.1038/hdy.2011.16. PMC 3182497. PMID 21427751.
  73. ^ Weatherall DJ (May 2008). "Genetic variation and susceptibility to infection: the red cell and malaria". British Journal of Haematology. 141 (3): 276–286. doi:10.1111/j.1365-2141.2008.07085.x. PMID 18410566.
  74. ^ a b Bhalla A, Suri V, Singh V (2006). "Malarial hepatopathy". Journal of Postgraduate Medicine. 52 (4): 315–320. PMID 17102560. Archived from the original on 2013-09-21.
  75. ^ Cunnington AJ, Riley EM (April 2010). "Suppression of vaccine responses by malaria: insignificant or overlooked?". Expert Review of Vaccines. 9 (4): 409–429. doi:10.1586/erv.10.16. PMID 20370551.
  76. ^ a b c d e f g h i j k l "5.1 Diagnosing Malaria (2015)". WHO Guidelines for Malaria. World Health Organization. 13 July 2021. Archived from the original on 18 March 2023. Retrieved 28 November 2021.
  77. ^ WHO 2015, p. 73.
  78. ^ WHO 2015, p. 3.
  79. ^ a b "Fact sheet about Malaria". www.who.int. Archived from the original on 2 May 2020. Retrieved 6 May 2020.
  80. ^ World Health Organization (1958). "Malaria" (PDF). The First Ten Years of the World Health Organization. World Health Organization. pp. 172–87. Archived (PDF) from the original on 2011-07-08.
  81. ^ Sabot O, Cohen JM, Hsiang MS, Kahn JG, Basu S, Tang L, et al. (November 2010). "Costs and financial feasibility of malaria elimination". The Lancet. 376 (9752): 1604–1615. doi:10.1016/S0140-6736(10)61355-4. PMC 3044845. PMID 21035839.
  82. ^ "From 30 million cases to zero: China is certified malaria-free by WHO". www.who.int. Archived from the original on 2023-03-14. Retrieved 2022-08-11.
  83. ^ "Countries and territories certified malaria-free by WHO". www.who.int. Archived from the original on 2024-01-30. Retrieved 2024-01-30.
  84. ^ Athuman M, Kabanywanyi AM, Rohwer AC (January 2015). "Intermittent preventive antimalarial treatment for children with anaemia". The Cochrane Database of Systematic Reviews. 1 (1): CD010767. doi:10.1002/14651858.CD010767.pub2. PMC 4447115. PMID 25582096.
  85. ^ a b Kajfasz P (2009). "Malaria prevention". International Maritime Health. 60 (1–2): 67–70. PMID 20205131. Archived from the original on 2017-08-30.
  86. ^ Maia MF, Kliner M, Richardson M, Lengeler C, Moore SJ, et al. (Cochrane Infectious Diseases Group) (February 2018). "Mosquito repellents for malaria prevention". The Cochrane Database of Systematic Reviews. 2018 (2): CD011595. doi:10.1002/14651858.CD011595.pub2. PMC 5815492. PMID 29405263.
  87. ^ a b c d e Fox T, Furnival-Adams J, Chaplin M, Napier M, Olanga EA (October 2022). "House modifications for preventing malaria". The Cochrane Database of Systematic Reviews. 2022 (10): CD013398. doi:10.1002/14651858.CD013398.pub4. PMC 9536247. PMID 36200610.
  88. ^ Pryce J, Richardson M, Lengeler C (November 2018). "Insecticide-treated nets for preventing malaria". The Cochrane Database of Systematic Reviews. 11 (11): CD000363. doi:10.1002/14651858.CD000363.pub3. PMC 6418392. PMID 30398672.
  89. ^ Pluess B, Tanser FC, Lengeler C, Sharp BL (April 2010). Lengeler C (ed.). "Indoor residual spraying for preventing malaria". The Cochrane Database of Systematic Reviews. 2010 (4): CD006657. doi:10.1002/14651858.CD006657.pub2. PMC 6532743. PMID 20393950.
  90. ^ a b Raghavendra K, Barik TK, Reddy BP, Sharma P, Dash AP (April 2011). "Malaria vector control: from past to future". Parasitology Research. 108 (4): 757–779. doi:10.1007/s00436-010-2232-0. PMID 21229263. S2CID 1422449.
  91. ^ a b c Howitt P, Darzi A, Yang GZ, Ashrafian H, Atun R, Barlow J, et al. (August 2012). "Technologies for global health". The Lancet. 380 (9840): 507–535. doi:10.1016/S0140-6736(12)61127-1. PMID 22857974. S2CID 15311210.
  92. ^ a b "Malaria in Africa". UNICEF DATA. Archived from the original on 2023-11-05. Retrieved 2023-10-31.
  93. ^ Noor AM, Mutheu JJ, Tatem AJ, Hay SI, Snow RW (January 2009). "Insecticide-treated net coverage in Africa: mapping progress in 2000-07". The Lancet. 373 (9657): 58–67. Bibcode:2009Lanc..373...58N. doi:10.1016/S0140-6736(08)61596-2. PMC 2652031. PMID 19019422.
  94. ^ a b UNICEF (September 2015). Achieving the malaria MDG target: reversing the incidence of malaria 2000–2015 (PDF). WHO. ISBN 978-92-4-150944-2. Archived (PDF) from the original on 5 January 2016. Retrieved 26 December 2015.
  95. ^ Schlagenhauf-Lawlor 2008, p. 215
  96. ^ Instructions for treatment and use of insecticide-treated mosquito nets. World Health Organization. 2002. p. 34. hdl:10665/67573.
  97. ^ Gamble C, Ekwaru JP, ter Kuile FO, et al. (Cochrane Infectious Diseases Group) (April 2006). "Insecticide-treated nets for preventing malaria in pregnancy". The Cochrane Database of Systematic Reviews. 2006 (2): CD003755. doi:10.1002/14651858.CD003755.pub2. PMC 6532581. PMID 16625591.
  98. ^ a b Gleave K, Lissenden N, Chaplin M, Choi L, Ranson H (May 2021). "Piperonyl butoxide (PBO) combined with pyrethroids in insecticide-treated nets to prevent malaria in Africa". The Cochrane Database of Systematic Reviews. 5 (5): CD012776. doi:10.1002/14651858.CD012776.pub3. PMC 8142305. PMID 34027998.
  99. ^ Enayati A, Hemingway J (2010). "Malaria management: past, present, and future". Annual Review of Entomology. 55: 569–591. doi:10.1146/annurev-ento-112408-085423. PMID 19754246.
  100. ^ Indoor residual spraying : use of indoor residual spraying for scaling up global malaria control and elimination : WHO position statement. World Health Organization. 2006. hdl:10665/69386.
  101. ^ a b van den Berg H (November 2009). "Global status of DDT and its alternatives for use in vector control to prevent disease". Environmental Health Perspectives. 117 (11): 1656–1663. doi:10.1289/ehp.0900785. PMC 2801202. PMID 20049114.
  102. ^ Pates H, Curtis C (2005). "Mosquito behavior and vector control". Annual Review of Entomology. 50: 53–70. doi:10.1146/annurev.ento.50.071803.130439. PMID 15355233.
  103. ^ a b Pryce J, Medley N, Choi L (January 2022). "Indoor residual spraying for preventing malaria in communities using insecticide-treated nets". The Cochrane Database of Systematic Reviews. 1 (1): CD012688. doi:10.1002/14651858.CD012688.pub3. PMC 8763033. PMID 35038163.
  104. ^ Tusting LS, Ippolito MM, Willey BA, Kleinschmidt I, Dorsey G, Gosling RD, et al. (June 2015). "The evidence for improving housing to reduce malaria: a systematic review and meta-analysis". Malaria Journal. 14 (1): 209. doi:10.1186/s12936-015-0724-1. PMC 4460721. PMID 26055986.
  105. ^ a b "WHO Guidelines for Malaria" (PDF). WHO Guidelines for Malaria. October 16, 2023. Retrieved August 1, 2024.
  106. ^ a b c Nalinya S, Musoke D, Deane K (February 2022). "Malaria prevention interventions beyond long-lasting insecticidal nets and indoor residual spraying in low- and middle-income countries: a scoping review". Malaria Journal. 21 (1): 31. doi:10.1186/s12936-022-04052-6. PMC 8812253. PMID 35109848.
  107. ^ a b "Grant: In2Care EaveTubes". USAID DIV Impacts. August 1, 2024. Retrieved August 1, 2024.
  108. ^ "Lethal house lures". www.who.int. Retrieved 2024-08-01.
  109. ^ Webster JP, Molyneux DH, Hotez PJ, Fenwick A (2014). "The contribution of mass drug administration to global health: past, present and future". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 369 (1645): 20130434. doi:10.1098/rstb.2013.0434. PMC 4024227. PMID 24821920.
  110. ^ de Souza DK, Thomas R, Bradley J, Leyrat C, Boakye DA, Okebe J, et al. (Cochrane Infectious Diseases Group) (June 2021). "Ivermectin treatment in humans for reducing malaria transmission". The Cochrane Database of Systematic Reviews. 2021 (6): CD013117. doi:10.1002/14651858.CD013117.pub2. PMC 8240090. PMID 34184757.
  111. ^ Kamiya T (December 2022). "Targeting malaria parasites inside mosquitoes: ecoevolutionary consequences". Trends in Parasitology. 38 (12): 1031–1040. doi:10.1016/j.pt.2022.09.004. PMC 9815470. PMID 36209032.
  112. ^ Li Q, Kozar MP, Shearer TW, Xie LH, Lin AJ, Smith KS, et al. (2007). "Pharmacokinetics, Safety, and Hydrolysis of Oral Pyrroloquinazolinediamines Administered in Single and Multiple Doses in Rats". Antimicrobial Agents and Chemotherapy. 51 (8): 2898–2904. doi:10.1128/AAC.00932-06. ISSN 0066-4804. PMC 1932520. PMID 17562804.
  113. ^ Delves M, Plouffe D, Scheurer C, Meister S, Wittlin S, Winzeler EA, et al. (2012-02-21). "The Activities of Current Antimalarial Drugs on the Life Cycle Stages of Plasmodium: A Comparative Study with Human and Rodent Parasites". PLOS Medicine. 9 (2): e1001169. doi:10.1371/journal.pmed.1001169. ISSN 1549-1676. PMC 3283556. PMID 22363211.
  114. ^ Martello E, Yogeswaran G, Reithinger R, Leonardi-Bee J (November 2022). "Mosquito aquatic habitat modification and manipulation interventions to control malaria". The Cochrane Database of Systematic Reviews. 2022 (11): CD008923. doi:10.1002/14651858.CD008923.pub3. PMC 9651131. PMID 36367444.
  115. ^ Enayati AA, Hemingway J, Garner P (April 2007). Enayati A (ed.). "Electronic mosquito repellents for preventing mosquito bites and malaria infection". The Cochrane Database of Systematic Reviews. 2007 (2): CD005434. doi:10.1002/14651858.CD005434.pub2. PMC 6532582. PMID 17443590.
  116. ^ Pryce J, Choi L, Richardson M, Malone D, et al. (Cochrane Infectious Diseases Group) (November 2018). "Insecticide space spraying for preventing malaria transmission". The Cochrane Database of Systematic Reviews. 11 (11): CD012689. doi:10.1002/14651858.CD012689.pub2. PMC 6516806. PMID 30388303.
  117. ^ Choi L, Majambere S, Wilson AL, et al. (Cochrane Infectious Diseases Group) (August 2019). "Larviciding to prevent malaria transmission". The Cochrane Database of Systematic Reviews. 8 (8): CD012736. doi:10.1002/14651858.CD012736.pub2. PMC 6699674. PMID 31425624.
  118. ^ Walshe DP, Garner P, Adeel AA, Pyke GH, Burkot TR, et al. (Cochrane Infectious Diseases Group) (December 2017). "Larvivorous fish for preventing malaria transmission". The Cochrane Database of Systematic Reviews. 2017 (12): CD008090. doi:10.1002/14651858.CD008090.pub3. PMC 5741835. PMID 29226959.
  119. ^ a b Tickell-Painter M, Maayan N, Saunders R, Pace C, Sinclair D (October 2017). "Mefloquine for preventing malaria during travel to endemic areas". The Cochrane Database of Systematic Reviews. 2017 (10): CD006491. doi:10.1002/14651858.CD006491.pub4. PMC 5686653. PMID 29083100.
  120. ^ "Drug resistance in the Malaria Endemic World". Centers for Disease Control and Prevention. Archived from the original on 9 December 2017. Retrieved 4 January 2018.
  121. ^ a b Shah MP, Hwang J, Choi L, Lindblade KA, Kachur SP, Desai M (September 2021). "Mass drug administration for malaria". The Cochrane Database of Systematic Reviews. 2021 (9): CD008846. doi:10.1002/14651858.CD008846.pub3. PMC 8479726. PMID 34585740.
  122. ^ Freedman DO (August 2008). "Clinical practice. Malaria prevention in short-term travelers". The New England Journal of Medicine. 359 (6): 603–612. doi:10.1056/NEJMcp0803572. PMID 18687641.
  123. ^ Fernando SD, Rodrigo C, Rajapakse S (April 2011). "Chemoprophylaxis in malaria: drugs, evidence of efficacy and costs". Asian Pacific Journal of Tropical Medicine. 4 (4): 330–336. doi:10.1016/S1995-7645(11)60098-9. PMID 21771482.
  124. ^ Radeva-Petrova D, Kayentao K, ter Kuile FO, Sinclair D, Garner P (October 2014). "Drugs for preventing malaria in pregnant women in endemic areas: any drug regimen versus placebo or no treatment". The Cochrane Database of Systematic Reviews. 2014 (10): CD000169. doi:10.1002/14651858.CD000169.pub3. PMC 4498495. PMID 25300703.
  125. ^ Turschner S, Efferth T (February 2009). "Drug resistance in Plasmodium: natural products in the fight against malaria". Mini Reviews in Medicinal Chemistry. 9 (2): 206–2124. doi:10.2174/138955709787316074. PMID 19200025.
  126. ^ Esu EB, Oringanje C, Meremikwu MM (July 2021). "Intermittent preventive treatment for malaria in infants". The Cochrane Database of Systematic Reviews. 2021 (7): CD011525. doi:10.1002/14651858.CD011525.pub3. PMC 8406727. PMID 34273901.
  127. ^ González R, Pons-Duran C, Piqueras M, Aponte JJ, Ter Kuile FO, Menéndez C, et al. (Cochrane Infectious Diseases Group) (November 2018). "Mefloquine for preventing malaria in pregnant women". The Cochrane Database of Systematic Reviews. 11 (11): CD011444. doi:10.1002/14651858.CD011444.pub3. PMC 6517148. PMID 30480761.
  128. ^ Mathanga DP, Uthman OA, Chinkhumba J, et al. (Cochrane Infectious Diseases Group) (October 2011). "Intermittent preventive treatment regimens for malaria in HIV-positive pregnant women". The Cochrane Database of Systematic Reviews. 2011 (10): CD006689. doi:10.1002/14651858.CD006689.pub2. PMC 6532702. PMID 21975756.
  129. ^ Palmer J. "WHO gives indoor use of DDT a clean bill of health for controlling malaria". WHO. Archived from the original on 2012-10-22.
  130. ^ Vanderberg JP (January 2009). "Reflections on early malaria vaccine studies, the first successful human malaria vaccination, and beyond". Vaccine. 27 (1): 2–9. doi:10.1016/j.vaccine.2008.10.028. PMC 2637529. PMID 18973784.
  131. ^ "World Malaria Report 2013" (PDF). World Health Organization. Retrieved 13 February 2014.
  132. ^ Walsh F (24 July 2015). "Malaria vaccine gets 'green light'". BBC News Online. Archived from the original on 21 December 2016.
  133. ^ a b WHO 2020, p. [page needed].
  134. ^ Mendis K (September 2019). "Eliminating malaria should not be the end of vigilance". Nature. 573 (7772): 7. Bibcode:2019Natur.573....7M. doi:10.1038/d41586-019-02598-1. PMID 31485061.
  135. ^ World Health Organization (March 2020). "Q&A on the malaria vaccine implementation programme (MVIP)". WHO. Archived from the original on 13 May 2020. Retrieved 6 May 2020.
  136. ^ Abuga KM, Jones-Warner W, Hafalla JC (February 2021). "Immune responses to malaria pre-erythrocytic stages: Implications for vaccine development". Parasite Immunology. 43 (2): e12795. doi:10.1111/pim.12795. PMC 7612353. PMID 32981095.
  137. ^ Hill AV (October 2011). "Vaccines against malaria". Philosophical Transactions of the Royal Society of London. Series B, Biological Sciences. 366 (1579): 2806–2814. doi:10.1098/rstb.2011.0091. PMC 3146776. PMID 21893544.
  138. ^ Crompton PD, Pierce SK, Miller LH (December 2010). "Advances and challenges in malaria vaccine development". The Journal of Clinical Investigation. 120 (12): 4168–4178. doi:10.1172/JCI44423. PMC 2994342. PMID 21123952.
  139. ^ Graves P, Gelband H (October 2006). Graves PM (ed.). "Vaccines for preventing malaria (blood-stage)". The Cochrane Database of Systematic Reviews. 2006 (4): CD006199. doi:10.1002/14651858.CD006199. PMC 6532641. PMID 17054281.
  140. ^ Graves P, Gelband H (April 2006). Graves PM (ed.). "Vaccines for preventing malaria (SPf66)". The Cochrane Database of Systematic Reviews. 2006 (2): CD005966. doi:10.1002/14651858.CD005966. PMC 6532709. PMID 16625647.
  141. ^ "Malaria vaccine: WHO position paper-January 2016" (PDF). Relevé Épidémiologique Hebdomadaire. 91 (4): 33–51. January 2016. PMID 26829826. Archived from the original (PDF) on 2020-04-23.
  142. ^ Datoo MS, Natama MH, Somé A, Traoré O, Rouamba T, Bellamy D, et al. (May 2021). "Efficacy of a low-dose candidate malaria vaccine, R21 in adjuvant Matrix-M, with seasonal administration to children in Burkina Faso: a randomised controlled trial". The Lancet. 397 (10287): 1809–1818. doi:10.1016/S0140-6736(21)00943-0. PMC 8121760. PMID 33964223. SSRN 3830681.
  143. ^ Malaria vaccine becomes first to achieve WHO-specified 75% efficacy goal Archived 2021-04-23 at the Wayback Machine, News Release 23 April 2021, University of Oxford
  144. ^ "Home". Archived from the original on 2023-08-03. Retrieved 2023-08-03.
  145. ^ "VacZine Analytics | Our products - MarketVIEW: Travel vaccines segment report". Archived from the original on 2023-08-03. Retrieved 2023-08-03.
  146. ^ Lalloo DG, Olukoya P, Olliaro P (December 2006). "Malaria in adolescence: burden of disease, consequences, and opportunities for intervention". The Lancet Infectious Diseases. 6 (12): 780–793. doi:10.1016/S1473-3099(06)70655-7. PMID 17123898.
  147. ^ Mehlhorn H, ed. (2016). "Disease Control, Methods". Encyclopedia of Parasitology. pp. 740–745. doi:10.1007/978-3-662-43978-4_921. ISBN 978-3-662-43977-7.
  148. ^ Bardají A, Bassat Q, Alonso PL, Menéndez C (August 2012). "Intermittent preventive treatment of malaria in pregnant women and infants: making best use of the available evidence". Expert Opinion on Pharmacotherapy. 13 (12): 1719–1736. doi:10.1517/14656566.2012.703651. PMID 22775553. S2CID 25024561.
  149. ^ Meremikwu MM, Donegan S, Sinclair D, Esu E, Oringanje C (February 2012). Meremikwu MM (ed.). "Intermittent preventive treatment for malaria in children living in areas with seasonal transmission". The Cochrane Database of Systematic Reviews. 2012 (2): CD003756. doi:10.1002/14651858.CD003756.pub4. PMC 6532713. PMID 22336792.
  150. ^ Hanboonkunupakarn B, White NJ (February 2022). "Advances and roadblocks in the treatment of malaria". British Journal of Clinical Pharmacology. 88 (2): 374–382. doi:10.1111/bcp.14474. PMC 9437935. PMID 32656850. S2CID 220502723.
  151. ^ Greenwood B (January 2004). "The use of anti-malarial drugs to prevent malaria in the population of malaria-endemic areas". The American Journal of Tropical Medicine and Hygiene. 70 (1): 1–7. doi:10.4269/ajtmh.2004.70.1. PMID 14971690.
  152. ^ Meremikwu MM, Odigwe CC, Akudo Nwagbara B, Udoh EE (September 2012). Meremikwu MM (ed.). "Antipyretic measures for treating fever in malaria". The Cochrane Database of Systematic Reviews. 2012 (9): CD002151. doi:10.1002/14651858.CD002151.pub2. PMC 6532580. PMID 22972057.
  153. ^ Okwundu CI, Nagpal S, Musekiwa A, Sinclair D (May 2013). "Home- or community-based programmes for treating malaria". The Cochrane Database of Systematic Reviews. 2013 (5): CD009527. doi:10.1002/14651858.CD009527.pub2. PMC 6532579. PMID 23728693.
  154. ^ "Malaria-Malaria - Diagnosis & treatment". Mayo Clinic. 9 February 2023.
  155. ^ McIntosh HM, Olliaro P, et al. (Cochrane Infectious Diseases Group) (1999-04-26). "Artemisinin derivatives for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 1999 (2): CD000256. doi:10.1002/14651858.CD000256. PMC 6532741. PMID 10796519.
  156. ^ Pousibet-Puerto J, Salas-Coronas J, Sánchez-Crespo A, Molina-Arrebola MA, Soriano-Pérez MJ, Giménez-López MJ, et al. (July 2016). "Impact of using artemisinin-based combination therapy (ACT) in the treatment of uncomplicated malaria from Plasmodium falciparum in a non-endemic zone". Malaria Journal. 15 (1): 339. doi:10.1186/s12936-016-1408-1. PMC 4930579. PMID 27368160. S2CID 18043747.
  157. ^ Kokwaro G (October 2009). "Ongoing challenges in the management of malaria". Malaria Journal. 8 (Suppl 1): S2. doi:10.1186/1475-2875-8-S1-S2. PMC 2760237. PMID 19818169.
  158. ^ Omari AA, Gamble C, Garner P, et al. (Cochrane Infectious Diseases Group) (April 2006). "Artemether-lumefantrine (four-dose regimen) for treating uncomplicated falciparum malaria". The Cochrane Database of Systematic Reviews. 2006 (2): CD005965. doi:10.1002/14651858.CD005965. PMC 6532603. PMID 16625646.
  159. ^ Omari AA, Gamble C, Garner P, et al. (Cochrane Infectious Diseases Group) (October 2005). "Artemether-lumefantrine (six-dose regimen) for treating uncomplicated falciparum malaria". The Cochrane Database of Systematic Reviews. 2005 (4): CD005564. doi:10.1002/14651858.CD005564. PMC 6532733. PMID 16235412.
  160. ^ WHO 2015, p. 9.
  161. ^ Keating GM (May 2012). "Dihydroartemisinin/Piperaquine: a review of its use in the treatment of uncomplicated Plasmodium falciparum malaria". Drugs. 72 (7): 937–961. doi:10.2165/11203910-000000000-00000. PMID 22515619. S2CID 209172100.
  162. ^ Sinclair D, Zani B, Donegan S, Olliaro P, Garner P, et al. (Cochrane Infectious Diseases Group) (July 2009). "Artemisinin-based combination therapy for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2009 (3): CD007483. doi:10.1002/14651858.CD007483.pub2. PMC 6532584. PMID 19588433.
  163. ^ Isba R, Zani B, Gathu M, Sinclair D, et al. (Cochrane Infectious Diseases Group) (February 2015). "Artemisinin-naphthoquine for treating uncomplicated Plasmodium falciparum malaria". The Cochrane Database of Systematic Reviews. 2015 (2): CD011547. doi:10.1002/14651858.CD011547. PMC 4453860. PMID 25702785.
  164. ^ Bukirwa H, Orton L, et al. (Cochrane Infectious Diseases Group) (October 2005). "Artesunate plus mefloquine versus mefloquine for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2005 (4): CD004531. doi:10.1002/14651858.CD004531.pub2. PMC 6532646. PMID 16235367.
  165. ^ Blanshard A, Hine P (January 2021). "Atovaquone-proguanil for treating uncomplicated Plasmodium falciparum malaria". The Cochrane Database of Systematic Reviews. 1 (1): CD004529. doi:10.1002/14651858.CD004529.pub3. PMC 8094970. PMID 33459345.
  166. ^ van Eijk AM, Terlouw DJ, et al. (Cochrane Infectious Diseases Group) (February 2011). "Azithromycin for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2011 (2): CD006688. doi:10.1002/14651858.CD006688.pub2. PMC 6532599. PMID 21328286.
  167. ^ McIntosh HM, Jones KL, et al. (Cochrane Infectious Diseases Group) (October 2005). "Chloroquine or amodiaquine combined with sulfadoxine-pyrimethamine for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2005 (4): CD000386. doi:10.1002/14651858.CD000386.pub2. PMC 6532604. PMID 16235276.
  168. ^ Amukoye E, Winstanley PA, Watkins WM, Snow RW, Hatcher J, Mosobo M, et al. (October 1997). "Chlorproguanil-dapsone: effective treatment for uncomplicated falciparum malaria". Antimicrobial Agents and Chemotherapy. 41 (10): 2261–2264. doi:10.1128/AAC.41.10.2261. PMC 164103. PMID 9333058.
  169. ^ Bukirwa H, Garner P, Critchley J, et al. (Cochrane Infectious Diseases Group) (October 2004). "Chlorproguanil-dapsone for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2004 (4): CD004387. doi:10.1002/14651858.CD004387.pub2. PMC 6532720. PMID 15495106.
  170. ^ Graves PM, Choi L, Gelband H, Garner P, et al. (Cochrane Infectious Diseases Group) (February 2018). "Primaquine or other 8-aminoquinolines for reducing Plasmodium falciparum transmission". The Cochrane Database of Systematic Reviews. 2018 (2): CD008152. doi:10.1002/14651858.CD008152.pub5. PMC 5815493. PMID 29393511.
  171. ^ Bukirwa H, Critchley J, et al. (Cochrane Infectious Diseases Group) (January 2006). "Sulfadoxine-pyrimethamine plus artesunate versus sulfadoxine-pyrimethamine plus amodiaquine for treating uncomplicated malaria". The Cochrane Database of Systematic Reviews. 2006 (1): CD004966. doi:10.1002/14651858.CD004966.pub2. PMC 6532706. PMID 16437507.
  172. ^ Waters NC, Edstein MD (2011). "8-Aminoquinolines: Primaquine and Tafenoquine". Treatment and Prevention of Malaria. pp. 69–94. doi:10.1007/978-3-0346-0480-2_4. ISBN 978-3-0346-0479-6.
  173. ^ Rodrigo C, Rajapakse S, Fernando D (September 2020). "Tafenoquine for preventing relapse in people with Plasmodium vivax malaria". The Cochrane Database of Systematic Reviews. 9 (9): CD010458. doi:10.1002/14651858.CD010458.pub3. PMC 8094590. PMID 32892362.
  174. ^ Markus MB (May 2023). "Putative Contribution of 8-Aminoquinolines to Preventing Recrudescence of Malaria". Tropical Medicine and Infectious Disease. 8 (5): 278. doi:10.3390/tropicalmed8050278. PMC 10223033. PMID 37235326.
  175. ^ Tarning J (March 2016). "Treatment of Malaria in Pregnancy". The New England Journal of Medicine. 374 (10): 981–982. doi:10.1056/NEJMe1601193. PMID 26962733. Archived from the original on 2023-04-26. Retrieved 2023-01-15.
  176. ^ Manyando C, Kayentao K, D'Alessandro U, Okafor HU, Juma E, Hamed K (May 2012). "A systematic review of the safety and efficacy of artemether-lumefantrine against uncomplicated Plasmodium falciparum malaria during pregnancy". Malaria Journal. 11: 141. doi:10.1186/1475-2875-11-141. PMC 3405476. PMID 22548983.
  177. ^ Orton LC, Omari AA, et al. (Cochrane Infectious Diseases Group) (October 2008). "Drugs for treating uncomplicated malaria in pregnant women". The Cochrane Database of Systematic Reviews. 2008 (4): CD004912. doi:10.1002/14651858.CD004912.pub3. PMC 6532683. PMID 18843672.
  178. ^ Kochar DK, Saxena V, Singh N, Kochar SK, Kumar SV, Das A (January 2005). "Plasmodium vivax malaria". Emerging Infectious Diseases. 11 (1): 132–134. doi:10.3201/eid1101.040519. PMC 3294370. PMID 15705338.
  179. ^ Pasvol G (2005). "The treatment of complicated and severe malaria". British Medical Bulletin. 75–76: 29–47. doi:10.1093/bmb/ldh059. PMID 16495509.
  180. ^ "CDC - Malaria - Diagnosis & Treatment (United States) - Treatment (U.S.) - Artesunate dose 400 mg oral". CDC-Centers for Disease Control and Prevention. 2022-04-11. Archived from the original on 2016-10-29. Retrieved 2022-04-25.
  181. ^ Sinclair D, Donegan S, Isba R, Lalloo DG (June 2012). Sinclair D (ed.). "Artesunate versus quinine for treating severe malaria". The Cochrane Database of Systematic Reviews. 2012 (6): CD005967. doi:10.1002/14651858.CD005967.pub4. PMC 6532684. PMID 22696354.
  182. ^ Kyu HH, Fernández E (December 2009). "Artemisinin derivatives versus quinine for cerebral malaria in African children: a systematic review". Bulletin of the World Health Organization. 87 (12): 896–904. doi:10.2471/BLT.08.060327. PMC 2789363. PMID 20454480. Archived from the original on 2016-03-04.
  183. ^ McIntosh HM, Olliaro P, et al. (Cochrane Infectious Diseases Group) (1998-07-27). "Artemisinin derivatives for treating severe malaria". The Cochrane Database of Systematic Reviews. 1998 (2): CD000527. doi:10.1002/14651858.CD000527. PMC 6532607. PMID 10796551.
  184. ^ Lesi A, Meremikwu M, et al. (Cochrane Infectious Diseases Group) (2004-07-19). "High first dose quinine regimen for treating severe malaria". The Cochrane Database of Systematic Reviews. 2004 (3): CD003341. doi:10.1002/14651858.CD003341.pub2. PMC 6532696. PMID 15266481.
  185. ^ Eisenhut M, Omari AA, et al. (Cochrane Infectious Diseases Group) (January 2009). "Intrarectal quinine versus intravenous or intramuscular quinine for treating Plasmodium falciparum malaria". The Cochrane Database of Systematic Reviews. 2009 (1): CD004009. doi:10.1002/14651858.CD004009.pub3. PMC 6532585. PMID 19160229.
  186. ^ Afolabi BB, Okoromah CN, et al. (Cochrane Infectious Diseases Group) (October 2004). "Intramuscular arteether for treating severe malaria". The Cochrane Database of Systematic Reviews. 2004 (4): CD004391. doi:10.1002/14651858.CD004391.pub2. PMC 6532577. PMID 15495107.
  187. ^ Okebe J, Eisenhut M, et al. (Cochrane Infectious Diseases Group) (May 2014). "Pre-referral rectal artesunate for severe malaria". The Cochrane Database of Systematic Reviews. 2014 (5): CD009964. doi:10.1002/14651858.CD009964.pub2. PMC 4463986. PMID 24869943.
  188. ^ De Buck E, Borra V, Carlson JN, Zideman DA, Singletary EM, Djärv T, et al. (Cochrane Metabolic and Endocrine Disorders Group) (April 2019). "First aid glucose administration routes for symptomatic hypoglycaemia". The Cochrane Database of Systematic Reviews. 2019 (4): CD013283. doi:10.1002/14651858.CD013283.pub2. PMC 6459163. PMID 30973639.
  189. ^ Idro R, Marsh K, John CC, Newton CR (October 2010). "Cerebral malaria: mechanisms of brain injury and strategies for improved neurocognitive outcome". Pediatric Research. 68 (4): 267–274. doi:10.1203/pdr.0b013e3181eee738. PMC 3056312. PMID 20606600.
  190. ^ Okoromah CA, Afolabi BB, Wall EC, et al. (Cochrane Infectious Diseases Group) (April 2011). "Mannitol and other osmotic diuretics as adjuncts for treating cerebral malaria". The Cochrane Database of Systematic Reviews. 2011 (4): CD004615. doi:10.1002/14651858.CD004615.pub3. PMC 4018680. PMID 21491391.
  191. ^ Meremikwu M, Marson AG, et al. (Cochrane Infectious Diseases Group) (2002-04-22). "Routine anticonvulsants for treating cerebral malaria". The Cochrane Database of Systematic Reviews. 2002 (2): CD002152. doi:10.1002/14651858.CD002152. PMC 6532751. PMID 12076440.
  192. ^ Prasad K, Garner P, et al. (Cochrane Infectious Diseases Group) (1999-07-26). "Steroids for treating cerebral malaria". The Cochrane Database of Systematic Reviews. 1999 (2): CD000972. doi:10.1002/14651858.CD000972. PMC 6532619. PMID 10796562.
  193. ^ A Practical Handbook (third edition) Management Of Severe Malaria. World Health Organization. 2012. pp. 43–44. ISBN 9789241548526.
  194. ^ Meremikwu M, Smith HJ, et al. (Cochrane Infectious Diseases Group) (1999-10-25). "Blood transfusion for treating malarial anaemia". The Cochrane Database of Systematic Reviews. 1999 (2): CD001475. doi:10.1002/14651858.CD001475. PMC 6532690. PMID 10796646.
  195. ^ Smith HJ, Meremikwu M, et al. (Cochrane Infectious Diseases Group) (2003-04-22). "Iron chelating agents for treating malaria". The Cochrane Database of Systematic Reviews (2): CD001474. doi:10.1002/14651858.CD001474. PMC 6532667. PMID 12804409.
  196. ^ "Lab-made antibody stops malaria". Nature Biotechnology. 40 (9): 1304. September 2022. doi:10.1038/s41587-022-01480-2. PMID 36085505. S2CID 252181345.
  197. ^ Sinha S, Medhi B, Sehgal R (2014). "Challenges of drug-resistant malaria". Parasite. 21: 61. doi:10.1051/parasite/2014059. PMC 4234044. PMID 25402734.
  198. ^ O'Brien C, Henrich PP, Passi N, Fidock DA (December 2011). "Recent clinical and molecular insights into emerging artemisinin resistance in Plasmodium falciparum". Current Opinion in Infectious Diseases. 24 (6): 570–577. doi:10.1097/QCO.0b013e32834cd3ed. PMC 3268008. PMID 22001944.
  199. ^ Fairhurst RM, Nayyar GM, Breman JG, Hallett R, Vennerstrom JL, Duong S, et al. (August 2012). "Artemisinin-resistant malaria: research challenges, opportunities, and public health implications". The American Journal of Tropical Medicine and Hygiene. 87 (2): 231–241. doi:10.4269/ajtmh.2012.12-0025. PMC 3414557. PMID 22855752.
  200. ^ White NJ (April 2008). "Qinghaosu (artemisinin): the price of success". Science. 320 (5874): 330–334. Bibcode:2008Sci...320..330W. doi:10.1126/science.1155165. PMID 18420924. S2CID 39014319.
  201. ^ Wongsrichanalai C, Meshnick SR (May 2008). "Declining artesunate-mefloquine efficacy against falciparum malaria on the Cambodia-Thailand border". Emerging Infectious Diseases. 14 (5): 716–719. doi:10.3201/eid1405.071601. PMC 2600243. PMID 18439351.
  202. ^ Dondorp AM, Yeung S, White L, Nguon C, Day NP, Socheat D, et al. (April 2010). "Artemisinin resistance: current status and scenarios for containment". Nature Reviews. Microbiology. 8 (4): 272–280. doi:10.1038/nrmicro2331. PMID 20208550. S2CID 39148119.
  203. ^ World Health Organization (2013). "Q&A on artemisinin resistance". WHO Malaria Publications. Archived from the original on 2016-07-20.
  204. ^ Briggs H (2014-07-30). "Call for 'radical action' on drug-resistant malaria". BBC News. Archived from the original on 2023-02-23. Retrieved 2023-02-23.
  205. ^ Ashley EA, Dhorda M, Fairhurst RM, Amaratunga C, Lim P, Suon S, et al. (July 2014). "Spread of artemisinin resistance in Plasmodium falciparum malaria". The New England Journal of Medicine. 371 (5): 411–423. doi:10.1056/NEJMoa1314981. PMC 4143591. PMID 25075834.
  206. ^ Gallagher J (2019-07-23). "Resistant malaria spreading in South East Asia". Archived from the original on 2019-07-24. Retrieved 2019-07-25.
  207. ^ Orton L, Barnish G, et al. (Cochrane Infectious Diseases Group) (April 2005). "Unit-dose packaged drugs for treating malaria". The Cochrane Database of Systematic Reviews. 2005 (2): CD004614. doi:10.1002/14651858.CD004614.pub2. PMC 6532754. PMID 15846723.
  208. ^ "Frequently Asked Questions (FAQs): If I get malaria, will I have it for the rest of my life?". US Centers for Disease Control and Prevention. February 8, 2010. Archived from the original on May 13, 2012. Retrieved 2012-05-14.
  209. ^ Trampuz A, Jereb M, Muzlovic I, Prabhu RM (August 2003). "Clinical review: Severe malaria". Critical Care. 7 (4): 315–323. doi:10.1186/cc2183. PMC 270697. PMID 12930555.
  210. ^ a b c d Fernando SD, Rodrigo C, Rajapakse S (December 2010). "The 'hidden' burden of malaria: cognitive impairment following infection". Malaria Journal. 9: 366. doi:10.1186/1475-2875-9-366. PMC 3018393. PMID 21171998.
  211. ^ Riley EM, Stewart VA (February 2013). "Immune mechanisms in malaria: new insights in vaccine development". Nature Medicine. 19 (2): 168–178. doi:10.1038/nm.3083. PMID 23389617. S2CID 8763732.
  212. ^ a b Idro R, Marsh K, John CC, Newton CR (October 2010). "Cerebral malaria: mechanisms of brain injury and strategies for improved neurocognitive outcome". Pediatric Research. 68 (4): 267–274. doi:10.1203/PDR.0b013e3181eee738. PMC 3056312. PMID 20606600.
  213. ^ Tatem AJ, Jia P, Ordanovich D, Falkner M, Huang Z, Howes R, et al. (January 2017). "The geography of imported malaria to non-endemic countries: a meta-analysis of nationally reported statistics". The Lancet Infectious Diseases. 17 (1): 98–107. Bibcode:2017LanID..17...98T. doi:10.1016/S1473-3099(16)30326-7. PMC 5392593. PMID 27777030.
  214. ^ WHO (2021). World Malaria Report 2021. Switzerland: World Health Organization. ISBN 978-92-4-004049-6. Archived from the original on 2023-05-06. Retrieved 2022-01-24.
  215. ^ "CDC - Malaria - About Malaria - History - Elimination of Malaria in the United States (1947-1951)". CDC-Centers for Disease Control and Prevention. 28 January 2019. Archived from the original on 4 May 2012. Retrieved 17 January 2020.
  216. ^ "CDC - Malaria - About Malaria - Malaria Transmission in the United States". CDC-Centers for Disease Control and Prevention. 2019-01-28. Archived from the original on 2022-07-19. Retrieved 2021-09-03.
  217. ^ Health Alert Network (HAN) (2023-06-26). "Locally Acquired Malaria Cases Identified in the United States". emergency.cdc.gov. Archived from the original on 2023-06-26. Retrieved 2023-06-27.
  218. ^ "Important Updates on Locally Acquired Malaria Cases Identified in Florida, Texas, and Maryland". Health Alert Network (HAN) - 00496. 2023-08-28. Archived from the original on 2023-08-28. Retrieved 2023-08-28.
  219. ^ Layne SP. "Principles of Infectious Disease Epidemiology" (PDF). EPI 220. UCLA Department of Epidemiology. Archived from the original (PDF) on 2006-02-20. Retrieved 2007-06-15.
  220. ^ Provost C (April 25, 2011). "World Malaria Day: Which countries are the hardest hit? Get the full data". The Guardian. Archived from the original on August 1, 2013. Retrieved 2012-05-03.
  221. ^ Murray CJ, Rosenfeld LC, Lim SS, Andrews KG, Foreman KJ, Haring D, et al. (February 2012). "Global malaria mortality between 1980 and 2010: a systematic analysis". The Lancet. 379 (9814): 413–431. doi:10.1016/S0140-6736(12)60034-8. PMID 22305225. S2CID 46171431.
  222. ^ a b Guerra CA, Hay SI, Lucioparedes LS, Gikandi PW, Tatem AJ, Noor AM, et al. (February 2007). "Assembling a global database of malaria parasite prevalence for the Malaria Atlas Project". Malaria Journal. 6 (1): 17. doi:10.1186/1475-2875-6-17. PMC 1805762. PMID 17306022.
  223. ^ Hay SI, Okiro EA, Gething PW, Patil AP, Tatem AJ, Guerra CA, et al. (June 2010). I (ed.). "Estimating the global clinical burden of Plasmodium falciparum malaria in 2007". PLOS Medicine. 7 (6): e1000290. Bibcode:2010PLOSM...7..290H. doi:10.1371/journal.pmed.1000290. PMC 2885984. PMID 20563310.
  224. ^ Gething PW, Patil AP, Smith DL, Guerra CA, Elyazar IR, Johnston GL, et al. (December 2011). "A new world malaria map: Plasmodium falciparum endemicity in 2010". Malaria Journal. 10 (1): 378. Bibcode:2011MalJ...10..378G. doi:10.1186/1475-2875-10-378. PMC 3274487. PMID 22185615.
  225. ^ Weiss DJ, Lucas TC, Nguyen M, Nandi AK, Bisanzio D, Battle KE, et al. (July 2019). "Mapping the global prevalence, incidence, and mortality of Plasmodium falciparum, 2000-17: a spatial and temporal modelling study". The Lancet. 394 (10195): 322–331. doi:10.1016/S0140-6736(19)31097-9. PMC 6675740. PMID 31229234.
  226. ^ Battle KE, Lucas TC, Nguyen M, Howes RE, Nandi AK, Twohig KA, et al. (July 2019). "Mapping the global endemicity and clinical burden of Plasmodium vivax, 2000-17: a spatial and temporal modelling study". The Lancet. 394 (10195): 332–343. doi:10.1016/S0140-6736(19)31096-7. PMC 6675736. PMID 31229233.
  227. ^ Greenwood B, Mutabingwa T (February 2002). "Malaria in 2002". Nature. 415 (6872): 670–672. doi:10.1038/415670a. PMID 11832954. S2CID 4394237.
  228. ^ Jamieson A, Toovey S, Maurel M (2006). Malaria: A Traveller's Guide. Struik. p. 30. ISBN 978-1-77007-353-1.
  229. ^ Abeku TA (May 2007). "Response to malaria epidemics in Africa". Emerging Infectious Diseases. 13 (5): 681–686. doi:10.3201/eid1305.061333. PMC 2738452. PMID 17553244.
  230. ^ Cui L, Yan G, Sattabongkot J, Cao Y, Chen B, Chen X, et al. (March 2012). "Malaria in the Greater Mekong Subregion: heterogeneity and complexity". Acta Tropica. 121 (3): 227–239. doi:10.1016/j.actatropica.2011.02.016. PMC 3132579. PMID 21382335.
  231. ^ Machault V, Vignolles C, Borchi F, Vounatsou P, Pages F, Briolant S, et al. (May 2011). "The use of remotely sensed environmental data in the study of malaria". Geospatial Health. 5 (2): 151–168. Bibcode:2011GeosH...5..151M. doi:10.4081/gh.2011.167. PMID 21590665.
  232. ^ "Climate Change And Infectious Diseases" (PDF). Climate Change and Human Health—Risk and Responses. World Health Organization. Archived (PDF) from the original on 2016-03-04.
  233. ^ "Climate change and human health—risks and responses. Summary". www.who.int. Archived from the original on December 25, 2003. Retrieved 29 October 2018.
  234. ^ Hulme M, Doherty R, Ngara T, New M, Lister D (August 2001). "African climate change: 1900-2100" (PDF). Climate Research. 17 (2): 145–68. Bibcode:2001ClRes..17..145H. doi:10.3354/cr017145. Archived (PDF) from the original on 2021-06-30. Retrieved 2020-09-08.
  235. ^ a b Smith MW, Willis T, Alfieri L, James WH, Trigg MA, Yamazaki D, et al. (August 2020). "Incorporating hydrology into climate suitability models changes projections of malaria transmission in Africa". Nature Communications. 11 (1): 4353. Bibcode:2020NatCo..11.4353S. doi:10.1038/s41467-020-18239-5. PMC 7455692. PMID 32859908.
  236. ^ Harper K, Armelagos G (February 2010). "The changing disease-scape in the third epidemiological transition". International Journal of Environmental Research and Public Health. 7 (2): 675–697. doi:10.3390/ijerph7020675. PMC 2872288. PMID 20616997.
  237. ^ Prugnolle F, Durand P, Ollomo B, Duval L, Ariey F, Arnathau C, et al. (February 2011). Manchester M (ed.). "A fresh look at the origin of Plasmodium falciparum, the most malignant malaria agent". PLOS Pathogens. 7 (2): e1001283. doi:10.1371/journal.ppat.1001283. PMC 3044689. PMID 21383971.
  238. ^ Cox FE (October 2002). "History of human parasitology". Clinical Microbiology Reviews. 15 (4): 595–612. doi:10.1128/CMR.15.4.595-612.2002. PMC 126866. PMID 12364371.
  239. ^ Dave T, Habte A, Vora V, Sheikh MQ, Sanker V, Gopal SV (April 2024). "Sushruta: The Father of Indian Surgical History". Plastic and Reconstructive Surgery. Global Open. 12 (4): e5715. doi:10.1097/GOX.0000000000005715. PMC 11000756. PMID 38596573.
  240. ^ a b Strong RP (1944). Stitt's Diagnosis, Prevention and Treatment of Tropical Diseases (Seventh ed.). York, PA: The Blakiston Company. p. 3.
  241. ^ "DNA clues to malaria in ancient Rome". BBC News. February 20, 2001. Archived from the original on November 2, 2010., in reference to Sallares R, Gomzi S (2001). "Biomolecular archaeology of malaria". Ancient Biomolecules. 3 (3): 195–213. OCLC 538284457.
  242. ^ Sallares R (2002). Malaria and Rome: A History of Malaria in Ancient Italy. Oxford University Press. doi:10.1093/acprof:oso/9780199248506.001.0001. ISBN 978-0-19-924850-6.
  243. ^ Hays JN (2005). Epidemics and Pandemics: Their Impacts on Human History. Santa Barbara, CA: ABC-CLIO. p. 11. ISBN 978-1-85109-658-9. Archived from the original on 2023-01-13. Retrieved 2015-10-27.
  244. ^ Rodrigues PT, Valdivia HO, de Oliveira TC, Alves JM, Duarte AM, Cerutti-Junior C, et al. (January 2018). "Human migration and the spread of malaria parasites to the New World". Scientific Reports. 8 (1): 1993. Bibcode:2018NatSR...8.1993R. doi:10.1038/s41598-018-19554-0. PMC 5792595. PMID 29386521.
  245. ^ De Castro MC, Singer BH (2005). "Was malaria present in the Amazon before the European conquest? Available evidence and future research agenda". J. Archaeol. Sci. 32 (3): 337–40. Bibcode:2005JArSc..32..337D. doi:10.1016/j.jas.2004.10.004.
  246. ^ Yalcindag E, Elguero E, Arnathau C, Durand P, Akiana J, Anderson TJ, et al. (January 2012). "Multiple independent introductions of Plasmodium falciparum in South America". Proceedings of the National Academy of Sciences of the United States of America. 109 (2): 511–516. Bibcode:2012PNAS..109..511Y. doi:10.1073/pnas.1119058109. PMC 3258587. PMID 22203975.
  247. ^ "Malarial organisms in the blood". Scientific American. 46 (3). Munn & Company: 37–38. 21 January 1882.
  248. ^ "The Nobel Prize in Physiology or Medicine 1907: Alphonse Laveran". The Nobel Foundation. Archived from the original on 2012-06-23. Retrieved 2012-05-14.
  249. ^ Tan SY, Sung H (May 2008). "Carlos Juan Finlay (1833-1915): of mosquitoes and yellow fever" (PDF). Singapore Medical Journal. 49 (5): 370–371. PMID 18465043. Archived (PDF) from the original on 2008-07-23.
  250. ^ Chernin E (November 1983). "Josiah Clark Nott, insects, and yellow fever". Bulletin of the New York Academy of Medicine. 59 (9): 790–802. PMC 1911699. PMID 6140039.
  251. ^ Chernin E (September 1977). "Patrick Manson (1844-1922) and the transmission of filariasis". The American Journal of Tropical Medicine and Hygiene. 26 (5 Pt 2 Suppl): 1065–1070. doi:10.4269/ajtmh.1977.26.1065. PMID 20786.
  252. ^ a b c Cox FE (February 2010). "History of the discovery of the malaria parasites and their vectors". Parasites & Vectors. 3 (1): 5. doi:10.1186/1756-3305-3-5. PMC 2825508. PMID 20205846.
  253. ^ "Ross and the Discovery that Mosquitoes Transmit Malaria Parasites". CDC Malaria website. Archived from the original on 2007-06-02. Retrieved 2012-06-14.
  254. ^ Simmons JS (1979). Malaria in Panama. Ayer Publishing. ISBN 978-0-405-10628-6. Archived from the original on 2023-01-13. Retrieved 2015-10-27.
  255. ^ "Amico Bignami". www.whonamedit.com. Archived from the original on 30 July 2019. Retrieved 30 July 2019.
  256. ^ Kaufman TS, Rúveda EA (January 2005). "The quest for quinine: those who won the battles and those who won the war". Angewandte Chemie. 44 (6): 854–885. doi:10.1002/anie.200400663. PMID 15669029.
  257. ^ Pelletier PJ, Caventou JB (1820). "Des recherches chimiques sur les Quinquinas" [Chemical research on quinquinas]. Annales de Chimie et de Physique (in French). 15: 337–65.
  258. ^ Kyle RA, Shampe MA (July 1974). "Discoverers of quinine". JAMA. 229 (4): 462. doi:10.1001/jama.229.4.462 (inactive 1 November 2024). PMID 4600403.{{cite journal}}: CS1 maint: DOI inactive as of November 2024 (link)
  259. ^ Achan J, Talisuna AO, Erhart A, Yeka A, Tibenderana JK, Baliraine FN, et al. (May 2011). "Quinine, an old anti-malarial drug in a modern world: role in the treatment of malaria". Malaria Journal. 10 (1): 144. doi:10.1186/1475-2875-10-144. PMC 3121651. PMID 21609473.
  260. ^ Ekiert H, Świątkowska J, Klin P, Rzepiela A, Szopa A (July 2021). "Artemisia annua - Importance in Traditional Medicine and Current State of Knowledge on the Chemistry, Biological Activity and Possible Applications". Planta Medica. 87 (8): 584–599. doi:10.1055/a-1345-9528. PMID 33482666.
  261. ^ Timóteo P, Wessels C, Righeschi C, Goris H, Bilia A (24 August 2010). "Evaluation of stability of constituents of herbal drug preparations from Artemisia annua L". Planta Medica. 76 (12). doi:10.1055/s-0030-1264749.
  262. ^ WHO monograph on good agricultural and collection practices (GACP) for Artemisia annua L. World Health Organization. 2006. hdl:10665/43509. ISBN 978-92-4-159443-1.[page needed]
  263. ^ van der Kooy F, Sullivan SE (October 2013). "The complexity of medicinal plants: the traditional Artemisia annua formulation, current status and future perspectives". Journal of Ethnopharmacology (Review). 150 (1): 1–13. doi:10.1016/j.jep.2013.08.021. PMID 23973523.
  264. ^ Hsu E (June 2006). "Reflections on the 'discovery' of the antimalarial qinghao". British Journal of Clinical Pharmacology. 61 (6): 666–670. doi:10.1111/j.1365-2125.2006.02673.x. PMC 1885105. PMID 16722826.
  265. ^ Hao C (29 September 2011). "Lasker Award Rekindles Debate Over Artemisinin's Discovery". News: ScienceInsider. Science/AAAS. Archived from the original on 4 January 2014.
  266. ^ "Nobel Prize announcement" (PDF). NobelPrize.org. Archived (PDF) from the original on 6 October 2015. Retrieved 5 October 2015.
  267. ^ Vogel G (November 2013). "The forgotten malaria". Science. 342 (6159): 684–687. Bibcode:2013Sci...342..684V. doi:10.1126/science.342.6159.684. PMID 24202156.
  268. ^ "Eradication of Malaria in the United States (1947–1951)". US Centers for Disease Control and Prevention. February 8, 2010. Archived from the original on May 4, 2012. Retrieved 2012-05-02.
  269. ^ Killeen GF, Fillinger U, Kiche I, Gouagna LC, Knols BG (October 2002). "Eradication of Anopheles gambiae from Brazil: lessons for malaria control in Africa?". The Lancet Infectious Diseases. 2 (10): 618–627. doi:10.1016/S1473-3099(02)00397-3. PMID 12383612.
  270. ^ Meade MS, Emch M (2010). Medical Geography (3rd ed.). Guilford Press. pp. 120–23. ISBN 978-1-60623-016-9. Archived from the original on 2023-01-13. Retrieved 2015-10-27.
  271. ^ Williams LL (January 1963). "Malaria eradication in the United States". American Journal of Public Health and the Nation's Health. 53 (1): 17–21. doi:10.2105/AJPH.53.1.17. PMC 1253858. PMID 14000898.
  272. ^ "Malaria Elimination Group description and list of elimination countries". Archived from the original on 27 July 2011. Retrieved 2011-07-12.
  273. ^ a b Gladwell M (July 2, 2001). "The Mosquito Killer". The New Yorker. Archived from the original on April 16, 2016. Retrieved August 20, 2014.
  274. ^ "World Malaria Report" (PDF). World Health Organization. 2009. Archived (PDF) from the original on January 12, 2010. Retrieved December 17, 2009.
  275. ^ a b Duintjer Tebbens RJ, Thompson KM (2009). "Priority Shifting and the Dynamics of Managing Eradicable Infectious Diseases". Management Science. 55 (4): 650–663. doi:10.1287/mnsc.1080.0965.
  276. ^ Mendis K, Rietveld A, Warsame M, Bosman A, Greenwood B, Wernsdorfer WH (July 2009). "From malaria control to eradication: The WHO perspective". Tropical Medicine & International Health. 14 (7): 802–809. doi:10.1111/j.1365-3156.2009.02287.x. PMID 19497083. S2CID 31335358.
  277. ^ a b c Sadasivaiah S, Tozan Y, Breman JG (December 2007). "Dichlorodiphenyltrichloroethane (DDT) for indoor residual spraying in Africa: how can it be used for malaria control?". The American Journal of Tropical Medicine and Hygiene. 77 (6 Suppl): 249–263. doi:10.4269/ajtmh.2007.77.249. PMID 18165500.
  278. ^ a b Harrison GA (1978). Mosquitoes, Malaria, and Man: A History of the Hostilities Since 1880. Dutton. ISBN 978-0-525-16025-0. Archived from the original on October 19, 2021. Retrieved August 29, 2022.
  279. ^ a b Chapin G, Wasserstrom R (1981). "Agricultural production and malaria resurgence in Central America and India". Nature. 293 (5829): 181–185. Bibcode:1981Natur.293..181C. doi:10.1038/293181a0. PMID 7278974. S2CID 4346743.
  280. ^ van den Berg H (October 23, 2008). "Global status of DDT and its alternatives for use in vector control to prevent disease" (PDF). Stockholm Convention on Persistent Organic Pollutants/United Nations Environment Programme. Archived from the original (PDF) on December 17, 2010. Retrieved November 22, 2008.
  281. ^ Feachem RG, Sabot OJ (May 2007). "Global malaria control in the 21st century: a historic but fleeting opportunity". JAMA. 297 (20): 2281–2284. doi:10.1001/jama.297.20.2281. PMID 17519417.
  282. ^ Garrett L (1994). The Coming Plague: Newly Emerging Diseases in a World Out of Balance. Farrar, Straus and Giroux. p. 51. ISBN 978-1-4299-5327-6. Archived from the original on October 19, 2021. Retrieved August 29, 2022.
  283. ^ McNeil Jr DG (December 27, 2010). "Malaria: A Disease Close to Eradication Grows, Aided by Political Tumult in Sri Lanka". The New York Times. Archived from the original on January 4, 2017. Retrieved February 7, 2017.
  284. ^ Karunaweera ND, Galappaththy GN, Wirth DF (February 2014). "On the road to eliminate malaria in Sri Lanka: lessons from history, challenges, gaps in knowledge and research needs". Malaria Journal. 13: 59. doi:10.1186/1475-2875-13-59. PMC 3943480. PMID 24548783.
  285. ^ a b Nájera JA, González-Silva M, Alonso PL (January 2011). "Some lessons for the future from the Global Malaria Eradication Programme (1955-1969)". PLOS Medicine. 8 (1): e1000412. doi:10.1371/journal.pmed.1000412. PMC 3026700. PMID 21311585.
  286. ^ Rogan WJ, Chen A (2005). "Health risks and benefits of bis(4-chlorophenyl)-1,1,1-trichloroethane (DDT)". The Lancet. 366 (9487): 763–773. doi:10.1016/S0140-6736(05)67182-6. PMID 16125595. S2CID 3762435. Archived from the original on October 17, 2019. Retrieved June 13, 2019.
  287. ^ a b Sato S (January 2021). "Plasmodium-a brief introduction to the parasites causing human malaria and their basic biology". Journal of Physiological Anthropology. 40 (1): 1. doi:10.1186/s40101-020-00251-9. PMC 7792015. PMID 33413683.
  288. ^ Enserink M (29 March 2021). "Is setting a deadline for eradicating malaria a good idea? Scientists are divided". Science. doi:10.1126/science.aaz2906.
  289. ^ Strom S (April 1, 2011). "Mission Accomplished, Nonprofits Go Out of Business". The New York Times. OCLC 292231852. Archived from the original on December 25, 2011. Retrieved 2012-05-09.
  290. ^ "Fighting AIDS, Tuberculosis and Malaria". The Global Fund. Archived from the original on 2012-05-05. Retrieved 2012-05-09.
  291. ^ Schoofs M (July 17, 2008). "Clinton foundation sets up malaria-drug price plan". The Wall Street Journal. Archived from the original on January 19, 2016. Retrieved 2012-05-14.
  292. ^ "Executive summary and key points" (PDF). World Malaria Report 2013. World Health Organization. Archived (PDF) from the original on 4 March 2016. Retrieved 13 February 2014.
  293. ^ a b Fletcher M (16 July 2019). "Mosquito gene-editing: can it wipe out malaria?". The Telegraph.
  294. ^ Radwick D (October 5, 2016). "Can Malaria Be Eradicated?". Council on Foreign Relations. Archived from the original on October 5, 2016.
  295. ^ "Fact Sheet: World Malaria Report 2015". 9 December 2015. Archived from the original on December 17, 2015.
  296. ^ a b c d e "World Malaria Report 2020". www.who.int. Archived from the original on 2022-03-25. Retrieved 2021-05-26.
  297. ^ Chandler CI, Beisel U (July 2017). "The Anthropology of Malaria: Locating the Social". Medical Anthropology. 36 (5): 411–421. doi:10.1080/01459740.2017.1306858. PMID 28318308.
  298. ^ "Algeria and Argentina certified malaria-free by WHO". www.who.int. Archived from the original on 2021-11-26. Retrieved 2021-11-26.
  299. ^ Eliminating malaria: 21 countries, a common goal, World Health Organization, Wikidata Q108595589
  300. ^ From 30 million cases to zero: China is certified malaria-free by WHO, World Health Organization, 30 June 2021, Wikidata Q108595181.
  301. ^ Zeroing in on Malaria Elimination: Final report of the E-2020 initiative, World Health Organization, 21 April 2021, Wikidata Q108595714
  302. ^ Ro C (26 September 2019). "The tiny kingdom fighting an epidemic". BBC Future. Archived from the original on 2019-10-08. Retrieved 2019-09-30.
  303. ^ "WHO certifies Paraguay malaria-free". World Health Organization. 11 June 2018. Archived from the original on 15 June 2018. Retrieved 17 June 2018.
  304. ^ "WHO certifies Azerbaijan and Tajikistan as malaria-free". World Health Organization. 2023-03-29. Archived from the original on 2023-06-21. Retrieved 2023-06-22.
  305. ^ "Belize certified malaria-free by WHO". World Health Organization. 2023-06-21. Archived from the original on 2023-06-21. Retrieved 2023-06-22.
  306. ^ "Who declares Cape Verde free of malaria". World Health Organization. 2024-01-12. Archived from the original on 2024-01-12. Retrieved 2024-01-13.
  307. ^ "'Historic': Egypt declared malaria free by the World Health Organization". Al Jazeera. 20 October 2024. Retrieved 21 October 2024.
  308. ^ Malaria could be eradicated by 2050, say global experts| https://www.bmj.com/content/366/bmj.l5501
  309. ^ MALARIA ERADICATION WITHIN A GENERATION| https://live-malariaeradicationcommission.pantheonsite.io/sites/default/files/overview-brief-english.pdf
  310. ^ Humphreys M (2001). Malaria: Poverty, Race, and Public Health in the United States. Johns Hopkins University Press. p. 256. ISBN 0-8018-6637-5.
  311. ^ Sachs J, Malaney P (February 2002). "The economic and social burden of malaria". Nature. 415 (6872): 680–685. doi:10.1038/415680a. PMID 11832956. S2CID 618837.
  312. ^ Roll Back Malaria WHO partnership (2003). "Economic costs of malaria" (PDF). WHO. Archived from the original (PDF) on 2009-12-29.
  313. ^ Ricci F (2012). "Social implications of malaria and their relationships with poverty". Mediterranean Journal of Hematology and Infectious Diseases. 4 (1): e2012048. doi:10.4084/MJHID.2012.048. PMC 3435125. PMID 22973492.
  314. ^ Lon CT, Tsuyuoka R, Phanouvong S, Nivanna N, Socheat D, Sokhan C, et al. (November 2006). "Counterfeit and substandard antimalarial drugs in Cambodia". Transactions of the Royal Society of Tropical Medicine and Hygiene. 100 (11): 1019–1024. doi:10.1016/j.trstmh.2006.01.003. PMID 16765399.
  315. ^ Newton PN, Fernández FM, Plançon A, Mildenhall DC, Green MD, Ziyong L, et al. (February 2008). "A collaborative epidemiological investigation into the criminal fake artesunate trade in South East Asia". PLOS Medicine. 5 (2): e32. doi:10.1371/journal.pmed.0050032. PMC 2235893. PMID 18271620.
  316. ^ Newton PN, Green MD, Fernández FM, Day NP, White NJ (September 2006). "Counterfeit anti-infective drugs". The Lancet Infectious Diseases. 6 (9): 602–613. doi:10.1016/S1473-3099(06)70581-3. PMID 16931411.
  317. ^ Parry J (May 2005). "WHO combats counterfeit malaria drugs in Asia". BMJ. 330 (7499): 1044. doi:10.1136/bmj.330.7499.1044-d. PMC 557259. PMID 15879383.
  318. ^ Gautam CS, Utreja A, Singal GL (May 2009). "Spurious and counterfeit drugs: a growing industry in the developing world". Postgraduate Medical Journal. 85 (1003): 251–256. doi:10.1136/pgmj.2008.073213. PMID 19520877. S2CID 35470138.
  319. ^ Caudron JM, Ford N, Henkens M, Macé C, Kiddle-Monroe R, Pinel J (August 2008). "Substandard medicines in resource-poor settings: a problem that can no longer be ignored". Tropical Medicine & International Health. 13 (8): 1062–1072. doi:10.1111/j.1365-3156.2008.02106.x. hdl:10144/37334. PMID 18631318.
  320. ^ Nayyar GM, Breman JG, Newton PN, Herrington J (June 2012). "Poor-quality antimalarial drugs in southeast Asia and sub-Saharan Africa". The Lancet Infectious Diseases. 12 (6): 488–496. doi:10.1016/S1473-3099(12)70064-6. PMID 22632187.
  321. ^ Russell PF (2009). "Communicable diseases Malaria". Medical Department of the United States Army in World War II. U.S. Army Medical Department. Office of Medical History. Archived from the original on October 9, 2012. Retrieved 2012-09-24.
  322. ^ Melville CH (1910). "The prevention of malaria in war". In Ross R (ed.). The Prevention of Malaria. New York: E.P. Dutton. p. 577. Archived from the original on 2016-03-12.
  323. ^ Bryant BJ, Knights KM (2011). Pharmacology for Health Professionals. Elsevier Australia. p. 895. ISBN 9780729539296.
  324. ^ Bray RS (2004). Armies of Pestilence: The Effects of Pandemics on History. James Clarke. p. 102. ISBN 978-0-227-17240-7. Archived from the original on 2023-01-12. Retrieved 2015-10-27.
  325. ^ Byrne JP (2008). Encyclopedia of Pestilence, Pandemics, and Plagues: A-M. ABC-CLIO. p. 383. ISBN 978-0-313-34102-1.[permanent dead link]
  326. ^ Kakkilaya BS (April 14, 2006). "History of Malaria During Wars". Malariasite.com. Archived from the original on April 3, 2012. Retrieved 2012-05-03.
  327. ^ "History | CDC Malaria". US Centers for Disease Control and Prevention. February 8, 2010. Archived from the original on August 28, 2010. Retrieved 2012-05-15.
  328. ^ Hall BF, Fauci AS (December 2009). "Malaria control, elimination, and eradication: the role of the evolving biomedical research agenda". The Journal of Infectious Diseases. 200 (11): 1639–1643. doi:10.1086/646611. PMID 19877843.
  329. ^ "WHO | A research agenda for malaria eradication". www.who.int. Archived from the original on 2016-03-07. Retrieved 2016-03-07.
  330. ^ Kalanon M, McFadden GI (June 2010). "Malaria, Plasmodium falciparum and its apicoplast". Biochemical Society Transactions. 38 (3): 775–782. doi:10.1042/BST0380775. PMID 20491664.
  331. ^ Müller IB, Hyde JE, Wrenger C (January 2010). "Vitamin B metabolism in Plasmodium falciparum as a source of drug targets". Trends in Parasitology. 26 (1): 35–43. doi:10.1016/j.pt.2009.10.006. PMID 19939733.
  332. ^ Du Q, Wang H, Xie J (January 2011). "Thiamin (vitamin B1) biosynthesis and regulation: a rich source of antimicrobial drug targets?". International Journal of Biological Sciences. 7 (1): 41–52. doi:10.7150/ijbs.7.41. PMC 3020362. PMID 21234302.
  333. ^ Biot C, Castro W, Botté CY, Navarro M (June 2012). "The therapeutic potential of metal-based antimalarial agents: implications for the mechanism of action". Dalton Transactions. 41 (21): 6335–6349. doi:10.1039/C2DT12247B. PMID 22362072.
  334. ^ Roux C, Biot C (April 2012). "Ferrocene-based antimalarials". Future Medicinal Chemistry. 4 (6): 783–797. doi:10.4155/fmc.12.26. PMID 22530641.
  335. ^ a b John C (8 December 2014). "New malaria drug unleashes an immune system assault on infected cells". fiercebiotechresearch.com. Archived from the original on 4 April 2016. Retrieved 16 December 2014.
  336. ^ Singh R, Bhardwaj V, Purohit R (January 2021). "Identification of a novel binding mechanism of Quinoline based molecules with lactate dehydrogenase of Plasmodium falciparum". Journal of Biomolecular Structure & Dynamics. 39 (1): 348–356. doi:10.1080/07391102.2020.1711809. PMID 31903852.
  337. ^ a b c d e Stanway RR, Bushell E, Chiappino-Pepe A, Roques M, Sanderson T, Franke-Fayard B, et al. (November 2019). "Genome-Scale Identification of Essential Metabolic Processes for Targeting the Plasmodium Liver Stage". Cell. 179 (5): 1112–1128.e26. doi:10.1016/j.cell.2019.10.030. PMC 6904910. PMID 31730853.
  338. ^ Roy M, Rawat A, Kaushik S, Jyoti A, Srivastava VK (August 2022). "Endogenous cysteine protease inhibitors in upmost pathogenic parasitic protozoa". Microbiological Research. 261: 127061. doi:10.1016/j.micres.2022.127061. PMID 35605309. S2CID 248741177.
  339. ^ Gardner MJ, Hall N, Fung E, White O, Berriman M, Hyman RW, et al. (October 2002). "Genome sequence of the human malaria parasite Plasmodium falciparum". Nature. 419 (6906): 498–511. Bibcode:2002Natur.419..498G. doi:10.1038/nature01097. PMC 3836256. PMID 12368864.
  340. ^ Malaria Genomics, Vaccine Development, and Microbiome| https://www.mdpi.com/2076-0817/12/8/1061
  341. ^ Charon J, Grigg MJ, Eden JS, Piera KA, Rana H, William T, et al. (December 2019). "Novel RNA viruses associated with Plasmodium vivax in human malaria and Leucocytozoon parasites in avian disease". PLOS Pathogens. 15 (12): e1008216. doi:10.1371/journal.ppat.1008216. PMC 6953888. PMID 31887217.
  342. ^ Aultman KS, Gottlieb M, Giovanni MY, Fauci AS (October 2002). "Anopheles gambiae genome: completing the malaria triad". Science. 298 (5591): 13. doi:10.1126/science.298.5591.13. PMID 12364752.
  343. ^ Ito J, Ghosh A, Moreira LA, Wimmer EA, Jacobs-Lorena M (May 2002). "Transgenic anopheline mosquitoes impaired in transmission of a malaria parasite". Nature. 417 (6887): 452–455. Bibcode:2002Natur.417..452I. doi:10.1038/417452a. PMID 12024215. S2CID 4376984.
  344. ^ Gantz VM, Jasinskiene N, Tatarenkova O, Fazekas A, Macias VM, Bier E, et al. (December 2015). "Highly efficient Cas9-mediated gene drive for population modification of the malaria vector mosquito Anopheles stephensi". Proceedings of the National Academy of Sciences of the United States of America. 112 (49): E6736–E6743. Bibcode:2015PNAS..112E6736G. doi:10.1073/pnas.1521077112. PMC 4679060. PMID 26598698.
  345. ^ "Malarial mosquitoes suppressed in experiments that mimic natural environments". 28 July 2021. Archived from the original on 21 November 2021. Retrieved 21 November 2021.
  346. ^ Flam F (4 February 2016). "Fighting Zika Virus With Genetic Engineering". Bloomberg. Archived from the original on 6 June 2016.
  347. ^ a b Griffiths EC, Fairlie-Clarke K, Allen JE, Metcalf CJ, Graham AL (December 2015). "Bottom-up regulation of malaria population dynamics in mice co-infected with lung-migratory nematodes" (PDF). Ecology Letters. 18 (12): 1387–1396. Bibcode:2015EcolL..18.1387G. doi:10.1111/ele.12534. PMID 26477454.
  348. ^ Arshad AR, Bashir I, Ijaz F, Loh N, Shukla S, Rehman UU, et al. (December 2020). "Is COVID-19 Fatality Rate Associated with Malaria Endemicity?". Discoveries. 8 (4): e120. doi:10.15190/d.2020.17. PMC 7749783. PMID 33365386.
  349. ^ Wang S, Dos-Santos AL, Huang W, Liu KC, Oshaghi MA, Wei G, et al. (September 2017). "Driving mosquito refractoriness to Plasmodium falciparum with engineered symbiotic bacteria". Science. 357 (6358): 1399–1402. Bibcode:2017Sci...357.1399W. doi:10.1126/science.aan5478. PMC 9793889. PMID 28963255.
  350. ^ Servick K (28 September 2017). "The microbes in a mosquito's gut may help fight malaria". Science. doi:10.1126/science.aaq0811.
  351. ^ Huang W, Rodrigues J, Bilgo E, Tormo JR, Challenger JD, De Cozar-Gallardo C, et al. (August 2023). "Delftia tsuruhatensis TC1 symbiont suppresses malaria transmission by anopheline mosquitoes". Science. 381 (6657): 533–540. Bibcode:2023Sci...381..533H. doi:10.1126/science.adf8141. PMID 37535741.
  352. ^ Offord C (3 August 2023). "Microbe stops mosquitoes from harboring malaria parasite". Science. doi:10.1126/science.adk1267.
  353. ^ "Chance discovery helps fight against malaria". BBC News. 2023-08-04. Archived from the original on 2023-08-04. Retrieved 2023-08-04.
  354. ^ Foster WA (January 1995). "Mosquito sugar feeding and reproductive energetics". Annual Review of Entomology. 40 (1): 443–474. doi:10.1146/annurev.en.40.010195.002303. PMID 7810991.
  355. ^ Gu W, Müller G, Schlein Y, Novak RJ, Beier JC (January 2011). "Natural plant sugar sources of Anopheles mosquitoes strongly impact malaria transmission potential". PLOS ONE. 6 (1): e15996. Bibcode:2011PLoSO...615996G. doi:10.1371/journal.pone.0015996. PMC 3024498. PMID 21283732.
  356. ^ Hien DF, Dabiré KR, Roche B, Diabaté A, Yerbanga RS, Cohuet A, et al. (August 2016). "Plant-Mediated Effects on Mosquito Capacity to Transmit Human Malaria". PLOS Pathogens. 12 (8): e1005773. doi:10.1371/journal.ppat.1005773. PMC 4973987. PMID 27490374.
  357. ^ "Facts about malaria". European Centre for Disease Prevention and Control. 9 June 2017. Archived from the original on 6 July 2021. Retrieved 16 July 2021.
  358. ^ Brasil P, Zalis MG, de Pina-Costa A, Siqueira AM, Júnior CB, Silva S, et al. (October 2017). "Outbreak of human malaria caused by Plasmodium simium in the Atlantic Forest in Rio de Janeiro: a molecular epidemiological investigation". The Lancet Global Health. 5 (10): e1038–e1046. doi:10.1016/S2214-109X(17)30333-9. PMID 28867401.
  359. ^ Rich SM, Ayala FJ (2006). "Evolutionary Origins of Human Malaria Parasites". Malaria: Genetic and Evolutionary Aspects. pp. 125–146. doi:10.1007/0-387-28295-5_6. ISBN 978-0-387-28294-7.
  360. ^ Baird JK (September 2009). "Malaria zoonoses". Travel Medicine and Infectious Disease. 7 (5): 269–277. doi:10.1016/j.tmaid.2009.06.004. PMID 19747661.
  361. ^ Ameri M (March 2010). "Laboratory diagnosis of malaria in nonhuman primates". Veterinary Clinical Pathology. 39 (1): 5–19. doi:10.1111/j.1939-165X.2010.00217.x. PMID 20456124.
  362. ^ Mlambo G, Kumar N (November 2008). "Transgenic rodent Plasmodium berghei parasites as tools for assessment of functional immunogenicity and optimization of human malaria vaccines". Eukaryotic Cell. 7 (11): 1875–1879. doi:10.1128/EC.00242-08. PMC 2583535. PMID 18806208.
  363. ^ Lapointe DA, Atkinson CT, Samuel MD (February 2012). "Ecology and conservation biology of avian malaria". Annals of the New York Academy of Sciences. 1249 (1): 211–226. Bibcode:2012NYASA1249..211L. doi:10.1111/j.1749-6632.2011.06431.x. PMID 22320256.

Sources

[edit]

Further reading

[edit]
  • Barber, Marshall Albert. "The history of malaria in the United States." Public Health Reports (1929): 2575-2587. online
  • Bynum W.F. and C. Overy. The Beast in the Mosquito: The Correspondence of Ronald Ross and Patrick Manson (Rodopi, 1998) ISBN 978-90-420-0721-5
  • Harrison, Gordon. Malaria: Mosquitoes, Malaria and Man. A History of the Hostilities since 1880 (Dutton, 1978), a major scholarly survey.
  • Jarvis B (29 July 2019). "How Mosquitoes Changed Everything". The New Yorker. Archived from the original on 7 August 2019. Retrieved 8 August 2019.
  • Malpede, Maurizio. "Malaria and economic activity: Evidence from US agriculture." American Journal of Agricultural Economics 105.5 (2023): 1516-1542.
  • Watts, Sheldon J. Epidemics and history: disease, power, and imperialism (Yale University Press, 1999) pp213-268, worldwide. online.
[edit]
The offline app allows you to download all of Wikipedia's medical articles in an app to access them when you have no Internet.
Wikipedia's health care articles can be viewed offline with the Medical Wikipedia app.