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In susceptible persons, beryllium exposure can lead to a cell-mediated immune response. The T-cells become sensitized to beryllium. Each subsequent exposure leads to an immune response involving [[T helper cell|CD4+ helper T-lymphocytes]] and [[macrophage]]s accumulating in the lungs. As this response continues macrophages, CD4+ T-lymphocytes and plasma cells aggregate together to form the [[Granuloma|noncaseating granulomas]].<ref>{{Cite journal|last1=Falta|first1=Michael T.|last2=Pinilla|first2=Clemencia|last3=Mack|first3=Douglas G.|last4=Tinega|first4=Alex N.|last5=Crawford|first5=Frances|last6=Giulianotti|first6=Marc|last7=Santos|first7=Radleigh|last8=Clayton|first8=Gina M.|last9=Wang|first9=Yuxiao|date=2013-07-01|title=Identification of beryllium-dependent peptides recognized by CD4+ T cells in chronic beryllium disease|journal=The Journal of Experimental Medicine|language=en|volume=210|issue=7|pages=1403–1418|doi=10.1084/jem.20122426|issn=0022-1007|pmc=3698527|pmid=23797096}}</ref><ref>{{Cite journal|last1=Freiman|first1=D. G.|last2=Hardy|first2=H. L.|date=1970-03-01|title=Beryllium disease. The relation of pulmonary pathology to clinical course and prognosis based on a study of 130 cases from the U.S. beryllium case registry|journal=Human Pathology|volume=1|issue=1|pages=25–44|issn=0046-8177|pmid=5521721|doi=10.1016/S0046-8177(70)80003-X}}</ref> When beryllium is [[Phagocytosis|phagocytized]] by macrophages, the beryllium triggers macrophage apoptosis, thereby reducing beryllium clearance from the lungs and eventually resulting in secondary necrosis and lysis.<ref>{{Cite journal|last1=Sawyer|first1=Richard T.|last2=Maier|first2=Lisa A.|last3=Kittle|first3=Lori A.|last4=Newman|first4=Lee S.|date=February 2002|title=Chronic beryllium disease: a model interaction between innate and acquired immunity|journal=International Immunopharmacology|volume=2|issue=2–3|pages=249–261|issn=1567-5769|doi=10.1016/S1567-5769(01)00177-1|pmid=11811929}}</ref> Eventually, the outcome is [[fibrosis]] of the lung.<ref>{{Cite journal|last1=Saltini|first1=C.|last2=Amicosante|first2=M.|last3=Franchi|first3=A.|last4=Lombardi|first4=G.|last5=Richeldi|first5=L.|date=1998-12-01|title=Immunogenetic basis of environmental lung disease: lessons from the berylliosis model|journal=European Respiratory Journal|language=en|volume=12|issue=6|pages=1463–1475|doi=10.1183/09031936.98.12061463|issn=0903-1936|pmid=9877510|doi-access=free}}</ref><ref name=ATSDRmanagement>Agency for Toxic Substances and Disease Registry via the CDC. [https://www.atsdr.cdc.gov/csem/csem.html Beryllium Toxicity: How Should Patients Exposed to Beryllium Be Treated and Managed?] Page last updated: May 23, 2008</ref> |
In susceptible persons, beryllium exposure can lead to a cell-mediated immune response. The T-cells become sensitized to beryllium. Each subsequent exposure leads to an immune response involving [[T helper cell|CD4+ helper T-lymphocytes]] and [[macrophage]]s accumulating in the lungs. As this response continues macrophages, CD4+ T-lymphocytes and plasma cells aggregate together to form the [[Granuloma|noncaseating granulomas]].<ref>{{Cite journal|last1=Falta|first1=Michael T.|last2=Pinilla|first2=Clemencia|last3=Mack|first3=Douglas G.|last4=Tinega|first4=Alex N.|last5=Crawford|first5=Frances|last6=Giulianotti|first6=Marc|last7=Santos|first7=Radleigh|last8=Clayton|first8=Gina M.|last9=Wang|first9=Yuxiao|date=2013-07-01|title=Identification of beryllium-dependent peptides recognized by CD4+ T cells in chronic beryllium disease|journal=The Journal of Experimental Medicine|language=en|volume=210|issue=7|pages=1403–1418|doi=10.1084/jem.20122426|issn=0022-1007|pmc=3698527|pmid=23797096}}</ref><ref>{{Cite journal|last1=Freiman|first1=D. G.|last2=Hardy|first2=H. L.|date=1970-03-01|title=Beryllium disease. The relation of pulmonary pathology to clinical course and prognosis based on a study of 130 cases from the U.S. beryllium case registry|journal=Human Pathology|volume=1|issue=1|pages=25–44|issn=0046-8177|pmid=5521721|doi=10.1016/S0046-8177(70)80003-X}}</ref> When beryllium is [[Phagocytosis|phagocytized]] by macrophages, the beryllium triggers macrophage apoptosis, thereby reducing beryllium clearance from the lungs and eventually resulting in secondary necrosis and lysis.<ref>{{Cite journal|last1=Sawyer|first1=Richard T.|last2=Maier|first2=Lisa A.|last3=Kittle|first3=Lori A.|last4=Newman|first4=Lee S.|date=February 2002|title=Chronic beryllium disease: a model interaction between innate and acquired immunity|journal=International Immunopharmacology|volume=2|issue=2–3|pages=249–261|issn=1567-5769|doi=10.1016/S1567-5769(01)00177-1|pmid=11811929}}</ref> Eventually, the outcome is [[fibrosis]] of the lung.<ref>{{Cite journal|last1=Saltini|first1=C.|last2=Amicosante|first2=M.|last3=Franchi|first3=A.|last4=Lombardi|first4=G.|last5=Richeldi|first5=L.|date=1998-12-01|title=Immunogenetic basis of environmental lung disease: lessons from the berylliosis model|journal=European Respiratory Journal|language=en|volume=12|issue=6|pages=1463–1475|doi=10.1183/09031936.98.12061463|issn=0903-1936|pmid=9877510|doi-access=free}}</ref><ref name=ATSDRmanagement>Agency for Toxic Substances and Disease Registry via the CDC. [https://www.atsdr.cdc.gov/csem/csem.html Beryllium Toxicity: How Should Patients Exposed to Beryllium Be Treated and Managed?] Page last updated: May 23, 2008</ref> |
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Several studies have shown that there is a genetic component to beryllium sensitivity. Specifically, those beryllium-exposed workers with a mutation at the [[HLA-DPB1]] Glu<sup>69</sup> position have increased prevalence of beryllium sensitization and chronic beryllium disease.<ref name=GeneRev2011>{{cite journal |vauthors=Rosenman KD, Rossman M, Hertzberg V, Reilly MJ, Rice C, Kanterakis E, Monos D |title=HLA class II DPB1 and DRB1 polymorphisms associated with genetic susceptibility to beryllium toxicity |journal=Occup Environ Med |volume=68 |issue=7 |pages=487–93 |year=2011 |pmid=21186201 |doi=10.1136/oem.2010.055046 |s2cid=27610317 }}</ref> The HLA-DPB1 gene is important for [[MHC class II]] molecule function on [[Antigen-presenting cell|antigen presenting cells]].<ref name=GeneRev2011/> A study of the immune response to beryllium in individuals who express the [[HLA-DP2]] allele found that CD4 T-cells do not detect the Be+ cation itself, but instead detect surface changes in the HLA-DP2/peptide complex in which Be+ is embedded. Those researchers concluded that chronic beryllium disease is a predisposition that lies between "[[allergy|allergic hypersensitivity]] and [[autoimmunity]]."<ref name=Cell2014>{{cite journal |vauthors=Clayton GM, Wang Y, Crawford F, Novikov A, Wimberly BT, Kieft JS, Falta MT, Bowerman NA, Marrack P, Fontenot AP, Dai S, Kappler JW |title=Structural Basis of Chronic Beryllium Disease: Linking Allergic Hypersensitivity and Autoimmunity |journal=Cell |volume=158 |issue=1 |pages=132–142 |year=2014 |pmid= 24995984|doi=10.1016/j.cell.2014.04 | |
Several studies have shown that there is a genetic component to beryllium sensitivity. Specifically, those beryllium-exposed workers with a mutation at the [[HLA-DPB1]] Glu<sup>69</sup> position have increased prevalence of beryllium sensitization and chronic beryllium disease.<ref name=GeneRev2011>{{cite journal |vauthors=Rosenman KD, Rossman M, Hertzberg V, Reilly MJ, Rice C, Kanterakis E, Monos D |title=HLA class II DPB1 and DRB1 polymorphisms associated with genetic susceptibility to beryllium toxicity |journal=Occup Environ Med |volume=68 |issue=7 |pages=487–93 |year=2011 |pmid=21186201 |doi=10.1136/oem.2010.055046 |s2cid=27610317 }}</ref> The HLA-DPB1 gene is important for [[MHC class II]] molecule function on [[Antigen-presenting cell|antigen presenting cells]].<ref name=GeneRev2011/> A study of the immune response to beryllium in individuals who express the [[HLA-DP2]] allele found that CD4 T-cells do not detect the Be+ cation itself, but instead detect surface changes in the HLA-DP2/peptide complex in which Be+ is embedded. Those researchers concluded that chronic beryllium disease is a predisposition that lies between "[[allergy|allergic hypersensitivity]] and [[autoimmunity]]."<ref name=Cell2014>{{cite journal |vauthors=Clayton GM, Wang Y, Crawford F, Novikov A, Wimberly BT, Kieft JS, Falta MT, Bowerman NA, Marrack P, Fontenot AP, Dai S, Kappler JW |title=Structural Basis of Chronic Beryllium Disease: Linking Allergic Hypersensitivity and Autoimmunity |journal=Cell |volume=158 |issue=1 |pages=132–142 |year=2014 |pmid= 24995984|doi=10.1016/j.cell.2014.04.048 |pmc=4269484 |s2cid= |quote="Individuals carrying the MHCII allele, HLA-DP2, are at risk for chronic beryllium disease (CBD), a debilitating inflammatory lung condition caused by the reaction of CD4 T cells to inhaled beryllium."}}</ref> |
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According to the [[International Agency for Research on Cancer]], beryllium and beryllium compounds are [[List of IARC Group 1 carcinogens|Category 1 carcinogens]]; they are carcinogenic to both animals and humans.<ref>{{Cite web|url = http://www.inchem.org/documents/iarc/vol58/mono58-1.html|publisher = International Agency for Research on Cancer|title = IARC Monograph, Volume 58|year = 1993|access-date = 2008-09-18}}</ref> |
According to the [[International Agency for Research on Cancer]], beryllium and beryllium compounds are [[List of IARC Group 1 carcinogens|Category 1 carcinogens]]; they are carcinogenic to both animals and humans.<ref>{{Cite web|url = http://www.inchem.org/documents/iarc/vol58/mono58-1.html|publisher = International Agency for Research on Cancer|title = IARC Monograph, Volume 58|year = 1993|access-date = 2008-09-18}}</ref> |
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The radiologic and pathologic features of berylliosis are very similar to sarcoidosis. Due to the strong clinical and histopathological resemblance of sarcoidosis and berylliosis, patients are sometimes misdiagnosed with sarcoidosis until the history of exposure to beryllium is elicited and beryllium hypersensitivity demonstrated with specific testing. Some studies suggest that up to 6% of all cases of sarcoidosis are actually berylliosis.<ref>{{cite journal |last1=Rossman |first1=MD |last2=Kreider |first2=ME |date=June 2003 |title=Is chronic beryllium disease sarcoidosis of known etiology? |journal=Sarcoidosis, Vasculitis and Diffuse Lung Diseases |volume=20 |issue=2 |pages=104–9 |pmid=12870719}}</ref> <ref>{{Cite journal |last1=Cheva |first1=Angeliki |last2=Kilmpasani |first2=Maria |last3=Stathakis |first3=Eustathios |last4=Dimitriadis |first4=Ioannis |last5=Mpikos |first5=Vasileios |last6=Papaemmanouil |first6=Styliani |date=November 2016 |title=AB042. Sarcoidosis or Berylliosis? Two diseases with similar histologic findings |journal=Annals of Translational Medicine |volume=4 |issue=22 |pages=AB042 |doi=10.21037/atm.2016.AB042 |issn=2305-5839 |pmc=5159372 |doi-access=free }}</ref> |
The radiologic and pathologic features of berylliosis are very similar to sarcoidosis. Due to the strong clinical and histopathological resemblance of sarcoidosis and berylliosis, patients are sometimes misdiagnosed with sarcoidosis until the history of exposure to beryllium is elicited and beryllium hypersensitivity demonstrated with specific testing. Some studies suggest that up to 6% of all cases of sarcoidosis are actually berylliosis.<ref>{{cite journal |last1=Rossman |first1=MD |last2=Kreider |first2=ME |date=June 2003 |title=Is chronic beryllium disease sarcoidosis of known etiology? |journal=Sarcoidosis, Vasculitis and Diffuse Lung Diseases |volume=20 |issue=2 |pages=104–9 |pmid=12870719}}</ref> <ref>{{Cite journal |last1=Cheva |first1=Angeliki |last2=Kilmpasani |first2=Maria |last3=Stathakis |first3=Eustathios |last4=Dimitriadis |first4=Ioannis |last5=Mpikos |first5=Vasileios |last6=Papaemmanouil |first6=Styliani |date=November 2016 |title=AB042. Sarcoidosis or Berylliosis? Two diseases with similar histologic findings |journal=Annals of Translational Medicine |volume=4 |issue=22 |pages=AB042 |doi=10.21037/atm.2016.AB042 |issn=2305-5839 |pmc=5159372 |doi-access=free }}</ref> |
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The beryllium lymphocyte proliferation test (BeLPT) is the standard way of determining sensitivity to beryllium.<ref name=":02">{{Cite journal|last1=Balmes|first1=John R.|last2=Abraham|first2=Jerrold L.|last3=Dweik|first3=Raed A.|last4=Fireman|first4=Elizabeth|last5=Fontenot|first5=Andrew P.|last6=Maier|first6=Lisa A.|last7=Muller-Quernheim|first7=Joachim|last8=Ostiguy|first8=Gaston|last9=Pepper|first9=Lewis D.|title=An Official American Thoracic Society Statement: Diagnosis and Management of Beryllium Sensitivity and Chronic Beryllium Disease|journal=American Journal of Respiratory and Critical Care Medicine|volume=190|issue=10|pages=e34–e59|doi=10.1164/rccm.201409-1722st|pmid=25398119|year=2014}}</ref> The test is performed by acquiring either peripheral blood or fluid from a bronchial alveolar lavage, and lymphocytes are cultured with beryllium sulfate. Cells are then counted and those with elevated number of cells are considered abnormal.<ref>{{Cite journal|last1=Frome|first1=Edward L|last2=Newman|first2=Lee S|last3=Cragle|first3=Donna L|last4=Colyer|first4=Shirley P|last5=Wambach|first5=Paul F|date=2003-02-01|title=Identification of an abnormal beryllium lymphocyte proliferation test|journal=Toxicology|volume=183|issue=1–3|pages=39–56|doi=10.1016/S0300-483X(02)00439-0|pmid=12504341|url=https://zenodo.org/record/1259989}}</ref> Those exposed persons with two abnormal BeLPT tested with peripheral blood, or one abnormal and one borderline result, are considered beryllium sensitized. Also, those with one abnormal BeLPT tested with fluid from a bronchial alveolar lavage are considered sensitized.<ref name=":02" /> |
The beryllium lymphocyte proliferation test (BeLPT) is the standard way of determining sensitivity to beryllium.<ref name=":02">{{Cite journal|last1=Balmes|first1=John R.|last2=Abraham|first2=Jerrold L.|last3=Dweik|first3=Raed A.|last4=Fireman|first4=Elizabeth|last5=Fontenot|first5=Andrew P.|last6=Maier|first6=Lisa A.|last7=Muller-Quernheim|first7=Joachim|last8=Ostiguy|first8=Gaston|last9=Pepper|first9=Lewis D.|title=An Official American Thoracic Society Statement: Diagnosis and Management of Beryllium Sensitivity and Chronic Beryllium Disease|journal=American Journal of Respiratory and Critical Care Medicine|volume=190|issue=10|pages=e34–e59|doi=10.1164/rccm.201409-1722st|pmid=25398119|year=2014}}</ref> The test is performed by acquiring either peripheral blood or fluid from a bronchial alveolar lavage, and lymphocytes are cultured with beryllium sulfate. Cells are then counted and those with elevated number of cells are considered abnormal.<ref>{{Cite journal|last1=Frome|first1=Edward L|last2=Newman|first2=Lee S|last3=Cragle|first3=Donna L|last4=Colyer|first4=Shirley P|last5=Wambach|first5=Paul F|date=2003-02-01|title=Identification of an abnormal beryllium lymphocyte proliferation test|journal=Toxicology|volume=183|issue=1–3|pages=39–56|doi=10.1016/S0300-483X(02)00439-0|pmid=12504341|bibcode=2003Toxgy.183...39F |url=https://zenodo.org/record/1259989}}</ref> Those exposed persons with two abnormal BeLPT tested with peripheral blood, or one abnormal and one borderline result, are considered beryllium sensitized. Also, those with one abnormal BeLPT tested with fluid from a bronchial alveolar lavage are considered sensitized.<ref name=":02" /> |
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Chest radiography findings of berylliosis are non-specific. Early in the disease radiography findings are usually normal. In later stages interstitial fibrosis, pleural irregularities, hilar [[lymphadenopathy]] and [[Ground-glass opacity|ground-glass opacities]] have been reported.<ref>{{Cite journal|last1=Aronchick|first1=J. M.|last2=Rossman|first2=M. D.|last3=Miller|first3=W. T.|date=1987-06-01|title=Chronic beryllium disease: diagnosis, radiographic findings, and correlation with pulmonary function tests|journal=Radiology|volume=163|issue=3|pages=677–682|doi=10.1148/radiology.163.3.3575713|issn=0033-8419|pmid=3575713}}</ref><ref name=Sharma>{{Cite journal|last1=Sharma|first1=Nidhi|last2=Patel|first2=Jeet|last3=Mohammed|first3=Tan-Lucien H.|title=Chronic Beryllium Disease|journal=Journal of Computer Assisted Tomography|volume=34|issue=6|pages=945–948|doi=10.1097/rct.0b013e3181ef214e|pmid=21084914|year=2010}}</ref> Findings on CT are also not specific to berylliosis. Findings that are common in CT scans of people with berylliosis include parenchymal nodules in early stages. One study found that ground-glass opacities were more commonly seen on CT scan in berylliosis than in sarcoidosis. In later stages hilar lymphadenopathy, interstitial pulmonary fibrosis and pleural thickening.<ref name=Sharma /> |
Chest radiography findings of berylliosis are non-specific. Early in the disease radiography findings are usually normal. In later stages interstitial fibrosis, pleural irregularities, hilar [[lymphadenopathy]] and [[Ground-glass opacity|ground-glass opacities]] have been reported.<ref>{{Cite journal|last1=Aronchick|first1=J. M.|last2=Rossman|first2=M. D.|last3=Miller|first3=W. T.|date=1987-06-01|title=Chronic beryllium disease: diagnosis, radiographic findings, and correlation with pulmonary function tests|journal=Radiology|volume=163|issue=3|pages=677–682|doi=10.1148/radiology.163.3.3575713|issn=0033-8419|pmid=3575713}}</ref><ref name=Sharma>{{Cite journal|last1=Sharma|first1=Nidhi|last2=Patel|first2=Jeet|last3=Mohammed|first3=Tan-Lucien H.|title=Chronic Beryllium Disease|journal=Journal of Computer Assisted Tomography|volume=34|issue=6|pages=945–948|doi=10.1097/rct.0b013e3181ef214e|pmid=21084914|year=2010}}</ref> Findings on CT are also not specific to berylliosis. Findings that are common in CT scans of people with berylliosis include parenchymal nodules in early stages. One study found that ground-glass opacities were more commonly seen on CT scan in berylliosis than in sarcoidosis. In later stages hilar lymphadenopathy, interstitial pulmonary fibrosis and pleural thickening.<ref name=Sharma /> |
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==Prevention== |
==Prevention== |
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Typical levels of beryllium that industries may release into the air are of the order of {{nowrap|0.01 µg/m<sup>3</sup>}}, averaged over a 30-day period, or {{nowrap|2 µg/m<sup>3</sup>}} of workroom air for an 8-hour work shift. Compliance with the current U.S. [[Occupational Safety and Health Administration]] (OSHA) [[permissible exposure limit]] for beryllium of {{nowrap|2 µg/m<sup>3</sup>}} has been determined to be inadequate to protect workers from developing beryllium sensitization and chronic beryllium disease. The [[American Conference of Governmental Industrial Hygienists]] (ACGIH), which is an independent organization of experts in the field of occupational health, has proposed a threshold limit value (TLV) of {{nowrap|0.05 µg/m<sup>3</sup>}} in a 2006 Notice of Intended Change (NIC). This TLV is 40 times lower than the current OSHA permissible exposure limit, reflecting the ACGIH analysis of best available peer-reviewed research data concerning how little airborne beryllium is required to cause sensitization and chronic beryllium disease.{{Citation needed|date = August 2015}} |
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Because it can be difficult to control industrial exposures to beryllium, it is advisable to use any methods possible to reduce airborne and surface contamination by beryllium, to minimize the use of beryllium and beryllium-containing alloys whenever possible, and to educate people about the potential hazards if they are likely to encounter beryllium dust or fumes.<ref name="Lang">{{Cite journal|journal=Environmental Health Perspectives|volume=102|issue=6–7|date=June–July 1994|title=Beryllium: A Chronic Problem|author=Lang, Leslie|pmc=1569745|pmid=9679108|pages=526–31|doi=10.1289/ehp.94102526}}</ref> It is important to damp wipe [[metallographic]] preparation equipment to prevent accumulation of dry particles. Sectioning, grinding, and polishing must be performed under sufficiently vented hoods equipped with special filters.<ref>Batich, Ray and James M. Marder. (1985) Beryllium In (Ed. 9), Metals Handbook: Metallography and Microstructures (pp. 389–391). Metals Park, Ohio: American Society for Metals.</ref> |
Because it can be difficult to control industrial exposures to beryllium, it is advisable to use any methods possible to reduce airborne and surface contamination by beryllium, to minimize the use of beryllium and beryllium-containing alloys whenever possible, and to educate people about the potential hazards if they are likely to encounter beryllium dust or fumes.<ref name="Lang">{{Cite journal|journal=Environmental Health Perspectives|volume=102|issue=6–7|date=June–July 1994|title=Beryllium: A Chronic Problem|author=Lang, Leslie|pmc=1569745|pmid=9679108|pages=526–31|doi=10.1289/ehp.94102526}}</ref> It is important to damp wipe [[metallographic]] preparation equipment to prevent accumulation of dry particles. Sectioning, grinding, and polishing must be performed under sufficiently vented hoods equipped with special filters.<ref>Batich, Ray and James M. Marder. (1985) Beryllium In (Ed. 9), Metals Handbook: Metallography and Microstructures (pp. 389–391). Metals Park, Ohio: American Society for Metals.</ref> |
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Latest revision as of 04:21, 2 November 2024
Berylliosis | |
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Other names | Chronic beryllium disease (CBD) |
Peribronchal non-necrotizing granuloma from berylliosis | |
Specialty | Pulmonology |
Berylliosis, or chronic beryllium disease (CBD), is a chronic allergic-type lung response and chronic lung disease caused by exposure to beryllium and its compounds, a form of beryllium poisoning. It is distinct from acute beryllium poisoning, which became rare following occupational exposure limits established around 1950.[1] Berylliosis is an occupational lung disease.
While there is no cure, symptoms can be treated.[2]
Signs and symptoms
[edit]With single or prolonged exposure by inhalation the lungs may become sensitized to beryllium. Berylliosis has a slow onset and progression. Some people who are sensitized to beryllium may not have symptoms.[1] Continued exposure causes the development of small inflammatory nodules, called granulomas.[3] Of note, the authors of a 2006 study suggested that beryllium inhalation was not the only form of exposure and perhaps skin exposure was also a cause, as they found that a reduction in beryllium inhalation did not result in a reduction in chronic beryllium disease or beryllium sensitization.[4]
Granuloma formation is seen in other diseases such as tuberculosis and sarcoidosis. Sarcoidosis, like berylliosis, also produces granulomas without a necrotic core, and so distinction between the two processes can be difficult.
Ultimately, this process leads to restrictive lung disease (a decrease in diffusion capacity).
The earliest symptoms are typically cough and shortness of breath.[5] Other symptoms include chest pain, joint aches, weight loss, and fever.
Rarely, one can get granulomas in other organs including the liver.
The onset of symptoms can range from weeks up to tens of years from the initial exposure. In some individuals, a single exposure to beryllium can cause berylliosis.
Pathogenesis
[edit]In susceptible persons, beryllium exposure can lead to a cell-mediated immune response. The T-cells become sensitized to beryllium. Each subsequent exposure leads to an immune response involving CD4+ helper T-lymphocytes and macrophages accumulating in the lungs. As this response continues macrophages, CD4+ T-lymphocytes and plasma cells aggregate together to form the noncaseating granulomas.[6][7] When beryllium is phagocytized by macrophages, the beryllium triggers macrophage apoptosis, thereby reducing beryllium clearance from the lungs and eventually resulting in secondary necrosis and lysis.[8] Eventually, the outcome is fibrosis of the lung.[9][10]
Several studies have shown that there is a genetic component to beryllium sensitivity. Specifically, those beryllium-exposed workers with a mutation at the HLA-DPB1 Glu69 position have increased prevalence of beryllium sensitization and chronic beryllium disease.[11] The HLA-DPB1 gene is important for MHC class II molecule function on antigen presenting cells.[11] A study of the immune response to beryllium in individuals who express the HLA-DP2 allele found that CD4 T-cells do not detect the Be+ cation itself, but instead detect surface changes in the HLA-DP2/peptide complex in which Be+ is embedded. Those researchers concluded that chronic beryllium disease is a predisposition that lies between "allergic hypersensitivity and autoimmunity."[12]
According to the International Agency for Research on Cancer, beryllium and beryllium compounds are Category 1 carcinogens; they are carcinogenic to both animals and humans.[13]
Diagnosis
[edit]The differential diagnosis for berylliosis includes:[14]
- Sarcoidosis
- Granulomatous lung diseases
- Tuberculosis
- Fungal infections (e.g., histoplasmosis)
- Granulomatosis with polyangiitis
- Idiopathic pulmonary fibrosis
- Hypersensitivity pneumonitis
- Asthma
Diagnosis of berylliosis is based on history of beryllium exposures, documented beryllium sensitivity, and granulomatous inflammation on lung biopsy. Given the invasive nature of a lung biopsy, diagnosis can also be based on clinical history consistent with berylliosis, abnormal chest x-ray or CT scan findings, and abnormalities in pulmonary function tests.[15]
The radiologic and pathologic features of berylliosis are very similar to sarcoidosis. Due to the strong clinical and histopathological resemblance of sarcoidosis and berylliosis, patients are sometimes misdiagnosed with sarcoidosis until the history of exposure to beryllium is elicited and beryllium hypersensitivity demonstrated with specific testing. Some studies suggest that up to 6% of all cases of sarcoidosis are actually berylliosis.[16] [17]
The beryllium lymphocyte proliferation test (BeLPT) is the standard way of determining sensitivity to beryllium.[15] The test is performed by acquiring either peripheral blood or fluid from a bronchial alveolar lavage, and lymphocytes are cultured with beryllium sulfate. Cells are then counted and those with elevated number of cells are considered abnormal.[18] Those exposed persons with two abnormal BeLPT tested with peripheral blood, or one abnormal and one borderline result, are considered beryllium sensitized. Also, those with one abnormal BeLPT tested with fluid from a bronchial alveolar lavage are considered sensitized.[15]
Chest radiography findings of berylliosis are non-specific. Early in the disease radiography findings are usually normal. In later stages interstitial fibrosis, pleural irregularities, hilar lymphadenopathy and ground-glass opacities have been reported.[19][20] Findings on CT are also not specific to berylliosis. Findings that are common in CT scans of people with berylliosis include parenchymal nodules in early stages. One study found that ground-glass opacities were more commonly seen on CT scan in berylliosis than in sarcoidosis. In later stages hilar lymphadenopathy, interstitial pulmonary fibrosis and pleural thickening.[20]
Classification
[edit]Berylliosis is an occupational disease.[1] Relevant occupations are those where beryllium is mined, processed or converted into metal alloys, or where machining of metals containing beryllium and recycling of scrap alloys occurs.[21] It is associated with aerospace manufacturing, microwave semiconductor electronics, beryllium mining or manufacturing of fluorescent light bulbs (which once contained beryllium compounds in their internal phosphor coating).[22][23][24] Beryllia was used in lamp manufacture because of ceramic's obvious virtues for insulation and heat resistance, and also because beryllia could be made transparent.[25] Certain welding anodes along with other electrical contacts and even non-sparking tools are made of beryllium copper alloy and the subsequent machining of such materials would cause the disease as well.
Prevention
[edit]Because it can be difficult to control industrial exposures to beryllium, it is advisable to use any methods possible to reduce airborne and surface contamination by beryllium, to minimize the use of beryllium and beryllium-containing alloys whenever possible, and to educate people about the potential hazards if they are likely to encounter beryllium dust or fumes.[26] It is important to damp wipe metallographic preparation equipment to prevent accumulation of dry particles. Sectioning, grinding, and polishing must be performed under sufficiently vented hoods equipped with special filters.[27]
On 29 January 2009, the Los Alamos National Laboratory announced it was notifying nearly 2,000 current and former employees and visitors that they may have been exposed to beryllium in the lab and may be at risk of disease. Concern over possible exposure to the material was first raised in November 2008, when a box containing beryllium was received at the laboratory's short-term storage facility.[28]
Treatment
[edit]There is no cure for berylliosis; the goals of treatment are to reduce symptoms and slow the progression of disease.[10][29]
Although the evidence that stopping exposure to beryllium decreases progression of the disease is limited,[30] it is still considered to be an accepted approach to treatment in any stage of disease.[31]
People with early stages of disease, without lung function abnormalities or clinical symptoms, are periodically monitored with physical exams, pulmonary function testing and radiography.[29]
Once clinical symptoms or significant abnormalities in pulmonary function testing appear, treatments include oxygen and oral corticosteroids and whatever supportive therapy is required.[1][15][29]
Outcomes
[edit]Overall mortality rates are 5–38%.[32]
Epidemiology
[edit]The number of workers in the United States exposed to beryllium vary but has been estimated to be as high as 800,000 during the 1960s and 1970s.[33] A more recent study from 2004 estimated the number of exposed workers in the United States to be around 134,000.[34]
The rate of workers becoming sensitized to beryllium varies based on genetics and exposure levels. In one study researchers found the prevalence of beryllium sensitization to range from 9–19% depending on the industry.[35] Many workers who are found to be sensitive to beryllium also meet the diagnostic criteria for chronic beryllium disease.[35] In one study of nuclear workers, among those who were sensitized to beryllium, 66% were found to have chronic beryllium disease as well.[36] The rate of progression from beryllium sensitization to chronic beryllium disease has been estimated to be approximately 6–8% per year.[30][37] Stopping exposure to beryllium in those sensitized has not been definitively shown to stop the progression to chronic beryllium disease.[30]
The overall prevalence of chronic beryllium disease among workers exposed to beryllium has ranged from 1–5% depending on industry and time period of study.[35][36][38]
The general population is unlikely to develop acute or chronic beryllium disease because ambient air levels of beryllium are normally very low (<0.03 ng/m3).[39] However, a study found 1% of people living within 3/4 of a mile of a beryllium plant in Lorain, Ohio, had berylliosis after exposure to concentrations estimated to be less than 1 milligram per cubic metre of air. In the United States the Beryllium Case Registry contained 900 records, early cases relating to extraction and fluorescent lamp manufacture, later ones coming from the aerospace, ceramics and metallurgical industries.[40][41]
History
[edit]Since the 1920s, beryllium has been used in electronics, ceramics, research and development labs, aircraft, and the atomic energy and defense industry.[26] Cases of bronchitis and pneumonia-like symptoms were reported in Germany and Russia in the 1930s among workers mining and refining beryllium. By 1946, a cluster of cases associated with fluorescent lamp manufacturers were apparent in the United States, and the lamp industry stopped using beryllium in 1949.[31] At that time, most construction trades and industries were unaware of the potential risks associated with beryllium exposure.[42]
It occasionally killed early workers in nuclear weapons design, such as Herbert L. Anderson.[43]
Beryllium sensitivity testing was first performed as a cutaneous beryllium patch test in the early 1950s, but was discontinued due to the test stimulating sensitization or aggravating existing chronic beryllium disease.[44]: 115
In the 1990s, the DOE began screening employees using the BeLPT test in facilities where beryllium was used, to take preventive measures against beryllium exposure. Somewhat alarmingly, clerical staff who were never involved in handling the material had developed asymptomatic sensitivities.[45]
References
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Individuals carrying the MHCII allele, HLA-DP2, are at risk for chronic beryllium disease (CBD), a debilitating inflammatory lung condition caused by the reaction of CD4 T cells to inhaled beryllium.
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- ^ a b Kreiss, K.; Mroz, M. M.; Zhen, B.; Martyny, J. W.; Newman, L. S. (1993-10-01). "Epidemiology of beryllium sensitization and disease in nuclear workers". The American Review of Respiratory Disease. 148 (4 Pt 1): 985–991. doi:10.1164/ajrccm/148.4_Pt_1.985. ISSN 0003-0805. PMID 8214955.
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External links
[edit]- ATSDR Case Studies in Environmental Medicine: Beryllium Toxicity U.S. Department of Health and Human Services
- CDC – Research on Beryllium Sensitization and Chronic Beryllium Disease – NIOSH Workplace Safety and Health Topic
- Beryllium Network
- Health-cares.net
- Instant insight from the Royal Society of Chemistry examining the molecular basis of chronic beryllium disease
- Rosner, David; Markowitz, Gerald E. (February 1987). "Ch. 7: Salem Sarcoid:The Origins of Beryllium Disease". Dying for work: workers' safety and health in twentieth-century America. Indiana University Press. pp. 103–. ISBN 978-0-253-31825-1.