Abstract

Main

The adverse effects of obesity are well known to healthcare professionals and persons who live with this chronic disease^1–4, as are the benefits of weight reduction. Decreasing baseline body weight by 5–10% reduces the likelihood of developing type2 diabetes while also improving cardiometabolic risk factors (for example, blood pressure) and other obesity-related complications (for example, osteoarthritis)^5–8.

Intensive lifestyle intervention is recommended as the cornerstone of obesity management^3,5,8–10. It consists of a reduced-calorie diet (for example, 1,200–1,500kcalper day based on weight or sex), physical activity (≥150min per week) and frequent behavioral counseling (for example, ≥14sessions over 6months), and induces mean reductions of 5–8% of baseline weight with accompanying improvements in health⁵. Its overall effectiveness, however, is limited by two factors. Large weight reductions are critical for achieving optimal control of obesity-related complications (for example, obstructive sleep apnea and nonalcoholic steatohepatitis)^6–8 and decreasing cardiovascular mortality^11–14, but <20% of patients treated with lifestyle interventions lose ≥15% of baseline weight¹⁵. Patients also regain one-third of lost weight in the year following treatment, with increasing weight regain over time^5,16. Weight regain after diet and exercise intervention is attributable, in part, to persistent metabolic adaptations in which patients’ hunger hormones increase, satiety hormones decrease and energy expenditure declines out of proportion to the amount of weight lost^17–19 such that an even lower energy intake is needed to maintain the weight-reduced state.

New incretin-based, antiobesity medications could bolster the results of intensive lifestyle intervention²⁰. Semaglutide 2.4mg is a glucagon-like peptide-1 (GLP-1) receptor agonist, originally approved at a lower dose for control of type2 diabetes and which, in persons with obesity or overweight (but not diabetes), reduces baseline body weight by 15% at up to 2years (versus 2–3% for placebo)^21,22. It decreases energy intake principally by modification of hunger and satiety signaling in select neural regions²¹. Tirzepatide is a single molecule that combines glucose-dependent insulinotropic polypeptide and GLP-1 receptor agonism²³ to exert synergistic effects on appetite (for example, hunger and satiety), energy intake and metabolic function^24–26. It is approved in many geographies including the USA, European Union and Japan as a once-weekly subcutaneous injectable for type2 diabetes and is currently under review for chronic weight management^26–28. In the SURMOUNT-1 trial, patients with obesity or overweight (but not diabetes) who received tirzepatide 15mg, with monthly brief lifestyle counseling, lost 20.9% of baseline weight at 72weeks (versus 3.1% for placebo) with accompanying reductions in cardiometabolic risk factors²⁷.

Expert panels have suggested the use of antiobesity medications following intensive lifestyle intervention to induce additional weight reduction (which may be needed to achieve optimal control of obesity-related complications) or, at a minimum, to prevent weight regain^5,7,9,10. The present trial evaluated the efficacy of tirzepatide at 72weeks postrandomization in adults with obesity or overweight (but not diabetes) who successfully lost ≥5% of baseline weight during a 12-week lead-in period that provided intensive lifestyle intervention.

Results

Patient disposition

Intensive lifestyle intervention lead-in period

A total of 972participants were assessed for eligibility at screening, of whom 806 were enrolled into the 12-week intensive lifestyle intervention lead-in period (Fig. ​(Fig.1).1). The first participant was enrolled on 12April 2021 and the last on 3September 2021. The key demographics and clinical characteristics of these participants have previously been published²⁸.

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Fig. 1

Trial profile.

SURMOUNT-3 CONSORT flow diagram. MTD, maximum tolerated dose (10 or 15mg). TZP, tirzepatide.

Of the 806participants enrolled, 579 (71.8%) who achieved ≥5% weight reduction at the end of the lead-in period and were otherwise eligible to proceed to the next phase of the study were randomized to either tirzepatide maximum tolerated dose (MTD, n=287) or placebo (n=292) (Fig. ​(Fig.1).1). Mean body weight and body mass index (BMI) in these 579participants decreased from 109.5kg and 38.6kg/m², respectively, at screening to 101.9kg and 35.9kg/m², respectively, at randomization, representing an average 6.9% reduction in body weight after the 12-week intensive lifestyle intervention (Table ​(Table1).1). Weight reduction during lead-in was accompanied by reductions in waist circumference, systolic and diastolic blood pressure, glycated hemoglobinA_1c (HbA_1c), fasting glucose and fasting insulin. There were mean improvements in all lipid levels, except for high-density lipoprotein (HDL) cholesterol and free fatty acids (Table ​(Table11).

Table 1

Clinical characteristics and changes during intensive lifestyle intervention lead-in period

	Mean (s.d.)
	Tirzepatide MTD (n=287)			Placebo (n=292)			Total (n=579)
	Start of intensive lifestyle intervention lead-in	Start of double-blind treatment period (randomization)	Change during lead-in	Start of intensive lifestyle intervention lead-in	Start of double-blind treatment period (randomization)	Change during lead-in	Start of intensive lifestyle intervention lead-in	Start of double-blind treatment period (randomization)	Change during lead-in
Body weight, kg	110.1 (23.9)	102.5 (22.1)	−7.6 (2.9) kg −6.9 (1.9)%	108.9 (22.2)	101.3 (20.7)	−7.6 (2.8) kg −7.0 (2.0)%	109.5 (23.0)	101.9 (21.4)	−7.6 (2.9) kg −6.9 (2.0)%
BMI, kg/m2	38.7 (6.6)	36.1 (6.1)	−2.7 (0.9)	38.4 (6.8)	35.7 (6.4)	−2.7 (0.9)	38.6 (6.7)	35.9 (6.3)	−2.7 (0.9)
Waist circumference, cm	115.9 (15.6)	109.3 (15.2)	−6.6 (5.4)	116.3 (15.3)	109.6 (15.1)	−6.7 (4.9)	116.1 (15.4)	109.4 (15.0)	−6.7 (5.2)
Blood pressure, mmHg
Systolic	125.9 (12.7)	121.4 (12.7)	−4.5 (11.4)	126.0 (13.3)	120.5 (12.4)	−5.4 (11.3)	126.0 (13.0)	121.0 (12.6)	−5.0 (11.4)
Diastolic	81.8 (8.5)	79.1 (8.9)	−2.6 (8.1)	81.2 (8.4)	78.1 (9.2)	−3.1 (8.2)	81.5 (8.5)	78.6 (9.1)	−2.9 (8.1)
Pulse rate, beats permin	73.4 (10.0)	72.0 (10.8)	−1.4 (10.2)	72.2 (9.9)	70.4 (10.3)	−1.8 (9.1)	72.8 (9.9)	71.2 (10.6)	−1.6 (9.6)
HbA1c, %	5.5 (0.4)	5.3 (0.4)	−0.1 (0.3)	5.5 (0.4)	5.4 (0.4)	−0.1 (0.3)	5.5 (0.4)	5.4 (0.4)	−0.1 (0.3)
Fasting glucose, mgdl−1	95.7 (9.9)	92.6 (11.3)	−3.1 (10.1)	94.0 (8.8)	91.3 (9.4)	−2.8 (10.0)	94.9 (9.4)	91.9 (10.4)	−2.9 (10.0)
Fasting insulin, mIUl−1	97.7 (75.3)	70.7 (59.0)	−18.5 (52.9)%	93.6 (87.7)	62.9 (44.4)	−22.3 (41.3)%	95.6 (81.7)	66.7 (52.2)	−20.4 (47.4)%
Lipid level, mgdl−1
Total cholesterol	191.4 (36.8)	185.2 (37.2)	−2.5 (13.7)%	196.2 (39.0)	185.3 (38.2)	−4.9 (12.1)%	193.8 (38.0)	185.3 (37.6)	−3.7 (13.0)%
Non-HDL cholesterol	141.9 (35.8)	136.7 (35.6)	−2.3 (18.1)%	145.6 (37.5)	135.90 (35.7)	−5.5 (15.4)%	143.7 (36.7)	136.3 (35.6)	−3.9 (16.8)%
HDL cholesterol	49.6 (14.0)	48.4 (12.7)	−0.8 (13.9)%	50.6 (13.8)	49.3 (12.9)	−1.5 (13.4)%	50.1 (13.9)	48.9 (12.8)	−1.2 (13.7)%
LDL cholesterol	113.7 (30.4)	112.5 (32.5)	0.8 (24.3)%	118.0 (32.4)	112.3 (32.3)	−3.6 (18.2)%	115.9 (31.5)	112.4 (32.4)	−1.4 (21.5)%
VLDL cholesterol	60.3 (27.2)	54.4 (21.7)	−3.8 (33.1)%	62.1 (30.9)	54.2 (24.4)	−5.5 (34.3)%	61.2 (29.1)	54.3 (23.1)	−4.7 (33.7)%
Triglycerides	141.2 (112.3)	121.4 (55.7)	−4.4 (33.4)%	138.2 (73.5)	118.6 (53.3)	−6.0 (34.1)%	139.7 (94.7)	120.0 (54.5)	−5.2 (33.8)%
Free fatty acids, mEql−1	0.6 (0.2)	0.6 (0.3)	23.0 (82.0)%	0.5 (0.2)	0.6 (0.2)	29.9 (86.3)%	0.5 (0.2)	0.6 (0.2)	26.5 (84.2)%
eGFR, mlmin−11.73m−2	99.0 (17.1)	95.6 (17.1)	−3.4 (10.4)	100.3 (15.7)	97.1 (16.7)	−3.3 (8.9)	99.6 (16.4)	96.4 (16.9)	−3.3 (9.7)
Patient-reported outcomes
SF-36v2 physical functioning domain scorea	48.9 (7.8)	51.7 (6.7)	2.7 (7.7)	48.6 (7.8)	51.7 (6.8)	3.1 (5.8)	48.8 (7.8)	51.7 (6.7)	2.9 (6.8)
IWQOL-Lite-CT physical function composite scoreb	59.5 (22.7)	73.4 (21.3)	13.9 (17.6)	57.4 (24.3)	71.4 (22.0)	13.9 (17.7)	58.4 (23.5)	72.4 (21.6)	13.9 (17.7)

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eGFR, estimated glomerular filtration rate; HDL-C, high-density lipoprotein cholesterol; IWQOL-Lite-CT, Impact of Weight on Quality of Life-Lite-Clinical Trials Version; LDL-C, low-density lipoprotein cholesterol; SF-36v2, Short Form-36v.2 Health Survey acute form; VLDL-C, very-low-density lipoprotein cholesterol.

^aSF-36v2 measures health-related quality of life and general health status. SF-36v2 scores are norm based—that is, scores are transformed to a scale in which the 2009 US general population has a mean score of 50 and s.d. of 10. An increase in score represents an improvement in health status.

^bIWQOL-Lite-CT measures weight-specific, health-related quality of life. All items are rated on either a five-point frequency scale (‘never’ to ‘always’) or a five-point truth scale (‘not at all true’ to ‘completely true’). Scores are transformed to a scale of 0–100, with higher scores reflecting better levels of functioning.

Tirzepatide versus placebo postrandomization

The majority of the 579randomized participants were white (86.0%) and female (62.9%), with an overall mean age of 45.6years (Table ​(Table2).2). The average duration of obesity was 15.1years, and 66.1% had a medical history of one or more obesity-related complications. Demographics and clinical characteristics at randomization (week0), as well as weight reduction and cardiometabolic changes during the lead-in period, were similar across the tirzepatide MTD (10 or 15mg) and placebo groups (Tables ​(Tables11 and ​and22 and Extended Data Table ​Table11).

Table 2

Baseline characteristics (at randomization) in all randomized participants

Characteristics	Tirzepatide MTD (n=287)	Placebo (n=292)	Total (n=579)
Age, mean (s.d.), years	45.4 (12.6)	45.7 (11.8)	45.6 (12.2)
Sex, no. (%)
Female	181 (63.1)	183 (62.7)	364 (62.9)
Male	106 (36.9)	109 (37.3)	215 (37.1)
Race, no. (%)a
Asian	2 (0.7)	2 (0.7)	4 (0.7)
Black or African American	31 (10.8)	32 (11.0)	63 (10.9)
Multiple	6 (2.1)	2 (0.7)	8 (1.4)
American Indian or Alaskan	2 (0.7)	4 (1.4)	6 (1.0)
White	246 (85.7)	252 (86.3)	498 (86.0)
Ethnicity, no. (%)a
Hispanic or Latino	151 (52.6)	161 (55.1)	312 (53.9)
Not Hispanic or Latino	132 (46.0)	129 (44.2)	261 (45.1)
Not reported	4 (1.4)	2 (0.7)	6 (1.0)
Country
Argentina	43 (15.0)	44 (15.1)	87 (15.0)
Brazil	59 (20.6)	60 (20.5)	119 (20.6)
USA	185 (64.5)	188 (64.4)	373 (64.4)
Duration of obesity, mean (s.d.), yearsb	15.4 (11.6)	14.8 (10.8)	15.1 (11.2)
BMI category, no. (%)
<27	5 (1.7)	12 (4.1)	17 (2.9)
≥27 to <30	32 (11.1)	38 (13.0)	70 (12.1)
≥30 to <35	100 (34.8)	107 (36.6)	207 (35.8)
≥35 to <40	95 (33.1)	79 (27.1)	174 (30.1)
≥40	55 (19.2)	56 (19.2)	111 (19.2)
Obesity-related complications, n (%)c
Hypertension	95 (33.1)	104 (35.6)	199 (34.4)
Dyslipidemia	71 (24.7)	81 (27.7)	152 (26.3)
ASCVD	5 (1.7)	6 (2.1)	11 (1.9)
Polycystic ovarian syndrome	8 (4.4)	8 (4.4)	16 (4.4)
Obstructive sleep apnea	25 (8.7)	34 (11.6)	59 (10.2)
Osteoarthritis	43 (15.0)	48 (16.4)	91 (15.7)
Anxiety/depression	61 (21.3)	55 (18.8)	116 (20.0)
NAFLD	9 (3.1)	16 (5.5)	25 (4.3)
Asthma or COPD	21 (7.3)	31 (10.6)	52 (9.0)
Gout	6 (2.1)	9 (3.1)	15 (2.6)
Number of weight-related complications, n (%)c
0	96 (33.4)	100 (34.2)	196 (33.9)
1	102 (35.5)	81 (27.7)	183 (31.6)
2	48 (16.7)	54 (18.5)	102 (17.6)
3	22 (7.7)	36 (12.3)	58 (10.0)
4	14 (4.9)	14 (4.8)	28 (4.8)
≥5	5 (1.7)	7 (2.4)	12 (2.1)

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ASCVD, atherosclerotic cardiovascular disease; COPD, chronic obstructive pulmonary disease; NAFLD, non-alcoholic fatty liver disease.

^aRace and ethnicity were determined by the participant according to fixed selection categories.

^bDuration of obesity was assessed by self-report.

^cBaseline medical conditions were assessed through a review of participants’ medical history.

Extended Data Table 1

Demographics of Participants in the United States

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Demographics of Participants in the United States

^aRace and ethnicity were determined by the participant according to fixed selection categories. MTD, maximum tolerated dose (10 or 15mg).

Of the 579randomized participants, 479 (82.7%) completed the study (87.8% on tirzepatide MTD and 77.7% on placebo) and 429 (74.1%) completed the study on treatment (78.7% on tirzepatide MTD and 69.5% on placebo). The most common reasons for discontinuation of study treatment were adverse event (10.5%, detailed in Table ​Table3)3) and withdrawal by subject (6.3%) in the tirzepatide MTD group, and withdrawal by subject (14.4%) and lost to follow-up (6.5%) in the placebo group.

Table 3

Adverse events during the double-blind period and safety follow-up period (safety analysis set)

	No. (%)
	Tirzepatide MTD (n=287)	Placebo (n=292)
Participants with ≥1 adverse event	250 (87.1)	224 (76.7)
Serious adverse events	17 (5.9)	14 (4.8)
Deatha	1 (0.3)	1 (0.3)
Adverse events leading to treatment discontinuationb	30 (10.5)	6 (2.1)
Nausea	24 (8.4)	4 (1.4)
Vomiting	6 (2.1)	0
Diarrhea	3 (1.0)	0
Dyspepsia	3 (1.0)	0
Constipation	2 (0.7)	0
Adverse events occurring in ≥5% of participants in any treatment group
Nausea	114 (39.7)	41 (14.0)
Diarrhea	89 (31.0)	27 (9.2)
Constipation	66 (23.0)	20 (6.8)
COVID-19	66 (23.0)	74 (25.3)
Vomiting	52 (18.1)	4 (1.4)
Injection site reaction	32 (11.1)	3 (1.0)
Abdominal pain	30 (10.5)	7 (2.4)
Decreased appetite	27 (9.4)	12 (4.1)
Dyspepsia	27 (9.4)	9 (3.1)
Headache	27 (9.4)	22 (7.5)
Upper respiratory tract infection	25 (8.7)	21 (7.2)
Alopecia	20 (7.0)	4 (1.4)
Dizziness	20 (7.0)	6 (2.1)
Fatigue	20 (7.0)	9 (3.1)
Flatulence	19 (6.6)	8 (2.7)
Gastroesophageal reflux disease	19 (6.6)	7 (2.4)
Back pain	17 (5.9)	15 (5.1)
Eructation	16 (5.6)	3 (1.0)
Influenza	12 (4.2)	25 (8.6)
Urinary tract infection	11 (3.8)	15 (5.1)
Anxiety	9 (3.1)	19 (6.5)
Arthralgia	7 (2.4)	15 (5.1)
Sinusitis	6 (2.1)	16 (5.5)
Adverse events of special interest
Severe or serious gastrointestinal events	16 (5.6)	5 (1.7)
Malignancies	5 (1.7)	3 (1.0)
Severe or serious acute gall bladder diseases	2 (0.7)	0
MACE (adjudication confirmed)	1 (0.3)	1 (0.3)
Pancreatitis (adjudication confirmed)	1 (0.3)	1 (0.3)
Severe or serious renal events	1 (0.3)	0
Severe or serious MDD/suicidal behavior and ideation	1 (0.3)	0
Severe or serious arrhythmias and cardiac conduction disorders	0	1 (0.3)
Severe hypoglycemia	0	0
Other adverse events of interest
Cholelithiasis	4 (1.4)	3 (1.0)
Acute cholecystitis	1 (0.3)	0
Chronic cholecystitis	0	1 (0.3)

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Events are listed according to Medical Dictionary for Regulatory Activities, v.26.0, preferred terms. MACE, major adverse cardiovascular event; MDD, major depressive disorder.

^aDeaths are also included as serious adverse events and discontinuations due to adverse event.

^bOnly adverse events occurring in ≥2 participants in any treatment group are presented.

In tirzepatide-treated participants, 248 (86.4%) had a tirzepatide MTD of 15mg. In this study, all randomized participants took at least one dose of the study intervention (tirzepatide MTD or placebo). Therefore, the intention-to-treat population is the same as the modified intention-to-treat population.

Primary outcomes

Figure 2a,b shows the mean percentage reduction in body weight from randomization to week72. For the treatment regimen estimand (TRE) the mean change at week72 was −18.4% (s.e. 0.7) with tirzepatide MTD and 2.5% (s.e. 1.0) with placebo. Tirzepatide MTD was superior to placebo, with an estimated treatment difference relative to placebo of −20.8 percentage points (95% CI −23.2, −18.5; P<0.001) (Table ​(Table4).4). The mean change in body weight for the efficacy estimand was −21.1% (s.e. 0.6) with tirzepatide MTD and 3.3% (s.e. 0.6) with placebo. The estimated treatment difference was −24.5 percentage points (95% CI −26.1, −22.8; P<0.001) for tirzepatide MTD versus placebo. Absolute body weight over time is shown in Extended Data Fig. ​Fig.11.

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Fig. 2

Effect of once-weekly tirzepatide on body weight in comparison with placebo.

a, Least-square mean (LSM) (s.e.) per cent change in body weight from randomization to week72 derived from an analysis of covariance model for the TRE (tirzepatide MTD, n=287 participants; placebo, n=292 participants), and from MMRM analysis for the efficacy estimand (tirzepatide MTD, n=284 participants; placebo, n=291 participants). b, LSM (s.e.) per cent change in body weight over time from randomization to 72weeks, derived from MMRM analysis for the efficacy estimand; week72 estimates for the TRE are also shown. c,d, LSM (s.e.) percentages of participants who had body weight reduction of at least 5, 10, 15, 20 or 25% from randomization to week72. c, Percentage of participants reaching weight reduction thresholds (TRE) was calculated using logistic regression with missing values imputed by hybrid imputation (tirzepatide MTD, n=287 participants; placebo; n=292 participants). d, Percentage of participants reaching weight reduction thresholds (efficacy estimand) was obtained by logistic regression with missing values at week72 imputed from MMRM analysis (tirzepatide MTD, n=284 participants; placebo, n=291 participants). e, LSM proportion of participants that maintained ≥80% of body weight reductions achieved at the end of the lead-in period. Both TRE and efficacy estimand shown. f, Mean (95% CI) per cent change in body weight over time from the start of the intensive lifestyle intervention lead-in period (–12 weeks) to 72weeks, derived from observed values, irrespective of treatment adherence; week 72 estimates for TRE and efficacy estimand (EFF), are also shown.

Table 4

Efficacy findings from randomization (week 0) to week 72

	LSM (s.e.)		Treatment comparison
	Tirzepatide MTD (n=287)	Placebo (n=292)	Difference from placebo (95% CI)	P value
Primary endpoints
Per cent change in body weight	−18.4 (0.7)	2.5 (1.0)	ETD −20.8 (−23.2, −18.5)	<0.001
Participants achieving ≥5% body weight reduction, %	87.5 (2.2)	16.5 (3.0)	OR 34.6 (19.2, 62.6)	<0.001
Key secondary endpoints
Participants achieving body weight reduction, %
≥10%	76.7 (2.7)	8.9 (2.4)	OR 34.7 (17.6, 68.3)	<0.001
≥15%	65.4 (3.0)	4.2 (1.8)	OR 48.2 (19.2, 121.0)	<0.001
≥20%	44.7 (3.0)	2.2 (1.3)	OR 40.4 (12.2, 133.8)	<0.001
Participants maintaining ≥80% of lead-in body weight lost at week 72, %	94.0 (1.7)	43.8 (3.9)	ETD 19.7 (10.3, 37.6)	<0.001
Change in waist circumference, cm	−14.6 (0.7)	0.2 (1.0)	ETD −14.8 (−17.2, −12.5)	<0.001
Additional secondary endpoints
Change in body weight, kg	−21.5 (0.7)	3.5 (0.7)	ETD −25.0 (−26.9, −23.2)	NRa
Change in BMI, kg/m2	−7.7 (0.2)	1.2 (0.2)	ETD −8.9 (−9.6, −8.3)	NR
Change in SBP, mmHg	−5.1 (0.7)	4.1 (0.7)	ETD −9.2 (−11.2, −7.2)	NR
Change in DBP, mmHg	−3.2 (0.5)	2.3 (0.5)	ETD –5.5 (−6.9, −4.1)	NR
Fasting lipids
Per cent change in total cholesterol	−3.0 (1.0)	5.2 (1.1)	ETD −7.8 (−10.4, −5.1)	NR
Per cent change in non-HDL cholesterol	−9.8 (1.3)	5.6 (1.5)	ETD −14.6 (−17.9, −11.2)	NR
Per cent change in HDL cholesterol	15.4 (1.2)	3.6 (1.1)	ETD 11.4 (8.2, 14.7)	NR
Per cent change in LDL cholesterol	−6.1 (1.4)	6.1 (1.7)	ETD −11.5 (−15.3, −7.5)	NR
Per cent change in VLDL cholesterol	−25.6 (1.6)	3.0 (2.3)	ETD −27.8 (−32.1, −23.2)	NR
Per cent change in triglycerides	−25.8 (1.6)	3.0 (2.3)	ETD −28.0 (−32.3, −23.4)	NR
Per cent change in free fatty acids	−33.1 (2.2)	−15.0 (3.0)	ETD −21.3 (−28.4, −13.6)	NR
Change in fasting glucose, mgdl−1	−8.8 (0.8)	2.4 (0.9)	ETD −11.2 (−13.5, −8.8)	NR
Change in HbA1c, %	−0.5 (0.0)	0.0 (0.0)	ETD −0.5 (−0.5, −0.4)	NR
Per cent change in fasting insulin	−39.1 (2.5)	17.3 (5.0)	ETD −48.1 (−53.7, −41.7)	NR
Patient-reported outcomes
Change in SF-36v2 Physical Functioning domain scoreb	3.3 (0.4)	−0.6 (0.4)	ETD 3.9 (2.8, 4.9)	NR
Change in IWQOL-Lite-CT Physical Function composite scorec	13.9 (1.1)	1.1 (1.2)	ETD 12.8 (9.7, 16.0)	NR
Prespecified exploratory endpoints
Participants achieving body weight reduction ≥25%, %	28.7 (2.7)	1.2 (0.9)	OR 33.70 (8.84, 128.52)	NR

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Primary, key secondary and prespecified exploratory endpoints are presented using the TRE, and additional secondary endpoints are presented using the efficacy estimand. Primary and key secondary endpoints were controlled for type1 error at a two-sided significance level of 0.05 within each estimand via a graphical testing approach. Other endpoints were not controlled for type1 error.

DBP, diastolic blood pressure; ETD, estimated treatment difference; NR, not reported; SBP, systolic blood pressure.

^aPvalues are not reported for additional secondary and prespecified exploratory endpoints because these were not controlled for type1 error.

^bSF-36v2 measures health-related quality of life and general health status. SF-36v2 scores are norm based—that is, transformed to a scale in which the 2009 US general population has a mean score of 50 and s.d. of 10. An increase in score represents an improvement in health status.

^cIWQOL-Lite-CT measures weight-specific, health-related quality of life. All items are rated on either a five-point frequency scale (‘never’ to ‘always’) or a five-point truth scale (‘not at all true’ to ‘completely true’). Scores are transformed to a scale of 0–100, with higher scores reflecting better levels of functioning.

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Extended Data Fig. 1

Body weight in kg over time.

Mean (standard error) body weight (kg) over time from randomization to 72 weeks derived from a mixed-model for repeated measures (MMRM) analysis for the efficacy estimand. Only participants with non-missing baseline value and at least one non-missing post-baseline value of the response variable were included in analysis. MTD, maximum tolerated dose (10 or 15mg).

For the TRE, 87.5% (251) of participants in the tirzepatide MTD group lost an additional ≥5% of body weight from randomization to week72 compared with 16.5% (48) in the placebo group (odds ratio (OR) 34.6 (95% CI 19.2, 62.6); P<0.001) (Fig. ​(Fig.2c2c and Table ​Table4).4). For the efficacy estimand, 94.4% (268) of participants in the tirzepatide MTD group had an additional body weight reduction of ≥5% from randomization compared with 10.7% (31) in the placebo group (OR 130.4 (95% CI 70.0, 242.8); P<0.001) (Fig. ​(Fig.2d2d).

Secondary outcomes

Change in body weight

At week 72, more participants on tirzepatide MTD than placebo achieved reductions in body weight of ≥10, ≥15 and ≥20% from randomization (P<0.001; Fig. 2c,d and Table ​Table44).

At 72 weeks, for the TRE, 94.0% (270) of participants in the tirzepatide MTD group maintained ≥80% of body weight lost during the 12-week lead-in period compared with 43.8% (128) in the placebo group (OR 19.7; 95% CI 10.3, 37.6; P<0.001; Fig. ​Fig.2e2e and Table ​Table4).4). For the efficacy estimand, 98.6% (280) of participants in the tirzepatide MTD group met this endpoint compared with 37.8% (110) in the placebo group (OR 101.6; 95% CI 39.2, 263.6; P<0.001; Fig. ​Fig.2e2e).

Overall, for the TRE, intensive lifestyle intervention followed by 72weeks of tirzepatide led to a total weight change of −24.3% compared with −4.5% with intensive lifestyle intervention followed by placebo (estimated treatment difference −19.9 percentage points (95% CI −23.5, −16.2) (Fig. ​(Fig.2f).2f). For the efficacy estimand, intensive lifestyle intervention followed by 72weeks of tirzepatide led to a total weight change of –26.6% compared with −3.8% with intensive lifestyle intervention followed by placebo (estimated treatment difference −22.8 percentage points (95% CI −24.3, −21.2; Fig. ​Fig.2f2f and Extended Data Table ​Table22).

Extended Data Table 2

Additional Efficacy Findings from Start of Intensive Lifestyle Intervention Lead-In (Week-12) to Week 72 (Efficacy Estimand)

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Additional Efficacy Findings from Start of Intensive Lifestyle Intervention Lead-In (Week-12) to Week 72 (Efficacy Estimand)

BMI, body mass index; DBP, diastolic blood pressure; ETD, estimated treatment difference; HbA1c, glycated hemoglobin; HDL-C, high-density lipoprotein cholesterol; IWQOL-Lite-CT, Impact of Weight on Quality of Life-Lite-Clinical Trials Version; LDL-C, low-density lipoprotein cholesterol; MTD, maximum tolerated dose (10 or 15mg); SBP, systolic blood pressure; SF-36v2, Short Form-36 version 2 Health Survey acute form; VLDL-C, very low-density lipoprotein cholesterol. ^aThe SF-36v2 measures health-related quality of life and general health status. The SF-36v2 scores are norm-based scores, ie, scores transformed to a scale in which the 2009 US general population has a mean score of 50 and an SD of 10. An increase in score represents an improvement in health status. ^bThe IWQOL-Lite-CT measures weight-specific health-related quality of life. All items are rated on either a 5-point frequency scale (‘never’ to ‘always’) or a 5-point truth scale (‘not at all true’ to ‘completely true’). Scores are transformed to a scale of 0 to 100, with higher scores reflecting better levels of functioning.

Accordingly, there was a reduction in BMI with tirzepatide compared with placebo from randomization to week72 (efficacy estimand: tirzepatide, −7.7kg/m² versus placebo, 1.2kg/m²; estimated treatment difference −8.9kg/m² (95% CI −9.6, −8.3; Table ​Table4).4). Total change in BMI with intensive lifestyle intervention followed by 72weeks of tirzepatide MTD was −10.4kg/m² compared with –1.4kg/m² with intensive lifestyle intervention followed by placebo (efficacy estimand: estimated treatment difference −8.9kg/m² (95% CI −9.6, −8.3; Extended Data Table ​Table22).

Cardiometabolic risk factors and physical function

At week 72 the change from randomization in waist circumference with tirzepatide MTD was superior to placebo using the TRE (tirzepatide, −14.6cm versus placebo, 0.2cm; estimated treatment difference, −14.8cm (95% CI −17.2, −12.5; P<0.001; Table ​Table4).4). Results were consistent for the efficacy estimand (tirzepatide, −16.8cm versus placebo, 1.1cm; estimated treatment difference −17.9cm (95% CI −19.5, −16.3; P<0.001). Improvements with tirzepatide MTD, from randomization to week72, were greater versus placebo in both systolic blood pressure (tirzepatide, −5.1mmHg versus placebo, 4.1mmHg; estimated treatment difference −9.2mmHg (−11.2, −7.2) and diastolic blood pressure (tirzepatide, −3.2mmHg versus placebo, 2.3mmHg; estimated treatment difference −5.5mmHg (−6.9, −4.1) using the efficacy estimand (Table ​(Table44 and Extended Data Fig. ​Fig.2).2). Treatment with tirzepatide MTD resulted in further improvements across all fasting lipid levels (HDL, LDL, VLDL, total cholesterol, triglycerides and free fatty acids), glycemic control (fasting glucose and HbA1c) and fasting insulin compared with placebo at 72weeks from randomization (Table ​(Table4).4). In addition, 4.9 and 2.8% of participants in the tirzepatide group compared with 1.0 and 1.7% of participants in the placebo group were reported as having a decrease in intensity of antihypertensive and lipid-lowering medications, respectively. Conversely, 2.4 and 0.3% of participants in the tirzepatide group were reported to have experienced an increase in intensity of antihypertensive and lipid-lowering therapies, respectively, compared with 6.5 and 2.1% of participants in the placebo group.

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Extended Data Fig. 2

Blood pressure change from start of lead-in period over time.

Panel A, mean (95% confidence interval) change from baseline over time in systolic blood pressure from start of intensive-lifestyle intervention lead-in period (week -12) to 72 weeks using observed means. Week 72 estimates for the efficacy estimand (EFF) are also shown. Panel B, mean (95% confidence interval) change from baseline over time in diastolic blood pressure from start of intensive-lifestyle intervention lead-in period (week -12) to 72 weeks using observed means. Week 72 estimates for the efficacy estimand (EFF) are also shown.

Participant-reported physical function improved more with tirzepatide than with placebo from randomization to week72 (Table ​(Table4).4). This was observed with both the physical functioning domain score for Short Form-36v.2 Health Survey (SF-36v2) (tirzepatide, 3.3 versus placebo, −0.6; estimated treatment difference 3.9 (95% CI 2.8, 4.9)) and the Impact of Weight on Quality of Life-Lite-Clinical Trials Version (IWQOL-Lite-CT) physical function composite score (tirzepatide, 13.9 versus placebo, 1.1; estimated treatment difference 12.8 (95% CI 9.7, 16.0)) using the efficacy estimand.

Changes in cardiometabolic parameters and patient-reported outcomes from the start of the lead-in period (week−12) to week72 are reported in Extended Data Table ​Table22.

Safety

Overall, 87.1% of the 287tirzepatide-treated participants reported at least one treatment-emergent adverse event compared with 76.7% of the 292placebo-treated participants (Table ​(Table3).3). The most frequently reported adverse events were gastrointestinal (nausea, diarrhea and constipation). These occurred in more participants in the tirzepatide MTD group than placebo, were mostly mild to moderate in severity and occurred primarily during dose escalation (Extended Data Fig. ​Fig.3).3). Antiemetic medication use was reported by 78 participants (27.2%) treated with tirzepatide and by 20 (6.8%) treated with placebo. Antidiarrheal medication use was reported by 23 participants (8.0%) treated with tirzepatide and by six (2.1%) treated with placebo.

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Extended Data Fig. 3

Incidence of nausea, vomiting, and diarrhea over time.

The percentage of participants receiving tirzepatide or placebo who reported nausea, vomiting, or diarrhea are presented. Percentages are based on number of participants at risk at specific observation time. Events were classed as mild (shown in green), moderate (shown in orange), or severe (shown in red). MTD, maximum tolerated dose (10 or 15mg); TZP, tirzepatide.

Serious adverse events were reported by 31participants (5.4%) overall. Occurrence was similar in participants treated with tirzepatide (5.9%) and placebo (4.8%) (Table ​(Table3).3). Two deaths (both myocardial infarction) were reported during the study, one in the tirzepatide MTD group and one in the placebo group. Both events were considered not to be related to the study treatment by the investigator.

Adjudication-confirmed cases of pancreatitis were reported in 0.3% (one) of participants in the tirzepatide MTD group and 0.3% (one) of participants in the placebo group from randomization to safety follow-up (Table ​(Table3).3). Cholelithiasis was reported in 1.4% (four) of participants in the tirzepatide group and 1.0% (three) of participants in the placebo group. There was one case (0.3%) of acute cholecystitis in the tirzepatide group and none in the placebo group. Malignancies were reported in 1.7% (five) of participants in the tirzepatide MTD group and 1.0% (three) of participants in the placebo group. None of the malignancies were considered related to the study treatment by the investigators, and no cases of medullary thyroid cancer or pancreatic cancer were reported. Additional safety measures are reported in Extended Data Table ​Table33.

Extended Data Table 3

Additional Safety Measures from Randomization to Week 72

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Additional Safety Measures from Randomization to Week 72

Data are model based estimate (standard error) and were analyzed with log transformation, except for pulse rate data. MTD, maximum tolerated dose (10 or 15mg).

Discussion

Tirzepatide substantially increased the magnitude of weight loss when administered following an initial 12-week intensive lifestyle intervention that reduced baseline body weight by an average of 6.9% in successful program completers. As measured from randomization (week0) to week72, participants who received tirzepatide MTD of 10 or 15mg lost an additional 18.4% of body weight, compared with a gain of 2.5% for placebo. In total, 87.5% of tirzepatide-treated participants lost an additional 5% or more of their randomization weight compared with 16.5% of placebo-treated participants, with tirzepatide also demonstrating superiority in the achievement of all other categorical weight losses. These findings indicate that individuals with overweight or obesity who have lost approximately 5–10% of their body weight with supervised lifestyle intervention—or potentially through their own self-directed diet and exercise efforts—could expect to achieve further clinically meaningful weight loss with the addition of tirzepatide.

The strength of tirzepatide is underscored by comparison with a similarly designed trial of liraglutide (3.0mg), approved for chronic weight management. After losing an average 6.0% of baseline weight in a comparable lead-in program, participants who received liraglutide achieved an additional 6.2% reduction in randomization weight at 56weeks compared with a 0.2% reduction for placebo²⁹. The liraglutide trial provided a total of 17lifestyle counseling sessions during the medication phase of the study compared with only quarterly visits in the present trial. This decreased frequency of counseling visits could explain the greater weight regain in the placebo group in the present study. The only other similarly designed trial of a medication approved for chronic weight management found that orlistat (120mg three times daily) was not effective in inducing additional weight loss over 1year when administered following an average 11.0% reduction achieved with intensive lifestyle intervention³⁰. Patients treated by both orlistat and placebo regained one-third or more of their lost weight. Tirzepatide was also superior to placebo on a traditional measure of weight loss maintenance—the proportion of participants who maintained a predefined percentage of their initial weight loss. In the present study, 94% of tirzepatide-treated participants, compared with 44% of those who received placebo, maintained ≥80% of their weight loss achieved in the lead-in period. These results compare favorably with those achieved with both liraglutide and orlistat but perhaps, more importantly, with the results of traditional lifestyle intervention. Individuals who receive such intervention typically regain one-third of their lost weight in the year following treatment completion³¹. Regain can be decreased to 10–15% at 1year with participation in a weight loss maintenance program, offered in person or by phone, which provides continued lifestyle counseling on a monthly or more frequent basis³². However, after 2.5years of such monthly phone-based counseling only 45% of participants maintained ≥4kg of an original mean 8.5kg loss achieved during a 6month lead-in period³³. These findings reveal the potential benefits of tirzepatide, relative to traditional weight loss maintenance counseling, in not only sustaining weight reduction achieved with intensive lifestyle intervention but in adding to it. Long-term comparative studies for weight loss maintenance are needed.

The cumulative 24.3% reduction in body weight achieved with intensive lifestyle intervention, followed by tirzepatide, approximates the 1year weight loss induced with sleeve gastrectomy³⁴. The overall BMI reduction of 10kg/m² represents a downward shift of about two BMI categories. Participants treated with lifestyle interventions have long sought to achieve a similar magnitude of weight loss, principally to improve their health and quality of life^35,36. Tirzepatide enhanced the improvements in cardiometabolic risk factors that were achieved in the lead-in period. Systolic and diastolic BP improved by an additional −5.1 and −3.2mmHg, respectively, lipids parameters improved by an additional −3% to −26% and fasting insulin further declined by 39%. Self-reported physical function improved by 3.3points on the SF-36v2 physical functioning domain score and by 13.9points on the IWQOL-Lite-CT physical function composite. These improvements underscore the additional benefits that patients may receive from treatment with tirzepatide after first losing weight with intensive lifestyle intervention, or potentially with their own self-directed diet and activity programs. By contrast, many of the cardiometabolic improvements achieved during the lead-in reverted toward baseline in the placebo group.

The safety profile of tirzepatide in this trial was consistent with findings from previous trials of tirzepatide when evaluated for the treatment of obesity^27,37 or type2 diabetes³⁸, as well as with the safety profile of the GLP-1 receptor agonist class in patients with obesity or overweight^39,40. Mild-to-moderate gastrointestinal events were the most frequent treatment-emergent adverse events, mostly transient and occurring during dose escalation. Compared with the tirzepatide 15mg group in SURMOUNT-1, the tirzepatide group in this study had modestly higher rates of gastrointestinal adverse events and treatment discontinuation due to adverse events. Other trials that combined intensive lifestyle intervention with pharmacotherapy have also shown higher rates of gastrointestinal events compared with trials investigating pharmacotherapy without intensive lifestyle intervention (for example, STEP-3 compared with STEP-1 for semaglutide 2.4mg and SCALE-MAINTENANCE compared with SCALE for liraglutide 3.0mg)^21,29,41,42. It has been speculated that caloric restriction could lead to a reduction in GLP-1 and other gastrointestinal satiety hormones⁴³. Whether this worsens initial gastrointestinal tolerability to incretin-based therapy and is a possible explanation for the observed findings requires further investigation.

Much remains to be learned about how lifestyle intervention and the new incretin-based antiobesity medications can be optimally used together. If the goal of combining these therapies is to increase total weight loss, results of the present trial and SCALE-MAINTENANCE²⁹ suggest that introducing the intensive lifestyle intervention first (for approximately 12weeks) followed by the addition of medication, as in the present study, could maximize weight reduction. The weight reduction observed with tirzepatide MTD in the 72week, double-blind period of the current trial was similar to that achieved with tirzepatide 10 and 15mg over 72weeks in the SURMOUNT-1 study. Therefore, the sequential use of these interventions appeared to produce additive weight loss that approached the combined results of each intervention used alone. However, providing intensive lifestyle intervention and medication concurrently, rather than sequentially, has not achieved the same degree of additive benefit in placebo-controlled trials^41,44. For example, the concurrent provision of intensive lifestyle intervention (plus meal replacements) and semaglutide 2.4mg in the STEP-3 trial produced a mean weight loss of 16.0%, which was comparable to that observed in the STEP-1 study (14.9%) in a similar population that did not receive this enhanced intensive lifestyle intervention^21,41.

The suggestion of additivity with sequential therapy, however, may be challenged by findings from preclinical studies. These studies have demonstrated that caloric restriction alone does not address the underlying physiology regulating body weight or fat mass, and antiobesity medication has the same overall ultimate effect regardless of whether or not caloric restriction preceded the medication⁴⁵. This implies that, if weight reduction in the lead-in period of the present trial was due only to a volitional reduction in caloric intake, the overall weight reduction of 24.3% could represent the effect the drug would have had even without an intensive lifestyle lead-in. Indeed, a recent 88week trial of tirzepatide has demonstrated this degree of weight reduction as early as 52weeks on treatment⁴⁶. The reason the weight reduction in the present trial may be higher than that observed in SURMOUNT-1 could be related to differences in demographics between the trial populations, or to the fact that this study, and other similarly designed trials, preselected for a highly responsive population by randomization of only participants who achieved an initial reduction of 5% or more with intensive lifestyle intervention. It is possible that participants who respond to lifestyle intervention are simply more responsive to tirzepatide. Further analyses should help examine this hypothesis.

Another major treatment issue concerns the intensity (that is, frequency) and scope of lifestyle intervention required with antiobesity medications. Weekly lifestyle visits and daily monitoring of food and energy intake historically have been required to help patients achieve and maintain the 500–750kcalper day deficit needed to induce clinically meaningful weight loss¹⁶. Semaglutide and tirzepatide both appear to physiologically drive this reduction in energy intake, which might enable patients to implement dietary behavior changes with greater ease and efficiency than conventional lifestyle counseling. Similarly, weight loss induced with antiobesity medication, with the accompanying improvement in physical function observed in the present study, could increase patients’ ease in engaging in physical activity, thus potentially further improving their cardiometabolic health.

The strengths of this study, which included an intensive lifestyle lead-in, include the fact that it had a relatively large sample size in which over one-third of the randomized population were men and over half were of Hispanic ethnicity. In addition, a 72-week treatment period facilitated at least 52weeks of treatment with tirzepatide at MTD. The allowance of dose de- and re-escalation during the titration phase helped to maximize tolerability and reflected dose adjustment strategies that may be relevant for clinical practice.

The study’s limitations include that it was geographically restricted to North and South America and that the study population was predominantly white, thus potentially limiting the generalizability of the findings. In addition, the 17.5% of participants who did not lose at least 5% of baseline weight in the intensive lifestyle intervention were not randomized to medication. To the extent that response to lifestyle intervention may predict response to medication, exclusion of these participants may have resulted in a higher mean weight loss with tirzepatide MTD than would have been observed if lifestyle nonresponders had been included. Trials of the response to antiobesity medications in persons who are unsuccessful with intensive lifestyle intervention are needed, because lack of success with lifestyle interventions has been a common prerequisite for initiation of pharmacotherapy or bariatric surgery. Future studies evaluating both genetic and behavioral predictors of response to lifestyle intervention and pharmacotherapy will help inform clinical management even earlier in the course of treatment.

In conclusion, in the SURMOUNT-3 trial, tirzepatide demonstrated clinically meaningful additional body weight reductions in adults with overweight or obesity following initial weight loss with intensive lifestyle intervention.

Methods

Study design and participants

This 84-week, multicenter, randomized, parallel-arm, double-blind, placebo-controlled trial was conducted at 62medical research centers in the USA, Argentina and Brazil. The study consisted of four periods: a 2-week screening period; a 12-week lead-in period during which participants received intensive lifestyle intervention to achieve ≥5.0% body weight reduction; a 72-week double-blind, placebo-controlled treatment period (including a 20-week dose escalation period); and a 4-week safety follow-up period (Extended Data Fig. ​Fig.44).

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Extended Data Fig. 4

SURMOUNT-3 study design.

This is a phase 3, multicenter, randomized, placebo-controlled, double- blinded clinical trial investigating the efficacy and safety of maximum tolerated dose (MTD) of tirzepatide (10mg or 15mg) administered once weekly (QW) subcutaneously compared with placebo for body weight management, in participants who have obesity, or overweight with at least 1 obesity-related complication (excluding type 2 diabetes), and with at least 5% weight reduction following a 12-week intensive lifestyle intervention lead-in. All randomized participants were planned to undergo a 72-week treatment period.

Eligible participants were ≥18years of age and had obesity (BMI≥30kg/m²) or overweight (BMI≥27kg/m²) with at least one weight-related complication. Female enrollment was capped at 70% to ensure adequate representation of the male population. Full eligibility criteria are listed below.

Online content

Any methods, additional references, Nature Portfolio reporting summaries, source data, extended data, supplementary information, acknowledgements, peer review information; details of author contributions and competing interests; and statements of data and code availability are available at 10.1038/s41591-023-02597-w.

Acknowledgements

Author contributions

N.N.A., M.C.B. and S.Z. contributed to the study design. T.A.W., A.M.C., S.M., G.S. and B.H. conducted the trial and collected data. J.C. and S.Z. were responsible for statistical analyses. S.Z., J.C., N.N.A., M.C.B. and T.F. are the guarantors of this work and, as such, take responsibility for the integrity of the data and the accuracy of data analysis. All authors participated in data interpretation, manuscript writing (assisted by a medical writer paid for by the funder) and critical review of the manuscript, had full access to all the data in the study and approved the submission of this manuscript for publication.

Peer review

Data availability

Eli Lilly and Company provides access to all individual participant data collected during the trial, after anonymization, except for pharmacokinetic or genetic data. Data are available to request 6months after the indication studied has been approved in the USA and European Union and after primary publication acceptance, whichever is later. No expiration date of data requests is currently set once data have been made available. Access is provided after a proposal has been approved by an independent review committee identified for this purpose and after receipt of a signed data-sharing agreement. Data and documents, including the study protocol, statistical analysis plan, clinical study report and blank or annotated case report forms, will be provided in a secure data-sharing environment. For details on submitting a request, see the instructions provided at www.vivli.org.

Competing interests

T.A.W. reports grants or contracts from Novo Nordisk, Epitomee Medical Co. and Eli Lilly and Company; and service on Scientific Advisory Boards for Novo Nordisk and WW. A.M.C. reports grants or contracts from National Institutes of Health, WW International, Inc, The EdnaG. Kynett Memorial Foundation, Novo Nordisk and Epitomee Medical; consulting fees from Eli Lilly and Company and Boehringer Ingelheim; and payment or honoraria for presentation and travel/meeting support from the Obesity Medicine Association. S.M. reports grants or contracts from Boehringer Ingelheim, Rhythm Pharmaceuticals and Novo Nordisk; consulting fees from Novo Nordisk, Rhythm Pharmaceuticals and Eli Lilly and Company; payment or honoraria from Columbia University Medical Center, Boston Obesity Course in Obesity medicine and Medical College of Wisconsin; and participation on Advisory Boards for Novo Nordisk and Eli Lilly and Company. R.K. reports participation on a Data Safety Monitoring Board or Advisory Board for Eli Lilly and Company, Novo Nordisk and Boehringer Ingelheim. J.A. reports grants or contracts from Nestle Healthcare Nutrition, Eli Lilly and Company, Boehringer Ingelheim, Epitomee, Inc., UnitedHealth Group R&D, KVK Tech and WW; consulting fees from Nestle Healthcare Nutrition, Eli Lilly and Company, Optum Labs R&D, Novo Nordisk, Spokes Health, Inc., Intuitive, Regeneron, Brightseed, Level2 and WW; receipt of equipment, materials, drugs, medical writing, gifts or other services from KVK Tech, WW and Nestle Healthcare Nutrition; and is President Elect of The Obesity Society and an Executive Board Member of the American Society for Nutrition Foundation. G.S. reports consulting fees from Rhythm Pharmaceuticals, Novo Nordisk and Eli Lilly and Company; and speaker’s bureau from Novo Nordisk. B.H. reports payment or honoraria from Eli Lilly and Company, Novo Nordisk, Merck S.A., Astra Zeneca and Abbott Nutrition; travel/meeting support from Novo Nordisk; participation on a Data Safety Monitoring Board or Advisory Board for Eli Lilly, Novo Nordisk and Merck S.A; receipt of equipment, materials, drugs, medical writing, gifts or other services from Eli Lilly and Company and Novo Nordisk; and is President of the Brazilian Association of Obesity and a Member of Board of Trustees of World Obesity Federation representing Latin America. S.Z., J.C., M.C.B., N.N.A. and T.F. are employees and shareholders of Eli Lilly and Company.

Footnotes

References