Recombinant Leptin for Weight Loss in Obese and Lean Adults: A Randomized, Controlled, Dose-Escalation Trial
CONTEXT The protein hormone leptin is important to the homeostatic regulation of body weight. Treatment with exogenous leptin may affect weight loss. OBJECTIVE To determine the relationship between increasing doses of exogenous leptin administration and weight loss in both lean and obese adults. DES...
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Veröffentlicht in: | JAMA : the journal of the American Medical Association 1999-10, Vol.282 (16), p.1568-1575 |
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Zusammenfassung: | CONTEXT The protein hormone leptin is important to the homeostatic regulation
of body weight. Treatment with exogenous leptin may affect weight loss. OBJECTIVE To determine the relationship between increasing doses of exogenous
leptin administration and weight loss in both lean and obese adults. DESIGN A randomized, double-blind, placebo-controlled, multicenter, escalating
dose cohort trial conducted from April 1997 to October 1998. SETTING Four university nutrition and obesity clinics and 2 contract clinical
research clinics. PARTICIPANTS Fifty-four lean (body mass index, 20.0-27.5 kg/m2; mean [SD]
body weight, 72.0 [9.7] kg) and 73 obese (body mass index, 27.6-36.0 kg/m2; mean [SD] body weight, 89.8 [11.4] kg) predominantly white (80%)
men (n = 67) and women (n = 60) with mean (SD) age of 39 (10.3) years. INTERVENTIONS Recombinant methionyl human leptin self-administered by daily morning
subcutaneous injection (0 [placebo], 0.01, 0.03, 0.10, or 0.30 mg/kg). In
part A, lean and obese subjects were treated for 4 weeks; in part B, obese
subjects were treated for an additional 20 weeks. Lean subjects consumed a
eucaloric diet to maintain body weight at the current value, and obese subjects
were prescribed a diet that reduced their daily energy intake by 2100 kJ/d
(500-kcal/d) from the amount needed to maintain a stable weight. MAIN OUTCOME MEASURES Body weight, body fat, and incidence of adverse events. RESULTS Weight loss from baseline increased with increasing dose of leptin among
all subjects at 4 weeks (P = .02) and among obese
subjects at 24 weeks (P = .01) of treatment. Mean
(SD) weight changes at 4 weeks ranged from −0.4 (2.0) kg for placebo
(n = 36) to −1.9 kg (1.6) kg for the 0.1 mg/kg dose (n = 29). Mean (SD)
weight changes at 24 weeks ranged from −0.7 (5.4) kg for the 0.01 mg/kg
dose (n = 6) to –7.1 (8.5) kg for the 0.30 mg/kg dose (n = 8). Fat mass
declined from baseline as dose increased among all subjects at 4 weeks (P = .002) and among obese subjects at 24 weeks of treatment
(P = .004); more than 95% of weight loss was fat
loss in the 2 highest dose cohorts at 24 weeks. Baseline serum leptin concentrations
were not related to weight loss at week 4 (P = .88)
or at week 24 (P = .76). No clinically significant
adverse effects were observed on major organ systems. Mild-to-moderate reactions
at the injection site were the most commonly reported adverse effects. CONCLUSIONS A dose-response relationship with weight and fat loss was observed with
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ISSN: | 0098-7484 1538-3598 |
DOI: | 10.1001/jama.282.16.1568 |