Investigation of setmelanotide, an MC4R agonist, for obesity in individuals with Smith-Magenis syndrome - 10/07/24

Doi : 10.1016/j.orcp.2024.07.001

Julia Lazareva ^a , Stephanie R. Sisley ^b , Sheila M. Brady ^a , Ann C.M. Smith ^c , Sarah H. Elsea ^d , Jeremy J. Pomeroy ^e , Christian L. Roth ^f , Jennifer E. Sprague ^g , Martin Wabitsch ^h , Jill Garrison ⁱ , Jack A. Yanovski ^a,^⁎
^a Section on Growth and Obesity, Eunice Kennedy Shriver National Institutes of Child Health and Human Development, National Institutes of Health Bethesda, 20892 MD, United States
^b Department of Pediatrics, Baylor College of Medicine, Houston, 77030 TX, United States
^c Office of the Clinical Director, National Human Genome Research Institute, National Institutes of Health, Bethesda, 20892 MD, United States
^d Department of Molecular & Human Genetics, Baylor College of Medicine, Houston, 77030 TX, United States
^e Marshfield Clinic Research Institute, Marshfield, WI 54449, United States
^f Seattle Children’s Research Institute, Seattle, WA 98145, United States
^g Department of Pediatrics, Washington University of St. Louis, St. Louis, MO 63110, United States
^h Division of Pediatric Endocrinology and Diabetes, University Medical Centre, 89075 Ulm, Germany
ⁱ Rhythm Pharmaceuticals, Boston, MA 02116, United States

^⁎Correspondence to: National Institutes of Health,10 Center Drive, Room 1–3330, MSC 1103, Bethesda, MD 20892-1103, United States.National Institutes of Health,10 Center Drive, Room 1–3330, MSC 1103BethesdaMD20892-1103United States

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Abstract

Background

Smith Magenis Syndrome (SMS) is a rare genetic disorder caused by RAI1 haploinsufficiency. Obesity in people with SMS is believed partially due to dysfunction of the proximal melanocortin 4 receptor (MC4R) pathway. We therefore studied effects of treatment with the MC4R agonist setmelanotide on obesity and hunger, as well as metabolic, cardiac and safety, in individuals with SMS.

Methods

People with SMS received once-daily setmelanotide injections, with the dose titrated bi-weekly to a maximum of 3 mg over ∼1 month; and a full-dose treatment duration of 3mo. The primary outcome was percent change in body weight. Secondary outcomes included hunger, waist circumference, body composition, and safety.

Results

12 individuals, ages 11–39 y, enrolled and 10 completed the full-dose treatment phase. Mean percent change in body weight at end-treatment was − 0.28 % [(95 % CI, −2.1 % to 1.5 %; n = 12; P = 0.66]. Participants experienced a significant decrease in total cholesterol associated with a significant decrease in HDL-cholesterol and a trend for lower LDL-cholesterol. Self-reported hunger was reduced at end-treatment (p = 0.011). All participants reported adverse events (AEs), most commonly injection-site reactions and skin hyperpigmentation. No AEs led to withdrawal or death.

Conclusions

In this trial, setmelanotide did not significantly reduce body weight in participants with SMS. Participants reported significant differences in hunger, but such self-reports are difficult to interpret without a placebo-treated group. The changes in lipid profiles require further investigation. Results of this study do not suggest that dysfunction of the proximal MC4R pathway is the main etiology for obesity in people with SMS.

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Highlights

•	Nonsignificant weight changes in individuals with SMS after setmelanotide treatment.
•	Lipid profiles changed in response to setmelanotide treatment for obesity in SMS.
•	SMS-related obesity may not be primarily caused by proximal MC4R pathway insufficiency.

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Keywords : Obesity, Pharmacotherapy, Setmelanotide, Melanocortin agonist, Smith-Magenis Syndrome, Hyperphagia