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Setmelanotide Potentially Enhances Obesity Drug Response in Hypothalamic Obesity - Featured image
Medical Research

Setmelanotide Potentially Enhances Obesity Drug Response in Hypothalamic Obesity

Dr. Adrian Vale, MD
Reviewed by Dr. Adrian Vale, MDInternal Medicine · Board-Certified Obesity Medicine
·November 7, 2025·2 min read

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A recent study presented at ObesityWeek suggests that setmelanotide, when used alongside GLP-1 therapy, may lead to a substantial reduction in BMI for individuals with acquired hypothalamic obesity. The research indicates that restoring melanocortin-4 receptor pathway signaling could improve response to other anti-obesity treatments.

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Setmelanotide Potentially Enhances Obesity Drug Response in Hypothalamic Obesity

According to a presentation at ObesityWeek, individuals (both children and adults) with acquired hypothalamic obesity who were treated with setmelanotide in conjunction with GLP-1 therapy experienced a 25.1 percentage point reduction in BMI.

Previously reported data from the TRANSCEND trial at ENDO 2025 indicated that setmelanotide, a melanocortin-4 receptor agonist, resulted in a 19.8-percentage point greater decrease in BMI compared to placebo (P < .0001). This earlier finding highlighted the potential of setmelanotide in managing this specific type of obesity.

The ObesityWeek presentation featured a post-hoc analysis of the TRANSCEND trial, revealing that the observed reduction in BMI with setmelanotide was more pronounced among participants who also used a GLP-1 during the trial. These results suggest a synergistic effect between the two therapies.

Christian L. Roth, MD, a professor of pediatrics at University Washington, stated that the consistent success of setmelanotide underscores the importance of impaired melanocortin-4 receptor pathway signaling in acquired hypothalamic obesity. He noted that setmelanotide, by targeting this pathway, may restore normal physiology and improve responsiveness to other anti-obesity treatments, including GLP-1s. Health tracking apps like Shotlee can help monitor progress and adherence to treatment plans.

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The TRANSCEND study involved 120 participants (children and adults) with hypothalamic obesity resulting from a tumor, lesion, or injury, with a mean age of 19.9 years. Participants were randomly assigned to receive either once-daily setmelanotide or a placebo for up to 60 weeks. The post-hoc analysis then stratified participants based on their concomitant GLP-1 use.

During the trial, fifteen participants received concomitant GLP-1 therapy. Within this subgroup, nine received setmelanotide, and six received a placebo.

Among participants who did not receive a GLP-1 during the trial, setmelanotide resulted in a mean BMI reduction of 15.5 percentage points, compared to a 3.5 percentage point BMI increase with placebo (P < .0001). In contrast, among those who received concomitant GLP-1 therapy, the setmelanotide group experienced a 25.1 percentage point BMI reduction, while the placebo group had a 2-percentage point BMI increase (P < .0001).

Roth emphasized the importance of these findings, stating that they demonstrate that nonresponse to GLP-1 does not necessarily indicate overall treatment resistance. He suggested that in acquired hypothalamic obesity, where alpha-melanocyte-stimulating hormone is deficient, patients may still respond favorably to setmelanotide, even if GLP-1s have previously proven ineffective.

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Originally published by Healio.Read the original article →

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Dr. Adrian Vale, MD — Internal Medicine · Board-Certified Obesity Medicine
Medically reviewed

Dr. Adrian Vale, MD

Internal Medicine · Board-Certified Obesity Medicine

Dr. Adrian Vale is a board-certified internal medicine physician with a clinical focus on obesity medicine and metabolic health. He reviews Shotlee guides and articles on GLP-1 medications, peptide therapy, and weight-management protocols for clinical accuracy.

View all articles reviewed by Dr. Adrian Vale, MD
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