Effects of tesamorelin, a growth hormone-releasing factor, in HIV-infected patients with abdominal fat accumulation: a randomized placebo-controlled trial with a safety extension.
Falutz. Julian J; Potvin. Diane D; Mamputu. Jean-Claude JC; Assaad. Hani H; Zoltowska. Monika M; Michaud. Sophie-Elise SE; Berger. Daniel D; Somero. Michael M; Moyle. Graeme G; Brown. Stephen S; Martorell. Claudia C; Turner. Ralph R; Grinspoon. Steven S
Key Findings
- Visceral adipose tissue (VAT) fell 10.9% (â21â¯cm²) vs. 0.6% with placebo after 6â¯months (pâ¯<â¯0.0001).
- Continuing tesamorelin for 12â¯months led to ~18% VAT reduction (pâ¯<â¯0.001); stopping the drug caused the benefit to disappear quickly.
- Bodyâimage scores improved (both patientâreported belly distress and physicianârated belly profile, pâ¯ââ¯0.02).
- IGFâ1 rose significantly, but fasting glucose and other metabolic safety markers stayed unchanged.
Practical Outcomes
- For biohackers interested in cutting deep belly fat, tesamorelin at 2â¯mg subcutaneously each day appears effective and safe over at least a year, provided you monitor IGFâ1 and keep an eye on glucose. The drugâs benefits fade if you stop, so continuous dosing is needed for sustained results. Access typically requires a prescription, so consider legal/medical pathways before experimenting.
Summary
In a 12âmonth trial with HIVâpositive adults on antiretroviral therapy, daily injections of 2â¯mg tesamorelin cut visceral belly fat by about 11% after six months and roughly 18% after a year, without raising blood sugar or causing major side effects. Participants also felt better about their midsection shape.
Abstract
HIV-infected patients receiving antiretroviral therapy often demonstrate excess visceral fat. A growth hormone-releasing factor, tesamorelin, may selectively reduce visceral fat in this population. We investigated the effects of tesamorelin (GHRH(1-44)) in HIV-infected patients with central fat accumulation. A 12-month study of 404 HIV-infected patients with excess abdominal fat in the context of antiretroviral therapy was conducted between January 2007 and October 2008. The study consisted of 2 sequential phases. In the primary efficacy phase (months 0-6), patients were randomly assigned to receive tesamorelin [2 mg subcutaneous (SC) every day] or placebo in a 2:1 ratio. In the extension phase (months 6-12), patients receiving tesamorelin were rerandomized to continue on tesamorelin (2 mg SC every day) or switch to placebo. Patients initially randomized to placebo switched to tesamorelin. Patients and investigators were blinded to treatment assignment throughout the study. The primary endpoint was visceral adipose tissue (VAT). Secondary endpoints included body image, IGF-I, safety measures, including glucose, and other body composition measures. VAT decreased by -10.9% (-21 cm(2)) in the tesamorelin group vs. -0.6% (-1 cm(2)) in the placebo group in the 6-month efficacy phase, P < 0.0001. Trunk fat (P < 0.001), waist circumference (P = 0.02), and waist-hip-ratio (P = 0.001) improved, with no change in limb or abdominal SC fat. Insulin-like growth factor-1 increased (P < 0.001), but no change in glucose parameters was observed. Patient rating of belly appearance distress (P = 0.02) and physician rating of belly profile (P = 0.02) were significantly improved in the tesamorelin vs. placebo-treated groups. The drug was well tolerated. VAT was reduced by approximately 18% (P < 0.001) in patients continuing tesamorelin for 12 months. The initial improvements over 6 months in VAT were rapidly lost in those switching from tesamorelin to placebo. Tesamorelin reduces visceral fat by approximately 18% and improves body image distress in HIV-infected patients with central fat accumulation. These changes are achieved without significant side effects or perturbation of glucose.
Study Information
pubmed
2010
10.1097/qai.0b013e3181cbdaff