Peptide News Digest

#Cardiometabolic

2 stories

Research · View digest

CROI 2026 Plenary (Dr. Todd Brown, Johns Hopkins): GLP-1 Receptor Agonists Show Cardiometabolic, Smoking, Liver, and Gut Benefits in People Living With HIV — Seven Poster Presentations Plus an Oral Abstract

The Conference on Retroviruses and Opportunistic Infections (CROI 2026, March 9-12) featured an oral plenary by Dr. Todd Brown of Johns Hopkins Medicine titled 'GLP-1 Agonists: Are They a Cure for Everything?' alongside one oral abstract and seven posters on the use of GLP-1 receptor agonists in people living with HIV (PLWH). The findings: GLP-1s generally work well in PLWH, may improve liver fibrosis, gut tissue immune health, and cardiovascular risk, and may reduce smoking on top of the established weight loss and diabetes effects. One oral abstract suggested potential to reverse the gut damage that persists from very early HIV infection despite effective ART. Brown's plenary concluded the enthusiasm is warranted but flagged unanswered questions around long-term use and global access — particularly relevant for PLWH in low- and middle-income countries.

Clinical Trials · View digest

Altimmune Pemvidutide IMPACT Phase 2b Week 48 Oral Presentation (May 28, 17:00 CEST): 1.8 mg Dose Cuts Triglycerides 23.7%, Total Cholesterol 15.4%, Weight 7.5%, Waist 5.3 cm at ~1% Discontinuation

Altimmune presented the full Week 48 top-line IMPACT Phase 2b oral data for pemvidutide in MASH today at EASL 2026 Barcelona (Dr. Mazen Noureddin, Houston Methodist Hospital, 17:00 CEST). The 1.8 mg dose reduced triglycerides 23.7%, total cholesterol 15.4%, body weight 7.5%, BMI 3.0 kg/m², and waist circumference 5.3 cm, alongside blood pressure reduction. Safety held at 48 weeks with roughly 1% discontinuation due to adverse events and mostly mild-to-moderate gastrointestinal events. Previously reported: 27.8% (1.2 mg) and 32.4% (1.8 mg) of patients achieved combined ELF and LSM improvements versus 3.2% on placebo. The 48-week analysis carries the 'Best of EASL 2026' designation. Pemvidutide is a balanced 1:1 GLP-1/glucagon dual receptor agonist peptide with FDA Fast Track + Breakthrough Therapy Designations for MASH. The cardiometabolic-risk-factor profile positions pemvidutide as differentiated on the lipid and cardiovascular axis versus pure GLP-1 agonists.