Pemvidutide

MOMENTUM Phase 2 Obesity Trial

The MOMENTUM trial evaluated pemvidutide at multiple doses (1.2 mg and 1.8 mg weekly) in adults with obesity or overweight (BMI ≥27 with comorbidity). At 48 weeks, participants receiving pemvidutide 1.8 mg achieved mean body weight reduction of approximately 10.3%, with the key differentiator being favorable body composition: approximately 65% of weight lost was fat mass, suggesting meaningful preservation of lean body mass. The trial also demonstrated improvements in waist circumference, blood pressure, and lipid parameters. [Altimmune press release and Obesity 2023 presentations]

NAFLD/NASH (Liver Fat Reduction)

Pemvidutide has demonstrated significant reductions in liver fat content, consistent with the direct hepatic effects of glucagon receptor agonism. In a Phase 1b study in patients with hepatic steatosis, pemvidutide produced dose-dependent reductions in liver fat as measured by MRI-proton density fat fraction (MRI-PDFF). Reductions of up to 50-60% from baseline were observed, positioning pemvidutide as a potential treatment for NAFLD and NASH. The glucagon-mediated direct hepatic lipid oxidation provides a mechanism distinct from weight-loss-mediated liver fat reduction.

Body Composition Analysis

Dual-energy X-ray absorptiometry (DEXA) analysis from clinical trials confirmed that pemvidutide produces a higher ratio of fat mass loss to total weight loss compared to historical data from GLP-1 receptor agonist trials. This body composition advantage is clinically meaningful for several reasons: preserved lean mass maintains resting metabolic rate (reducing weight regain risk), protects against sarcopenia (particularly relevant in older adults), and maintains functional capacity and physical performance.

Cardiovascular Risk Factors

Across clinical studies, pemvidutide produced improvements in systolic blood pressure, triglycerides, and LDL cholesterol consistent with the magnitude of weight loss achieved. The dual mechanism may provide additional cardiovascular benefits through glucagon-mediated improvements in hepatic lipid metabolism.

Clinical Research Protocols

Pemvidutide's clinical development includes trials for obesity and NAFLD:

MOMENTUM Phase 2 Obesity Trial (NCT05295875): Randomized, double-blind, placebo-controlled, 48-week study evaluating pemvidutide 1.2 mg and 1.8 mg weekly in adults with BMI ≥30 (or ≥27 with comorbidity). Primary endpoint: percent change in body weight from baseline at 48 weeks. Secondary endpoints include body composition (DEXA), waist circumference, blood pressure, and metabolic parameters. Dose escalation protocol over initial weeks to target maintenance dose.

NAFLD Trial (NCT05646693): Phase 2 study evaluating pemvidutide in patients with non-alcoholic fatty liver disease. Primary endpoint: change in liver fat content measured by MRI-PDFF. This trial leverages the direct hepatic effects of glucagon receptor agonism for liver fat reduction.

Dosing Protocol: Pemvidutide is administered as a once-weekly subcutaneous injection. Dose escalation from a starting dose to the target maintenance dose (1.2 mg or 1.8 mg) is used to mitigate gastrointestinal side effects.

Comparison to Related Compounds

Pemvidutide vs. Semaglutide: Pemvidutide's total weight loss (~10.3%) is less than semaglutide 2.4 mg (~15.8%), but the body composition of weight loss may be more favorable, with greater fat mass loss relative to total weight loss. The glucagon component provides direct hepatic lipid oxidation effects that semaglutide lacks. For patients where lean mass preservation is a priority (older adults, sarcopenic obesity), pemvidutide's profile may be advantageous.

Pemvidutide vs. Tirzepatide: Tirzepatide produces substantially greater total weight loss through dual GIP/GLP-1 agonism. However, pemvidutide's glucagon component may provide superior liver fat reduction through direct hepatic mechanisms and better lean mass preservation. The two agents target different receptor combinations (GIP/GLP-1 vs GLP-1/glucagon).

Pemvidutide vs. Retatrutide: Retatrutide is a triple agonist that includes glucagon receptor activity alongside GIP and GLP-1. Compared to pemvidutide's dual GLP-1/glucagon mechanism, retatrutide adds GIP agonism, which may contribute to the greater total weight loss observed (24.2% vs ~10.3%). Both share the glucagon-mediated liver fat reduction advantage.

Pemvidutide vs. Survodutide (BI 456906): Both are GLP-1/glucagon dual agonists but differ in molecular design, dosing, and clinical focus. Survodutide (Boehringer Ingelheim) is more advanced in development and has shown greater weight loss in Phase 2 trials (~14.9% at 46 weeks). Both share the theoretical advantage of glucagon-mediated hepatic lipid oxidation for NASH/NAFLD.

Ongoing & Future Research

Pemvidutide's clinical development is focused on obesity and NAFLD:

• MOMENTUM Phase 2b Extension (NCT05295875): Extended follow-up from the MOMENTUM trial to assess durability of weight loss, body composition changes, and long-term safety of pemvidutide in obesity.

• NAFLD Phase 2 (NCT05646693): Evaluation of pemvidutide's effect on liver fat content and potential NASH resolution. Histological endpoints may be included in future Phase 3 designs.

• Phase 3 Planning: Altimmune has indicated plans for Phase 3 trials in obesity and/or NAFLD, pending final Phase 2 data readouts. The body composition differentiation (lean mass preservation) is expected to be a key focus of the Phase 3 program.

• Sarcopenic Obesity: Potential future studies in older adults with sarcopenic obesity, where the lean mass preservation profile of pemvidutide may provide particular clinical benefit.