MariTidevsPemvidutide

MariTide (maridebart cafraglutide) is a peptide-antibody conjugate combining a GLP-1 receptor agonist peptide with a GIP receptor antagonist antibody. This dual GLP-1 agonist + GIP antagonist mechanism is distinctive — most competing dual incretin drugs (tirzepatide, CT-388, VK2735) activate both receptors. The rationale for GIP antagonism is based on genetic and pharmacological evidence that loss-of-function in GIP signalling is associated with reduced obesity, suggesting that blocking rather than activating GIP may produce superior weight-loss outcomes.

The GLP-1 agonist component drives the established appetite-suppression and glycemic-control effects of the incretin pathway. The GIP receptor antagonist antibody simultaneously blocks GIP signalling at adipocytes and centrally, which preclinical data suggest enhances energy expenditure, reduces lipid storage, and amplifies the weight-loss effect of GLP-1 receptor activation. Whether GIP agonism (as in tirzepatide) or GIP antagonism (as in MariTide) is superior remains an open question that Phase 3 head-to-head data may eventually resolve.

The antibody-conjugated structure produces an exceptional pharmacokinetic profile, with a half-life of approximately three weeks. This supports once-monthly subcutaneous dosing — a unique practical advantage over the once-weekly schedules of all other late-stage obesity drugs. Phase 2 results showed roughly 20% body weight loss at 52 weeks. Animal studies have also suggested slower weight regain after discontinuation than seen with shorter-acting GLP-1 agonists, possibly due to the prolonged drug exposure during the washout period. Phase 3 MARITIME trials launched in 2026 will define the molecule's clinical positioning.

Pemvidutide (ALT-801) is a once-weekly subcutaneous dual GLP-1 and glucagon receptor agonist, mechanistically similar to mazdutide and survodutide but with a distinct molecular design and a primary development focus on metabolic dysfunction-associated steatohepatitis (MASH) alongside obesity. The dual mechanism combines appetite suppression with enhanced energy expenditure and direct hepatic fat mobilisation.

The GLP-1 receptor component drives the established central appetite suppression through hypothalamic and brainstem signalling, slows gastric emptying, and stimulates glucose-dependent insulin secretion. The glucagon receptor agonism component is what differentiates pemvidutide from pure GLP-1 drugs — glucagon binding in hepatocytes activates adenylyl cyclase and protein kinase A, driving up fatty acid beta-oxidation and ketogenesis while reducing de novo lipogenesis. This directly mobilises stored hepatic triglycerides for energy use rather than continued storage, addressing the core pathology of MASH. In adipose tissue and beyond, glucagon signalling also raises whole-body energy expenditure through thermogenic and futile-cycle mechanisms.

The receptor potency ratio is balanced so that glucagon-driven hepatic glucose output is offset by GLP-1-driven insulinotropic effects, yielding net glycemic improvement alongside enhanced fat oxidation. Phase 2b results in obesity demonstrated approximately 15.6% mean body weight loss at 48 weeks, and parallel MASH trials showed significant reductions in liver fat content alongside improvements in fibrosis markers. Phase 3 trials in both obesity and MASH are now underway, positioning pemvidutide as Altimmune's lead asset and a competitor to mazdutide and survodutide in the dual GLP-1/glucagon class.