AmycretinvsSemaglutide

Amycretin is a unimolecular co-agonist that simultaneously activates both the GLP-1 receptor and the amylin (AMY) receptor — the first peptide engineered to combine these two complementary satiety pathways in a single molecule rather than as a two-drug combination. The design philosophy is to deliver the additive weight-loss benefit demonstrated by CagriSema (semaglutide + cagrilintide) without the manufacturing, dosing, and patient-acceptance complexities of co-formulating two separate drugs.

The GLP-1 component drives appetite suppression centrally through hypothalamic POMC/CART activation and NPY/AgRP inhibition, slows gastric emptying via vagal signalling, and stimulates glucose-dependent insulin secretion from pancreatic beta cells. The amylin component activates calcitonin-receptor/RAMP heterodimer complexes concentrated in the area postrema and nucleus tractus solitarius — brainstem regions outside the blood-brain barrier that form a parallel satiety circuit reducing meal size and food-seeking behaviour through neuroanatomically distinct pathways.

Because GLP-1 and amylin signal through different receptor families and target different neurons in the appetite control network, their effects are additive rather than redundant. Phase 1b/2a data showed up to 22% body weight reduction at 36 weeks for the subcutaneous form — comparable to CagriSema with a simpler one-molecule profile. A particularly notable feature is the parallel development of an oral formulation, which would be the first oral peptide combination therapy for obesity if approved. Novo Nordisk's branded development name is zenagamtide, and the molecule is positioned as the company's strategic answer to retatrutide and tirzepatide.

Semaglutide is a modified version of the natural incretin hormone GLP-1, engineered with 94% structural homology to the native peptide. It binds to GLP-1 receptors expressed throughout the body, triggering a cascade of metabolic effects. In the pancreas, it stimulates glucose-dependent insulin secretion from beta cells while suppressing glucagon release from alpha cells, providing dual glycemic control that only activates when blood sugar is elevated.

In the central nervous system, semaglutide crosses the blood-brain barrier and acts on GLP-1 receptors in the hypothalamic arcuate nucleus and the brainstem's nucleus tractus solitarius. This suppresses appetite by modulating POMC/CART (anorexigenic) and NPY/AgRP (orexigenic) neuronal pathways. The result is a significant reduction in hunger, food cravings, and caloric intake — patients typically experience a fundamental shift in their relationship with food.

The extended duration of action comes from a C18 fatty di-acid chain attached at position 26 (lysine), which enables strong non-covalent binding to circulating albumin. This albumin binding shields semaglutide from DPP-4 enzymatic degradation — the process that destroys native GLP-1 within minutes — extending its half-life to approximately 7 days. Additionally, semaglutide slows gastric emptying through vagal nerve signaling, contributing to post-meal satiety and reduced glycemic excursions.