EcnoglutidevsNN1706

Ecnoglutide is a long-acting GLP-1 receptor agonist engineered for once-weekly subcutaneous dosing using a structural design distinct from albumin-binding (semaglutide) or PEGylation. The molecule incorporates extended-half-life modifications that resist DPP-4 enzymatic degradation while maintaining high-affinity binding and full agonist activity at the GLP-1 receptor.

Receptor activation produces the standard GLP-1 pharmacology: glucose-dependent insulin secretion from pancreatic beta cells, suppression of glucagon release from alpha cells, slowed gastric emptying via vagal signalling, and central appetite suppression through hypothalamic and brainstem GLP-1 receptors. The clinical profile in Chinese Phase 3 trials closely mirrors semaglutide — approximately 14-15% body weight loss in obesity studies and substantial HbA1c reductions in type 2 diabetes trials — positioning ecnoglutide as a regional alternative to Wegovy and Ozempic with potentially lower pricing.

Ecnoglutide reflects a broader trend of Chinese biotech companies developing GLP-1 receptor agonists for both domestic and international markets. Sciwind Biosciences has filed for regulatory approval in China and is pursuing international development pathways. The molecule is one of several Chinese-developed GLP-1s approaching commercial launch alongside mazdutide, retatrutide-class triple agonists in early Chinese development, and a wave of biosimilar semaglutide products expected as patents expire in major markets through the late 2020s.

NN1706 is a once-daily GLP-1/GIP/glucagon triple receptor agonist — Novo Nordisk's mechanistic equivalent to Eli Lilly's retatrutide, designed to activate all three pathways simultaneously in a single molecule. Each receptor contributes complementary metabolic effects: GLP-1 agonism centrally suppresses appetite, slows gastric emptying, and stimulates glucose-dependent insulin secretion; GIP agonism augments insulin response and modulates adipose lipid handling; and glucagon receptor agonism in the liver drives fatty acid oxidation, ketogenesis, and hepatic glucose output, while in brown and beige adipose tissue it promotes thermogenesis and increases whole-body energy expenditure.

The key engineering challenge in any glucagon-containing multi-agonist is balancing glucagon's hyperglycemic tendency against the glucose-lowering effect of GLP-1 and GIP. NN1706's receptor potency ratios are tuned so that incretin-driven insulinotropic effects sufficiently offset glucagon-driven glucose production, producing net glycemic improvement alongside enhanced fat oxidation. The glucagon component is what differentiates triple agonists like NN1706 and retatrutide from dual GLP-1/GIP agonists like tirzepatide — the additional energy-expenditure and hepatic-fat-mobilising effects of glucagon are the main reason triple agonists have produced higher weight-loss numbers in early trials.

The pharmacokinetic profile gives NN1706 a half-life of roughly 14-18 hours, matched to once-daily subcutaneous dosing rather than the once-weekly schedule of retatrutide. The trade-off is more injections per week against tighter dose control, smoother plasma concentrations, and faster ability to adjust or pause dosing if side effects emerge. The first human data published in 2026 from Phase 1 trials in rodents, monkeys, and humans showed meaningful weight loss with an acceptable initial tolerability profile, setting up Phase 2 obesity and type 2 diabetes trials.