CT-388vsDanuglipron

CT-388 is a once-weekly subcutaneous dual GLP-1/GIP receptor agonist, mechanistically similar to tirzepatide but with a distinct molecular structure designed for differentiated pharmacology. Activation of both receptors produces complementary metabolic effects: GLP-1 receptor agonism centrally suppresses appetite through hypothalamic and brainstem signalling, slows gastric emptying, and stimulates glucose-dependent insulin secretion from pancreatic beta cells, while GIP receptor agonism enhances beta-cell insulin response, modulates lipid handling in adipose tissue, and amplifies the central anorectic effect of GLP-1 through distinct hypothalamic neuronal circuits.

The molecule was engineered with a balanced potency profile across the two receptors and incorporates fatty acid acylation that enables strong albumin binding, extending half-life to approximately one week. This pharmacokinetic profile supports once-weekly subcutaneous dosing with stable plasma exposure across the dosing interval, which is associated with better gastrointestinal tolerability than less stable formulations that produce sharp peaks and troughs.

In the Phase 2 obesity trial of 469 participants, CT-388 produced up to 22.5% placebo-adjusted body weight reduction at 48 weeks at the highest dose. The weight-loss curve had not yet plateaued at the end of the trial, suggesting further reductions might be achievable with longer dosing. Roche acquired Carmot Therapeutics in late 2024 specifically to obtain CT-388, positioning it as their lead anti-obesity asset competing directly against tirzepatide and the next-generation Lilly and Novo Nordisk pipeline.

Danuglipron (PF-06882961) is a non-peptide small molecule GLP-1 receptor agonist designed for oral administration without the food and water restrictions that limit Rybelsus (oral semaglutide). As a small molecule rather than a peptide, it is not destroyed by gastric acid or proteolytic enzymes, allowing flexible oral dosing.

The molecule binds the GLP-1 receptor outside the orthosteric peptide-binding pocket, producing biased agonism that activates the same downstream G-protein signalling as native GLP-1 — glucose-dependent insulin secretion, glucagon suppression, slowed gastric emptying, and central appetite regulation through hypothalamic and brainstem GLP-1 receptors. The key engineering feature is its short pharmacokinetic profile, with a half-life around 6-9 hours, designed for twice-daily dosing rather than once-daily exposure to limit peak plasma concentrations and improve gastrointestinal tolerability.

In Phase 2 obesity and type 2 diabetes trials, danuglipron produced meaningful weight loss and HbA1c reductions, validating the small-molecule oral GLP-1 concept. However, gastrointestinal tolerability was problematic — over 70% of trial participants experienced nausea — and the program was ultimately discontinued by Pfizer in 2025 following a single case of suspected drug-induced liver injury in a healthy volunteer. Pfizer pivoted to alternative oral GLP-1 candidates with reduced hepatic exposure profiles. Danuglipron remains a high-search-volume topic because of its prominent failure and because it set early benchmarks for what oral small-molecule GLP-1 drugs (notably orforglipron from Eli Lilly) needed to beat to succeed.