For laboratory research use only. Not for human consumption or veterinary use.
Structural Overview
Cagrilintide (development code AM833) is a 37-amino-acid synthetic analog of human amylin (islet amyloid polypeptide, IAPP) engineered for selective activation of the AMY1R complex — the heterodimer formed by the calcitonin receptor (CTR) and receptor-activity-modifying protein 1 (RAMP1). The C-terminal fatty-acid acylation enables albumin binding and extends circulating half-life to ~7 days in published research-model pharmacokinetics. CAS 1415456-99-3; molecular weight 4409.01 g/mol.
Receptor Pharmacology
Native amylin is co-secreted from pancreatic β-cells with insulin and acts at AMY1R in the area postrema, nucleus tractus solitarius, and hypothalamic regions controlling satiety and gastric emptying. Cagrilintide preserves this receptor selectivity through engineered substitutions characterized by Kruse et al. (J Med Chem 2021, DOI 10.1021/acs.jmedchem.1c00565). The amylin pathway is mechanistically non-overlapping with the GLP-1 / GIP / glucagon incretin axis, which underlies the additive research-model effects observed when cagrilintide is studied in combination with incretin agonists.
Published Phase 2 and Phase 3 Research Outcomes
Phase 2 monotherapy dose-finding work (Lau DCW et al., The Lancet 2021, PMID 34798060) established once-weekly cagrilintide pharmacology. Phase 2 combination with semaglutide in T2DM (Frias JP et al., The Lancet 2023, PMID 37364590) demonstrated tolerability of the co-administration regimen. The Phase 3 REDEFINE-1 trial (Garvey WT et al., NEJM 2025, PMID 40544433) reported approximately 22.7% mean body-weight reduction with the co-administered cagrilintide + semaglutide combination (CagriSema) at 68 weeks. The regional Phase 3 REDEFINE-5 (Yamauchi T et al., Lancet Diabetes & Endocrinology 2026, PMID 42009015) extended these findings to Japanese and Taiwanese research populations. No human dosing, administration route, reconstitution, or therapeutic protocol is provided — these are reported research outcomes from published primary literature only.
Regulatory Status
Cagrilintide is not FDA-approved for any human indication as a standalone product. Novo Nordisk’s CagriSema combination filing is the active regulatory path, with PDUFA action anticipated in late 2026. Standalone cagrilintide has no approved marketing context. There is no 503A/503B compounding pathway for cagrilintide. For research use only.
Counter-Evidence and Safety Context (Disclosed Honestly)
Cagrilintide monotherapy efficacy is modest relative to the combination: Phase 2 monotherapy reached approximately 10–11% body-weight reduction; the headline ~22.7% figure is specifically for the CagriSema combination with semaglutide. Researchers comparing cagrilintide to GLP-1 monotherapy alone should expect substantially lower standalone effect sizes. Published Phase 2/3 trials (Frias PMID 37364590; Garvey PMID 40544433) document nausea, vomiting, and diarrhea as dose-related adverse events consistent with the broader incretin-class profile. REDEFINE-2 (T2DM) and REDEFINE-3 (head-to-head vs tirzepatide) are pending peer-reviewed publication at time of this writing.
Supply Chain Integrity
Cagrilintide is one of three peptides — with retatrutide and tirzepatide — currently subject to elevated grey-market quality risk per industry reports. Independent third-party testing from late 2024 through early 2026 documented widespread quality failures across a significant share of sampled vendors selling these three peptides. Each Artemis Labs vial ships with a lot-specific Certificate of Analysis from a named third-party laboratory, mass-spectrometric identity confirmation (MW 4409.01 g/mol target), HPLC purity chromatogram (≥99% target), residual-solvent assay, and chain-of-custody documentation from manufacture through shipping. See the reading a Certificate of Analysis guide for the verification framework.
For laboratory research use only. No human dosing, administration, therapeutic, diagnostic, or preventative claim is made. These statements have not been evaluated by the FDA.




Reviews
There are no reviews yet.