CagriSema is Novo Nordisk's combination of cagrilintide (amylin analog) and semaglutide (GLP-1 agonist) in a single weekly injection, activating two independent satiety pathways for additive weight loss.

Amylin analog · Phase III · CagriSema · Spoke 4.6

Cagrilintide: the long-acting amylin analog that adds a second appetite-regulation signal to semaglutide — and what Phase III says about the combination.

Q: How does cagrilintide compare to tirzepatide?

Tirzepatide adds GIP receptor agonism to GLP-1 and produces ~20-22% weight loss. CagriSema adds amylin/CTR/RAMP hindbrain signaling to GLP-1, producing ~22-25% weight loss in Phase III.

By PeptideRadar Research Desk · April 30, 2026

DeveloperNovo Nordisk ClassLong-acting amylin analog (fatty acid-conjugated) Half-life~7 days (weekly dosing) ProgramCagriSema (cagrilintide + semaglutide 2.4 mg) Updated2026-04-30

Cagrilintide is a long-acting amylin analog developed by Novo Nordisk, fatty acid-conjugated for extended half-life and once-weekly dosing. It is being evaluated primarily in combination with semaglutide as "CagriSema" — the rationale being that amylin and GLP-1 regulate appetite through distinct hypothalamic pathways, and combining them could produce additive weight loss beyond what either achieves alone. Phase III CagriSema data showed roughly 22–25% weight loss — data that is reshaping how the obesity pharmacology field thinks about combination peptide approaches.

Key points

Amylin is a 37-amino-acid peptide co-secreted with insulin from pancreatic β-cells. It regulates satiety via calcitonin receptor/RAMP complexes in the area postrema and hypothalamus.
Cagrilintide is a modified amylin analog with a fatty acid chain enabling albumin binding and weekly half-life — analogous to the design approach used for semaglutide.
Phase II data showed ~10% weight loss with cagrilintide monotherapy at 4.5 mg weekly (PMID: 34379949).
CagriSema Phase III: ~22–25% body weight reduction at 68 weeks — exceeding tirzepatide benchmarks in some analyses.
Not yet approved; regulatory submissions expected 2025–2026.
Distinct from pramlintide (Symlin), the short-acting amylin analog already approved for type 1 and 2 diabetes.

Amylin biology: a satiety signal distinct from GLP-1

Amylin (islet amyloid polypeptide, IAPP) is a 37-amino-acid peptide co-secreted alongside insulin from pancreatic β-cells in response to meals. Its primary physiological roles:

Satiety signaling. Amylin acts on calcitonin receptors (CTR) complexed with receptor activity-modifying proteins (RAMPs) — particularly RAMP1 and RAMP3 — in the area postrema (AP) and nucleus tractus solitarius (NTS) in the brainstem. This produces satiety signals that reduce meal size and eating rate.
Gastric emptying slowing. Similar to GLP-1, amylin slows gastric emptying — reducing the rate of nutrient absorption and post-meal glucose peaks.
Glucagon suppression. Amylin suppresses glucagon release after meals, contributing to postprandial glucose regulation.

The key distinction from GLP-1: amylin and GLP-1 activate different receptors and signal through different brain circuits. GLP-1 receptors are expressed in hypothalamic arcuate nucleus neurons (NPY/AgRP and POMC neurons); amylin/CTR/RAMP complexes signal primarily through the hindbrain (AP and NTS). Combining both activates complementary satiety circuits, which is the mechanistic basis for the additive weight loss hypothesis.

Cagrilintide's design: extending amylin half-life

Native amylin has a short half-life (~20 minutes), similar to native GLP-1. Pramlintide (Symlin) — the approved amylin analog — requires three times daily injection. Cagrilintide solves this via a fatty acid chain conjugated to the amylin analog backbone, enabling reversible binding to serum albumin and extending half-life to approximately 7 days (once-weekly injection).

This design mirrors semaglutide's fatty acid approach. The modification also required some sequence changes to the amylin peptide backbone to reduce aggregation propensity — amylin is inherently amyloidogenic (pancreatic amyloid deposits in type 2 diabetes are composed of IAPP aggregates). Cagrilintide's modifications suppress this aggregation while maintaining receptor activity.

Phase II and Phase III clinical evidence

Cagrilintide's clinical development has been rapid and results-positive:

Phase II monotherapy (STEP-1 equivalence study): Cagrilintide 4.5 mg weekly produced ~10% weight loss at 26 weeks in overweight/obese adults without diabetes — comparable to older GLP-1 monotherapies (PMID: 34379949).
CagriSema Phase II combination: Cagrilintide 2.4 mg + semaglutide 2.4 mg weekly over 32 weeks produced ~15% weight loss — exceeding semaglutide monotherapy at 12 weeks by several percentage points, with dose escalation continuing.
CagriSema Phase III (REDEFINE trials): Published data indicates ~22–25% weight loss at 68 weeks in the full dose combination — data that competes with the highest tirzepatide results and represents potentially best-in-class weight loss from a weekly injectable combination.

Nausea and GI side effects from CagriSema are similar to or modestly higher than semaglutide alone — consistent with the additive mechanism bringing additive GI effects alongside additive weight loss.

Cagrilintide vs. pramlintide: the design comparison

Pramlintide (Symlin), approved since 2005, is a short-acting amylin analog requiring TID injection. Its clinical uptake has been limited precisely because of this dosing burden. Cagrilintide's once-weekly design solves the adherence problem. The weight loss from CagriSema substantially exceeds what pramlintide adds to insulin regimens (~3–4 kg in diabetic patients). This is the commercial and clinical case for cagrilintide over the existing amylin therapy.

Why this matters for the research peptide category Cagrilintide is a legitimately novel pharmaceutical compound in late-stage development — not a research chemical sold under RUO framing. It is covered here because it represents the state of the art in peptide-based obesity pharmacology, providing a benchmark against which research peptides like AOD-9604 should be contextualized. The ~22% weight loss from CagriSema sets a new reference point for what combination peptide approaches can achieve when properly developed.

Frequently asked

What is CagriSema?

CagriSema is Novo Nordisk's development program combining cagrilintide (amylin analog) and semaglutide (GLP-1 receptor agonist) in a single weekly injection. The combination activates two independent satiety signaling pathways, producing additive weight loss beyond either component alone.

How does cagrilintide compare to tirzepatide?

Tirzepatide (GIP+GLP-1 dual agonist) produces approximately 20–22% weight loss at maximum dose. CagriSema Phase III data suggests comparable or slightly superior weight reduction (~22–25%). These are different mechanisms: tirzepatide adds GIP receptor agonism to GLP-1; CagriSema adds amylin/CTR/RAMP hindbrain signaling to GLP-1.

Is cagrilintide available as a research peptide?

As of 2026, cagrilintide is in Phase III development as a pharmaceutical drug and is not commercially available as an approved drug or a mainstream research peptide. Some vendors may offer synthetic versions; verify authenticity and purity with particular caution given the compound's pharmaceutical development status.

Does cagrilintide cause nausea like GLP-1 drugs?

CagriSema combination produces GI side effects (nausea, vomiting, constipation) similar to or modestly higher than semaglutide alone — reflecting the additive pharmacology. Amylin alone also slows gastric emptying, which contributes to GI side effects when combined with GLP-1's similar effect.

Reviewer sign-off Reviewed 2026-04-30 by the PeptideRadar Research Desk for RUO compliance, mechanism accuracy, and citation integrity. Corrections: corrections@peptideradar.net.

Amylin biology: a satiety signal distinct from GLP-1

Cagrilintide's design: extending amylin half-life

Phase II and Phase III clinical evidence

Cagrilintide vs. pramlintide: the design comparison

Frequently asked

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