Tirzepatide vs Cagrilintide
Comprehensive side-by-side comparison of mechanisms, dosing, side effects, and research
Also: Mounjaro, Zepbound
Tirzepatide is a single peptide that activates two receptors at once: GIP and GLP-1, the two main incretin hormones your gut releases after eating. It is FDA-approved as Mounjaro for type 2 diabetes and as Zepbound for chronic weight management and obstructive sleep apnea, and it has produced the largest weight-loss numbers of any approved drug to date. Like semaglutide, this is a heavily trialed, fully approved medicine, not a gray-market research compound.
Also: AM833, NN9838
Cagrilintide (also called AM833) is a long-acting synthetic analog of amylin, the gut-brain satiety hormone co-secreted with insulin by pancreatic beta cells. It is an investigational once-weekly injectable being developed by Novo Nordisk for obesity, most prominently as the amylin half of CagriSema (cagrilintide plus semaglutide). It is not yet approved as a standalone drug, but it has cleared phase 2 trials and is in late-stage development.
Key Comparison Insights
- Tirzepatide is FDA approved, while Cagrilintide remains in research stages.
- Both peptides belong to the Weight Loss category, suggesting similar primary applications.
- Tirzepatide has stronger research evidence (FDA Approved) compared to Cagrilintide (Human Trials).
Detailed Comparison
| Attribute | Tirzepatide | Cagrilintide |
|---|---|---|
| Category | Weight Loss | Weight Loss |
| FDA Status | FDA Approved | Not FDA Approved |
| Clinical Status | Pre I II III IV FDA | Pre I II III IV FDA |
| Mechanism of Action | Tirzepatide is a dual agonist, meaning it switches on both the GIP receptor and the GLP-1 receptor with one molecule. GLP-1 activation boosts glucose-dependent insulin release, suppresses glucagon, slows gastric emptying, and reduces appetite through the brain. Adding GIP activation appears to enhance insulin response and improve how fat tissue handles energy, and the combination seems to outperform hitting GLP-1 alone. As with semaglutide, the peptide carries a fatty-acid chain that binds albumin to extend its half-life enough for once-weekly dosing. The exact reason the GIP arm adds so much benefit is still being worked out, but the clinical effect of combining the two is clear. | Cagrilintide is a non-selective agonist of the amylin and calcitonin receptor family. It activates amylin receptors (which are calcitonin receptors paired with RAMP accessory proteins) to signal satiety in the brain, slow gastric emptying, and blunt the post-meal glucagon rise. Mechanistic work in mice shows it reduces body weight mainly through amylin receptors AMY1R and AMY3R acting in the hindbrain, with the area postrema as a key entry point and downstream signaling through the nucleus of the solitary tract and parabrachial nucleus. Notably, weight loss in those studies persisted even after the acute appetite-suppressing effect faded, hinting at effects on energy balance beyond simple food-intake reduction. Chemically it is built on a pramlintide-like 37-amino-acid backbone with substitutions and a fatty-diacid chain attached to extend its half-life to roughly a week, enabling once-weekly dosing. |
| Common Dosing | 5-15 mg weekly (after titration) Once weekly | 2.4 mg weekly Once weekly |
| Administration | Subcutaneous injection weekly | Subcutaneous injection once weekly |
| Typical Duration | Long-term / chronic use | Long-term / chronic use expected |
| Best Time to Take | Morning, same day each week | Any consistent time weekly |
Possible Side Effects May vary by individual |
|
|
| Research Summary | The trial evidence is strong and recent. In SURMOUNT-1 (New England Journal of Medicine, 2022), adults with obesity but without diabetes lost an average of 22.5% of body weight on the 15 mg dose over 72 weeks, versus 2.4% on placebo, with about 9 in 10 participants losing weight. In a head-to-head trial, SURMOUNT-5 (2025), tirzepatide produced roughly 20% weight loss versus about 14% for semaglutide. The SURPASS diabetes program showed strong HbA1c reductions, and a large cardiovascular outcomes trial supported its safety profile. Side effects mirror other incretin drugs: mostly nausea, diarrhea, and other gastrointestinal issues, generally worst during dose titration. These are large, randomized, peer-reviewed trials, putting tirzepatide among the best-evidenced metabolic drugs available. | Cagrilintide has real human data, which sets it apart from most peptides in this category. In a 2021 Lancet phase 2 dose-finding trial (Lau et al.), once-weekly cagrilintide at 4.5 mg produced about 10.8% mean body weight loss over 26 weeks, beating both placebo (around 3%) and liraglutide 3.0 mg (around 9%), establishing that amylin agonism alone can drive clinically meaningful weight loss. Its bigger story is combination therapy: paired with semaglutide as CagriSema, it advanced into phase 3 REDEFINE trials for obesity and type 2 diabetes, with reported weight loss in the low 20% range, though final results came in somewhat below the most optimistic expectations. Side effects are dominated by the expected gastrointestinal effects (nausea, vomiting) common to gut-hormone drugs. As of 2026 cagrilintide is investigational and not FDA-approved on its own. The evidence is genuinely human and well-controlled here, which is rare, but it is still a drug under regulatory review rather than an approved therapy. |
Frequently Asked Questions: Tirzepatide vs Cagrilintide
What is the difference between Tirzepatide and Cagrilintide?
Tirzepatide is a weight loss peptide that tirzepatide is a single peptide that activates two receptors at once: gip and glp-1, the two main incretin hormones your gut releases after eating. it is fda-approved as mounjaro for type 2 diabetes and as zepbound for chronic weight management and obstructive sleep apnea, and it has produced the largest weight-loss numbers of any approved drug to date. like semaglutide, this is a heavily trialed, fully approved medicine, not a gray-market research compound. Cagrilintide is a weight loss peptide that cagrilintide (also called am833) is a long-acting synthetic analog of amylin, the gut-brain satiety hormone co-secreted with insulin by pancreatic beta cells. it is an investigational once-weekly injectable being developed by novo nordisk for obesity, most prominently as the amylin half of cagrisema (cagrilintide plus semaglutide). it is not yet approved as a standalone drug, but it has cleared phase 2 trials and is in late-stage development. The main differences lie in their mechanisms of action and clinical applications.
Which is better, Tirzepatide or Cagrilintide?
Neither is universally "better" - the choice depends on your specific goals. Tirzepatide is typically used for weight loss purposes, while Cagrilintide is used for weight loss. Always consult with a healthcare provider to determine which may be appropriate for your situation.
Can Tirzepatide and Cagrilintide be used together?
Some peptide protocols combine multiple compounds for synergistic effects. However, using Tirzepatide and Cagrilintide together should only be considered under medical supervision, as both compounds have their own side effect profiles and potential interactions. Research on their combined use may be limited.