Safety profile

Side effects of Retatrutide

In trials, Retatrutide shows a side-effect profile similar to established GLP-1 compounds. The most common adverse effects are gastrointestinal and dose-dependent — most appear during the first weeks of therapy.

Gastrointestinal side effects (common)

Nausea
up to 45%
Most common effect, especially during dose escalation. Usually mild to moderate.
Vomiting
10–20%
Occurs mainly in the first 4–8 weeks, resolves in most patients.
Diarrhea
15–25%
Dose-dependent, typically self-limiting.
Constipation
10–15%
Counterpart to diarrhea, often driven by delayed gastric emptying.
Loss of appetite
expected
Not really an adverse effect — part of the intended action.

Cardiovascular effects

Phase II data showed a mild increase in resting heart rate averaging 5–7 beats per minute — similar to Semaglutide and Tirzepatide. Blood pressure decreased slightly in most trials. Long-term cardiovascular outcome data are still pending.

Rare but relevant risks

Like other incretin mimetics, Retatrutide may theoretically increase risk of pancreatitis, gallstones or — with a corresponding family history — medullary thyroid carcinoma (extrapolated from animal studies with other GLP-1 compounds). These endpoints are systematically captured in the Phase III program.

Contraindications (expected)

  • Personal or family history of medullary thyroid carcinoma
  • Multiple endocrine neoplasia type 2 (MEN2)
  • Pregnancy and breastfeeding
  • History of acute pancreatitis

Important: All figures come from published Phase I and Phase II data. The final side-effect profile will only be known after completion of the TRIUMPH program and approval. This page does not replace medical advice.

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