Tirzepatide
181,50 €
- Body weight reduction of up to 22.5% in SURMOUNT-1.
- A 2.0–2.3% reduction in HbA1c in the SURPASS program.
- Superior glycemic control compared with semaglutide in a direct comparative trial.
- Reduction in triglycerides and LDL.
- Improvement in sleep apnea in the SURMOUNT-OSA trial.
- Approved by the FDA for T2DM as Mounjaro and for obesity as Zepbound.
MECHANISM OF ACTION
Dual GIP/GLP-1 receptor coagonist, with a GIP-based mechanism. Activation of the GIPR potentiates insulin, suppresses glucagon, promotes direct lipolysis in adipocytes, and modulates the central nervous system. GLP-1R promotes satiety, delays gastric emptying, and stimulates glucose-dependent insulin secretion. The C20 diacid fatty acid chain extends the half-life to approximately 5 days with weekly administration.
KEY BENEFITS
- Body weight reduction of up to 22.5% in SURMOUNT-1.
- A 2.0–2.3% reduction in HbA1c in the SURPASS program.
- Superior glycemic control compared with semaglutide in a direct comparative trial.
- Reduction in triglycerides and LDL.
- Improvement in sleep apnea in the SURMOUNT-OSA trial.
- Approved by the FDA for T2DM as Mounjaro and for obesity as Zepbound.
SIDE EFFECTS AND SAFETY
Gastrointestinal effects such as nausea, vomiting, and diarrhea. Class warning regarding C-cell thyroid tumors. Risk of pancreatitis. Dose titration is essential. Monitor renal function if gastrointestinal effects occur.
RESEARCH AND CLINICAL NOTES
SURPASS-2, a head-to-head trial against semaglutide: tirzepatide was superior in both HbA1c and body weight. SURMOUNT-1: 22.5% reduction in body weight. Dual-action peptide approved by the FDA for dual indications, marketed as Mounjaro and Zepbound. Second-largest commercial impact after semaglutide.
TARGET PROFILE:
Metabolic medicine, endocrinology, bariatric medicine, and weight loss.
| Weight | ,26 kg |
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