Retatrutide 10 mg
109,00 €
- Body weight reduction of up to 24% in Phase II trials; the most potent in its class.
- Greater reduction in body fat compared to tirzepatide.
- Improved glycemic control through multiple mechanisms.
- Improvement in cardiovascular risk factors.
- Potential for treating NASH and reducing liver fat.
MECHANISM OF ACTION
Triple agonist: GLP-1R for satiety and insulin secretion; GIPR for glucose-dependent insulin secretion and energy expenditure through activation of brown adipose tissue; and the glucagon receptor for energy expenditure, lipolysis, and normalization of hepatic glucose production. The GIP base conjugated with a fatty acid extends the half-life. Triple-receptor activation provides a superior metabolic effect compared to dual agonists.
KEY BENEFITS
- Body weight reduction of up to 24% in Phase II trials; the most potent in its class.
- Greater reduction in body fat compared to tirzepatide.
- Improved glycemic control through multiple mechanisms.
- Improvement in cardiovascular risk factors.
- Potential for treating NASH and reducing liver fat.
SIDE EFFECTS AND SAFETY
Prominent gastrointestinal side effects, such as nausea, vomiting, and diarrhea. Its action on the glucagon receptor leads to increased energy expenditure and possible mild hyperglycemia at the start of treatment. Titration minimizes intolerance.
RESEARCH AND CLINICAL NOTES
Jastreboff et al. (NEJM 2023): 24.2% reduction in body weight at 48 weeks with the highest dose; the highest result to date in a weight-loss drug trial. Phase III TRIUMPH trial ongoing. Compound under development by Eli Lilly.
TARGET PROFILE:
Obesity Medicine, Endocrinology, and Weight Loss.
| Weight | ,26 kg |
|---|
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