IMPORTANT: Read the Prep & Administration Guide for proper handling, reconstitution (if applicable), and administration technique. Mistakes here can compromise your research.
Retatrutide is an investigational incretin-based peptide engineered as a triple agonist of GLP-1, GIP, and glucagon receptors. It has been studied in clinical trials for obesity and metabolic disease, with reported effects on body weight, glycemic control, and cardiometabolic risk markers.
— 5 mg Vial —
Reconstitute: Add 1.0 mL bacteriostatic water → ~5.0 mg/mL concentration.
Typical weekly range: 2–8 mg once weekly (gradual escalation over 8–12 weeks).
Easy measuring: At 5.0 mg/mL, 1 unit = 0.01 mL ≈ 50 mcg on a U-100 insulin syringe.
Storage: Lyophilized: freeze at −20 °C; reconstituted: refrigerate at 2–8 °C for up to 4 weeks.
Schedule: Weekly subcutaneous injections for 12–48 weeks.
Cycle Length: Minimum 24 weeks; trials extended to 48 weeks.
Goal: Support significant weight reduction and metabolic improvements through triple-receptor activation.
Frequency: Inject once weekly subcutaneously. For doses >5 mg, reconstitute multiple vials. Volumes >1.0 mL may be split into 2 separate subcutaneous injections at different sites.
| Phase | Dose | Syringe (U-100) |
|---|---|---|
| Weeks 1–4 | 2 mg | 40 units (0.40 mL) |
| Weeks 5–8 | 4 mg | 80 units (0.80 mL) |
| Weeks 9–12 | 6 mg | 120 units (1.20 mL) |
| Weeks 13+ | 8 mg | 160 units (1.60 mL) |
— 10 mg Vial —
Reconstitute: Add 1.0 mL bacteriostatic water → ~10.0 mg/mL concentration.
Typical weekly range: 2–8 mg once weekly (gradual escalation over 8–12 weeks).
Easy measuring: At 10.0 mg/mL, 1 unit = 0.01 mL ≈ 100 mcg on a U-100 insulin syringe.
Storage: Lyophilized: freeze at −20 °C; reconstituted: refrigerate at 2–8 °C for up to 4 weeks.
Schedule: Weekly subcutaneous injections for 12–48 weeks.
Cycle Length: Minimum 24 weeks; trials extended to 48 weeks.
Goal: Support significant weight reduction and metabolic improvements through triple-receptor activation.
Frequency: Inject once weekly subcutaneously. All doses ≤10 mg can be drawn from one reconstituted 10 mg vial. Volumes >1.0 mL may be split into 2 separate subcutaneous injections at different sites.
| Phase | Dose | Syringe (U-100) |
|---|---|---|
| Weeks 1–4 | 2 mg | 20 units (0.20 mL) |
| Weeks 5–8 | 4 mg | 40 units (0.40 mL) |
| Weeks 9–12 | 6 mg | 60 units (0.60 mL) |
| Weeks 13+ | 8 mg | 80 units (0.80 mL) |
— 20 mg Vial —
Reconstitute: Add 2.0 mL bacteriostatic water → ~10.0 mg/mL concentration.
Typical weekly range: 2–8 mg once weekly (gradual escalation over 8–12 weeks).
Easy measuring: At 10.0 mg/mL, 1 unit = 0.01 mL ≈ 100 mcg on a U-100 insulin syringe.
Storage: Lyophilized: freeze at −20 °C; reconstituted: refrigerate at 2–8 °C for up to 4 weeks.
Schedule: Weekly subcutaneous injections for 12–48 weeks.
Cycle Length: Minimum 24 weeks; trials extended to 48 weeks.
Goal: Support significant weight reduction and metabolic improvements through triple-receptor activation.
Frequency: Inject once weekly subcutaneously. All doses ≤12 mg can be drawn from one reconstituted 20 mg vial. Volumes >1.0 mL may be split into 2 separate injections.
| Phase | Dose | Syringe (U-100) |
|---|---|---|
| Weeks 1–4 | 2 mg | 20 units (0.20 mL) |
| Weeks 5–8 | 4 mg | 40 units (0.40 mL) |
| Weeks 9–12 | 6 mg | 60 units (0.60 mL) |
| Weeks 13+ | 8 mg | 80 units (0.80 mL) |
— 30 mg Vial —
Reconstitute: Add 3.0 mL bacteriostatic water → ~10.0 mg/mL concentration.
Typical weekly range: 2–8 mg once weekly (gradual escalation over 8–12 weeks).
Easy measuring: At 10.0 mg/mL, 1 unit = 0.01 mL ≈ 100 mcg on a U-100 insulin syringe.
Storage: Lyophilized: freeze at −20 °C; reconstituted: refrigerate at 2–8 °C for up to 4 weeks.
Schedule: Weekly subcutaneous injections for 12–48 weeks.
Cycle Length: Minimum 24 weeks; trials extended to 48 weeks.
Goal: Support significant weight reduction and metabolic improvements through triple-receptor activation.
Frequency: Inject once weekly subcutaneously. All doses ≤12 mg can be drawn from one reconstituted 30 mg vial. Volumes >1.0 mL may be split into 2 separate injections.
| Phase | Dose | Syringe (U-100) |
|---|---|---|
| Weeks 1–4 | 2 mg | 20 units (0.20 mL) |
| Weeks 5–8 | 4 mg | 40 units (0.40 mL) |
| Weeks 9–12 | 6 mg | 60 units (0.60 mL) |
| Weeks 13+ | 8 mg | 80 units (0.80 mL) |
- Significant body-weight reduction reported in clinical trial settings (dose-dependent).
- Improved glycemic control markers (fasting glucose, HbA1c) in clinical research.
- Reductions in waist circumference and improvements in cardiometabolic risk markers in trials.
- Potential increases in energy expenditure via glucagon receptor agonism (mechanistic rationale).
Retatrutide activates GLP-1 and GIP receptors (enhancing glucose-dependent insulin secretion, slowing gastric emptying, and reducing appetite) while also activating the glucagon receptor, which can increase energy expenditure. The combined incretin + glucagon signaling is designed to drive greater weight loss than GLP-1-only agonism.
Potential adverse effects reported in literature and/or anecdotally include:
- Nausea, vomiting, diarrhea, constipation.
- Decreased appetite.
- GERD-like symptoms.
- Injection-site reactions.
- Possible gallbladder events with rapid weight loss (class-associated).
- Potential pancreatitis risk signals (class-associated; causality debated).
- Titrate slowly; most GI effects are dose-escalation related.
- Prioritize hydration and electrolytes if GI upset occurs.
- Smaller/lower-fat meals can reduce nausea.
- Pause escalation or reduce dose if persistent GI symptoms occur.
- Monitor for severe abdominal pain in clinical contexts.
- Personal/family history of medullary thyroid carcinoma or MEN2 (GLP-1 class boxed warning).
- History of pancreatitis (use caution).
- Severe gastroparesis or significant GI motility disorders.
- Pregnancy or breastfeeding.
PubMed-linked citations for verification. Many studies are preclinical (animal/in-vitro).
- Triple–hormone receptor agonist retatrutide for obesity: a randomized clinical trial. N Engl J Med. 2023. PMID: 37318111 (doi: 10.1056/NEJMoa2301972)
- Coagonism/triple agonism at GLP-1, GIP, and glucagon receptors for obesity: biology and pharmacology (review). Nat Rev Endocrinol. PubMed
- Glucagon receptor agonism and energy expenditure: mechanisms relevant to multi-agonist therapies. Endocr Rev. 2018. PubMed
Research Use Only. All information on this page is for educational purposes only and is not medical advice. PepSherpa does not sell peptides. Consult a licensed healthcare provider before making any health decisions. Many of the studies cited are preclinical (animal/in-vitro).
Research Use Only. All information on this page is for educational purposes only and is not medical advice. PepSherpa does not sell peptides. Consult a licensed healthcare provider before making any health decisions. Many of the studies cited are preclinical (animal/in-vitro).
