Retatrutide is the third generation in the incretin-class metabolic peptide research field. Where Semaglutide was a single GLP-1 receptor agonist and Tirzepatide added a second receptor (GIP), Retatrutide engages a third — the glucagon receptor. The published phase-2 trial literature (Jastreboff et al., 2023) reported the largest body-weight changes seen in this peptide class, attributable in part to glucagon-axis activation of hepatic energy expenditure pathways.
This guide is a complete research-frame deep-dive on Retatrutide as a laboratory research compound: the molecular structure, the triple-receptor mechanism documented in published literature, half-life and pharmacokinetics, the phase-2 trial program, storage and handling, and practical research-supply notes. Everything is research-frame language. No protocol guidance. No clinical recommendations.
Research use only
Retatrutide is supplied as lyophilized powder for laboratory research only. It is not approved as a medicine in any jurisdiction, and the laboratory research-grade material here is not therapeutic. This article documents what published peer-reviewed research has investigated — it is not a protocol, dosing guide, or therapeutic recommendation.
Quick reference — Retatrutide identifiers
| Property | Retatrutide |
|---|---|
| CAS number | 2381089-83-2 |
| Synonyms / development codes | LY3437943, GGG-tri-agonist |
| Receptor targets | GIP-R + GLP-1R + GCG-R (triple agonist) |
| Molecular formula | C221H343N51O59 |
| Molecular weight | 4731.41 g/mol |
| Sequence length | 39 amino acids (modified) |
| Backbone modification | Aib substitutions for DPP-4 resistance, C20 fatty-acid side chain via γ-Glu spacer for albumin binding |
| Half-life (research models) | ~108–144 hours |
| Vial strengths (TogoPeptide) | 5 / 10 / 20 / 30 mg lyophilized |
Structure — engineered for triple-receptor balance
Retatrutide is a 39-amino-acid synthetic peptide engineered to balance affinity across three structurally similar but functionally distinct G-protein-coupled receptors: GIP-R, GLP-1R, and the glucagon receptor (GCG-R). Designing a peptide that engages all three with appropriate relative potency is non-trivial — full agonism at glucagon receptor would normally drive blood-glucose elevation, counter to the GLP-1/GIP effects.
- Triple-balanced receptor binding: published binding-affinity studies report Retatrutide engages all three receptors with measured potency, with relative receptor activity calibrated so the GIP/GLP-1 incretin effects dominate the net metabolic response while glucagon-axis activity drives hepatic energy expenditure without net glucose elevation [1].
- Aib substitutions protect against DPP-4 enzymatic cleavage, extending plasma half-life.
- C20 fatty-acid side chain via γ-glutamic acid spacer enables reversible albumin binding for slow renal clearance and once-weekly research dosing kinetics.
Mechanism — triple GIP/GLP-1/glucagon receptor agonism
Retatrutide engages three receptor systems simultaneously, each contributing a different metabolic effect in published research-model literature:
- GLP-1 receptor activation drives the canonical incretin response — glucose-dependent insulin secretion, slowed gastric emptying, central satiety signaling. This is the foundational pathway shared with Semaglutide and Tirzepatide.
- GIP receptor activation adds adipose-tissue and lipid-handling effects layered on top of GLP-1 incretin signaling. Shared with Tirzepatide.
- Glucagon receptor activation is the distinguishing Retatrutide mechanism. Glucagon receptor signaling drives hepatic energy expenditure in research-model literature — increased lipolysis, hepatic ketogenesis, and metabolic-rate effects that GIP/GLP-1 alone do not produce [2].
Why glucagon agonism does not raise blood glucose
In isolation, glucagon receptor activation would elevate blood glucose. In Retatrutide research, the glucagon-axis activity is layered on top of strong simultaneous GLP-1 and GIP receptor activation — which together drive insulin secretion and glucose utilization more powerfully than glucagon alone could elevate it. The net effect in published phase-2 outcomes is glucose-neutral or glucose-lowering, while the glucagon-axis contribution adds the energy-expenditure component to the body-composition outcomes.
Half-life and pharmacokinetics
Retatrutide’s plasma half-life in published research models is approximately 108–144 hours (4.5–6 days), depending on dose and model. The albumin-binding fatty-acid side chain is the primary contributor — as with Tirzepatide and Semaglutide, this enables once-weekly research-design dosing.
Steady-state plasma concentration in once-weekly research-design protocols is reached after roughly 4–5 weeks (4 half-lives). Exposure is dose-dependent and approximately linear across the dose range studied in published phase-2 trial literature.
Phase-2 trial literature — body-composition research
The defining Retatrutide research publication is Jastreboff et al., 2023 in NEJM — a phase-2 trial in adults with obesity but without T2D. The headline body-weight outcomes documented in that publication exceeded all prior incretin-class research-trial reports:
- Highest dose group: mean body-weight reduction of ~24% at 48 weeks in the published primary outcome.
- Mid-dose groups: dose-dependent body-weight changes between approximately 8% and 17% at 48 weeks.
- Mechanism-attribution analysis: the published outcomes were larger than what Tirzepatide phase-2 / phase-3 trials produced at comparable durations, supporting the mechanistic hypothesis that the glucagon-axis component contributes additional body-weight effect via energy expenditure.
A separate phase-2 trial in T2D research populations (Rosenstock et al., 2023) documented HbA1c outcomes alongside body-composition outcomes [3]. Long-term outcome research and phase-3 cardiovascular-safety research is ongoing as of the most recent publication window.
Hepatic energy expenditure — what the glucagon axis adds
The mechanistic-research interest in Retatrutide centers on the glucagon-axis contribution. Published preclinical literature on triple-agonist molecules in obese mouse models documented:
- Increased hepatic energy expenditure — measurable via indirect calorimetry in research-animal models
- Increased hepatic lipid oxidation — reduced hepatic fat content beyond what GIP/GLP-1 dual agonism produces
- Adipose-tissue-specific effects on lipolysis and brown-adipose-tissue thermogenesis in some research models
The published mouse-model outcomes preceded and predicted the larger body-weight changes seen in Retatrutide phase-2 human trials.
Storage and handling — research-grade methodology
Retatrutide ships as lyophilized powder. Standard research-handling literature for albumin-binding incretin-class peptides documents:
- Lyophilized state: sealed at −20°C, protected from light. Stable for the manufacturer-stated window — typically 24+ months under proper storage.
- Diluent: bacteriostatic water (0.9% benzyl alcohol) is the standard reconstitution diluent. The benzyl alcohol enables multi-puncture access across approximately 28 days under refrigeration.
- Reconstituted state: refrigerate at 2–8°C immediately after reconstitution. Use within ~4 weeks.
- Avoid freeze-thaw cycles after reconstitution — albumin-binding peptides are sensitive to repeated phase changes.
- Vial inspection — clear, faintly straw-tinted solution after reconstitution. Cloudiness or particulates indicate aggregation; discard and re-reconstitute fresh.
Each TogoPeptide Retatrutide shipment includes a per-batch Certificate of Analysis with HPLC purity (target ≥98%), mass-spectrometry identity confirmation, lot number, manufacture date, analysis date. See how to read a COA for what each section means, or reconstitution methodology for the diluent volume math.
Reconstitution math — quick examples
Using the formula Volume in mL = Vial mass in mg / Target concentration in mg/mL:
- 5 mg vial → 5 mg/mL: 5 / 5 = 1 mL bacteriostatic water
- 10 mg vial → 5 mg/mL: 10 / 5 = 2 mL bacteriostatic water
- 10 mg vial → 10 mg/mL: 10 / 10 = 1 mL bacteriostatic water
- 20 mg vial → 10 mg/mL: 20 / 10 = 2 mL bacteriostatic water
- 30 mg vial → 15 mg/mL: 30 / 15 = 2 mL bacteriostatic water
For target concentrations or vial sizes not in this table, use the reconstitution calculator.
Practical research-supply considerations
- Newest in the class: Retatrutide phase-3 cardiovascular and long-term outcome research is still emerging. Published research designs that cite Retatrutide should reference the most recent peer-reviewed publication window.
- Dose-range research: the published phase-2 dose-response curve is steep. Multi-arm research designs benefit from dose-range coverage to detect mechanism-attribution.
- Cross-class research framing: Retatrutide outcomes are typically benchmarked against Tirzepatide and Semaglutide. The GLP-1 agonists compared article documents side-by-side identifiers across all three.
- Curated stack option: the Fat-Loss Stack bundles Retatrutide alongside Tirzepatide and Semaglutide for cross-generation research-supply orders.
Closing
Retatrutide represents the third generation of incretin-class metabolic research peptides — the first to engage three receptor systems simultaneously. Its triple GIP/GLP-1/glucagon mechanism produced the largest body-weight changes seen in this peptide class in published phase-2 trial literature, attributable in part to glucagon-axis activation of hepatic energy expenditure pathways.
This guide documents what published peer-reviewed research has investigated. It is structural and mechanism context for laboratory researchers, not therapeutic recommendation, not protocol guidance, not a basis for self-administration of any kind.
Source Retatrutide for laboratory research:
- Retatrutide product page — full identifiers, four vial strengths, per-batch COA
- Fat-loss research compounds — full category listing
- Fat-Loss Stack — Retatrutide + Tirzepatide + Semaglutide curated research-supply bundle
For methodology and laboratory-handling questions, contact our research-supply team at info@togopeptide.com.
References
- Knerr PJ, Mowery SA, Douros JD, et al. Next generation GLP-1/GIP/glucagon triple agonists normalize body weight in obese mice. Mol Metab. 2022. PubMedPMID: 34952210
- Jastreboff AM, Kaplan LM, Frías JP, et al. Triple-hormone-receptor agonist retatrutide for obesity — a phase 2 trial. N Engl J Med. 2023. PubMedPMID: 37344875
- Rosenstock J, Frias J, Jastreboff AM, et al. Retatrutide, a GIP, GLP-1 and glucagon receptor agonist, for people with type 2 diabetes — a phase 2 trial. Lancet. 2023. PubMedPMID: 37356870
- Day JW, Ottaway N, Patterson JT, et al. A new glucagon and GLP-1 co-agonist eliminates obesity in rodents. Nat Chem Biol. 2009. PubMedPMID: 19767731
- Finan B, Yang B, Ottaway N, et al. A rationally designed monomeric peptide triagonist corrects obesity and diabetes in rodents. Nat Med. 2015. PubMedPMID: 25569618
- Coskun T, Urva S, Roell WC, et al. LY3437943, a novel triple glucagon, GIP, and GLP-1 receptor agonist for glycemic control and weight loss: from discovery to clinical proof of concept. Cell Metab. 2022. PubMedPMID: 35921817