G3 - Research Grade 10mg

G3 - Research Grade 10mg

£60.00
£60.00
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G3 - Research Grade 10mg
  • G3 - Research Grade 10mg
  • G3 - Research Grade 10mg
G3 - Research Grade 10mg

G3 - Research Grade 10mg

£60.00
£60.00

For research purposes only. This product is supplied exclusively for scientific laboratory research and analytical purposes. It is not intended for human or animal use, and must not be misused in any way that contravenes MHRA regulations or applicable laws.

Ultra-Pure Research Grade Peptide – Minimum 98% Purity

Supplied in sterile, flip-top headspace vials designed for laboratory use

Manufactured to exacting standards and trusted by researchers worldwide

All of our peptides are supplied strictly for research and laboratory use only. Each vial contains sterile, lyophilised powder that has been finely milled and sieved to ensure consistency. The stated weight refers to the content of a single vial. Reconstitution requires Bacteriostatic Water containing 0.9% Benzyl Alcohol (or a suitable equivalent). Please note that we do not offer any advice or recommendations regarding dosage, administration, or use in humans or animals.

Retatrutide

  • What is Retatrutide?

    Retatrutide (LY3437943) is a novel triple hormone receptor agonist targeting GLP-1, GIP, and glucagon receptors. Phase III TRIUMPH-4 trial (Dec
    2025) achieved 28.7% weight loss (71.2 Ibs) at 68 weeks with 12mg dose - the highest recorded for any obesity medication. Currently in late-stage Phase III development by Eli Lilly with FDA approval expected 2026-2027.

  • Triple hormone receptor activation provides superior weight loss (24.2%), improved glycemic control, and enhanced cardiovascular benefits compared to single or dual agonists

  • Activates GLP-1 for appetite suppression, GIP for insulin sensitivity, and glucagon for increased energy expenditure and hepatic fat oxidation

  • Start 0.5mg weekly (clinical practice) or 1mg weekly (trial protocol), escalate every 4 weeks to target 8-12mg

  • Once weekly

  • Abdomen, thigh, upper arm - rotate weekly to prevent lipodystrophy

  • Any time of day, maintain same day each week for consistency

  • 24-48 hours: appetite suppression; 4-8 weeks: significant weight loss; 24+ weeks:
    maximum benefits

  • Lyophilized powder at room temperature; reconstituted solution refrigerated

  • Continuous therapy

  • Molecular Weight
    4,731.33 Da
    Chain Length
    39 amino acids
    Amino Acid Sequence
    His-Aib-Glu-Gly-Thr-Phe-Thr-Ser-Asp-Val-Ser-Ser-Tyr-Leu-Glu-Gly-Gln-Ala-Ala-Lys-Glu-Phe-
    Ile-Ala-Trp-Leu-Val-Arg-Gly-Arg-Gly-Pro-Ser-Ser-Gly-Ala-Pro-Pro-Pro-Ser

  • Administer on the same day each week for consistent hormone regulation. Can be taken with or without food due to subcutaneous administration.

  • Research starts very low and increases gradually over time. It begins with a conservative starting dose of 0.5 mg weekly for weeks 1 to 4, then rises to 1 mg weekly for weeks 4 to 8, 2 mg weekly for weeks 8 to 12, 4 mg weekly for weeks 12 to 16, and 8 mg weekly for weeks 16 to 20. 12 mg weekly from week 20 onward as the maximum-efficacy dose. For type 2 diabetes, it suggests a more cautious approach, starting at 0.5 to 1 mg weekly.

  • Weight Loss - Most Effective


    Superior Weight Reduction
    Clinical trials demonstrate 17.5% at 24 weeks and 24.2% at 48 weeks - highest recorded for any obesity medication in development
    Sustained Weight Management
    Continuous weight loss throughout trials with no plateau reached at 48 weeks, suggesting greater long-term potential than current therapies
    Triple Mechanism Obesity Treatment
    Addresses obesity through appetite suppression, increased energy expenditure, and improved metabolic efficiency via three hormone pathways

    Diabetes - Effective
    Superior Glycemic Control
    HbA1c reductions up to 2.16% with 82% of participants achieving target levels below 6.5% - exceeding dual agonist performance
    Glucose-Dependent Regulation
    Glucose-dependent insulin secretion and glucagon suppression provide balanced glycemic control with minimal hypoglycemia risk


    Insulin Sensitivity Enhancement
    Marked improvements in insulin sensitivity with potential for significant reduction in exogenous insulin requirements

  • * Week 1-2: Initial appetite suppression and mild Gl effects as body adapts to triple hormone activation
    * Week 2-4: Noticeable reduction in food cravings and portion sizes, early weight loss (2-5%)
    * Week 4-8: Significant appetite control and steady weight loss (5-10%), improved glucose control if diabetic
    * Week 8-16: Substantial weight reduction (10-18%) with enhanced energy expenditure and metabolic improvements
    * Week 16-24: Major weight loss milestone (15-22%) with cardiovascular benefits and liver fat reduction
    * Week 24-48: Maximum clinical efficacy (20-24.2%) with comprehensive metabolic improvements and sustained benefits

  • - Most common side effects are gastrointestinal (nausea 43%, diarrhea 33% at 12mg) - typically mild to moderate and dose-dependent
    - NEW SIGNAL (Dec 2025): Dysesthesia (abnormal touch sensations) reported in 8.8-20.9% of participants at 9-12mg doses in TRIUMPH-4 trial
    - Conservative start at 0.5mg weekly minimizes Gl side effects (13% vs 73-94% at higher doses) - escalate gradually every 4 weeks
    - Phase III discontinuation rates: 12.2% (9mg) and 18.2% (12mg) due to adverse events - correlated with baseline BMI
    - Monitor for signs of pancreatitis (severe abdominal pain radiating to back) - discontinue immediately if suspected
Heart rate increases are common, especially in first 24 weeks - monitor cardiovascular status regularly
Contraindicated in patients with personal/family history of medullary thyroid carcinoma or MEN2
syndrome
May cause rapid weight loss - some discontinuations due to perceived excessive weight loss

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