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Research Peptides for Weight Loss: GLP-1, GIP, and Triple Agonists

THEGLP-1 peptides(Glucagon-Like Peptide-1) represents the most studied class of research molecules in the field of obesity and energy metabolism. Large-scale clinical trials have demonstrated reductions in body mass ranging from-15% to -24.2%depending on the target and generation of the peptide. This page presents the main families — mono, dual and triple agonists — their mechanisms of action, the available scientific results, and the products offered by MyPeptide for research.

GLP-1 peptide families under investigation

1. GLP-1 monoagonists — Semaglutide

Le Semaglutideis a human GLP-1 analog with a prolonged half-life (≈7 days due to a C-18 modification). It exclusively targets the GLP-1 receptor (GLP-1R), stimulating glucose-dependent insulin secretion and suppressing glucagon secretion. In the STEP 1 trial (N=1961), Semaglutide 2.4 mg/week induced abody weight reduction of −15.3%over 68 weeks vs −2.6% placebo. It constitutes the first-generation reference for obesity studies.

2. Dual GLP-1/GIP agonists — Tirzepatide

Le Tirzepatideis a unimolar co-agonist peptide that simultaneously targets GLP-1R and GIPR (Glucose-dependent Insulinotropic Polypeptide receptor). GIP/GLP-1 co-activation produces a synergistic effect on insulin secretion, appetite suppression, and adipocyte lipolysis. In the SURMOUNT-1 trial, Tirzepatide 15 mg/week achieved-22.5% of body weightat 72 weeks, significantly outperforming Semaglutide in indirect comparison.

3. GLP-1/GIP/Glucagon Triple Agonists — Retatrutide

Le Retatrutiderepresents the third generation: a triple agonist targeting GLP-1R, GIPR, and the glucagon receptor (GCGR). The addition of glucagon agonism amplifies hepatic thermogenesis and basal energy expenditure, in addition to the GLP-1/GIP effects. In the phase 2 published in theNew England Journal of Medicine(2023), Retatrutide 12 mg produced a reduction in-24.2% of body weightat 48 weeks, setting a new clinical record in this class.

Mechanisms of action of GLP-1 peptides

Central satiety (hypothalamic pathway)

GLP-1R receptors are highly expressed in the arcuate nucleus and paraventricular nucleus of the hypothalamus. GLP-1R stimulation activates POMC/CART neurons (anorexigenic) and inhibits AgRP/NPY neurons (orexigenic), reducing total caloric intake by 20–35% in preclinical models.

Delayed gastric emptying

Via the vagus nerve and enteric plexuses, GLP-1 delays gastric emptying, prolonging the feeling of postprandial satiety. This effect is measured by gastric scintigraphy: Semaglutide delays emptying by approximately 35% compared to placebo, reducing postprandial blood glucose spikes.

Thermogenesis and energy expenditure (Glucagon effect)

Specific to the triple agonist Retatrutide, GCGR agonism stimulates hepatic thermogenesis (β-oxidation of fatty acids), increases basal energy expenditure via the activation of beige/brown adipocytes, and promotes hepatic ketogenesis. This additional effect explains the 24.2% superiority observed with Retatrutide versus 22.5% for Tirzepatide.

Adipolysis and remodeling of adipose tissue

The GLP-1/GIP combination activates lipolysis in visceral white adipocytes (preferential reduction of visceral fat), improves insulin sensitivity in peripheral tissues, and reduces inflammatory adipokine markers (IL-6, TNF-α, leptin) documented in adipose tissue biopsies.

Scientific comparison

Molecule Targets Weight reduction Clinical phase Key study
Semaglutide GLP-1R -15.3% FDA/EMA Approved STEP 1 (NEJM 2021)
Tirzepatide GLP-1R / GIPR -22.5% FDA/EMA Approved SURMOUNT-1 (NEJM 2022)
Retatrutide GLP-1R / GIPR / GCGR -24.2% Phase 3 is underway Phase 2 (NEJM 2023)

Data from published clinical trials. Percentages represent the average reduction in body weight at the maximum dose studied versus baseline.

Retatrutide products available for research

MyPeptide offers theRetatrutide R3with a purity ≥99% certified by HPLC (Janoshik), exclusively for scientific research in vitro or on animal models.

FAQ — GLP-1 Peptides for Weight Loss

Which GLP-1 peptides are used in obesity research?

The main GLP-1 peptides studied are theSemaglutide(mono-agonist, −15% weight), theTirzepatide(dual GLP-1/GIP, −22%) and theRetatrutide(triple GLP-1/GIP/Glucagon, −24.2% in phase 2). Retatrutide is currently the most effective as measured in clinical studies.

What is the difference between a mono, dual and triple GLP-1 agonist?

Un mono-agonistTargets only GLP-1 (e.g., Semaglutide). Onedual agonistGLP-1 and GIP targets (e.g., Tirzepatide). Onetriple agonisttargets GLP-1, GIP and Glucagon simultaneously (ex: Retatrutide), allowing a combined action on satiety, metabolism and thermogenesis for superior efficacy.

How do GLP-1 peptides work for weight loss?

GLP-1 peptides act through several mechanisms: reduction of appetite via hypothalamic centers, slowing of gastric emptying (prolonged feeling of satiety), improvement of insulin sensitivity, and for the triple agonist, activation of thermogenesis via the glucagon receptor.

Are these peptides available for human consumption?

MyPeptide offers these peptidesexclusively for scientific research purposesSemaglutide and Tirzepatide are approved as medications (Ozempic®, Mounjaro®). Retatrutide R3, offered by MyPeptide, is intended for in vitro or animal research only, in accordance with current regulations.

What is the purity of MyPeptide's GLP-1 peptides?

All MyPeptide peptides have apurity ≥99%certified by HPLC analysis (Janoshik). Each batch is accompanied by a Certificate of Analysis (COA) which can be downloaded directly from the product page.

Legal notice:The peptides presented on this page are offered exclusively for scientific research purposes. They are not intended for human, veterinary, or food use. MyPeptide does not provide medical advice. This information is derived from peer-reviewed scientific publications and does not constitute a therapeutic claim. The use of these molecules is subject to applicable local regulations.
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