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The incretin peptide science tirzepatide family has expanded dramatically over the past decade.
Researchers now have access to multiple receptor-targeting
strategies, from selective GLP-1 agonism to dual and triple receptor activation. This evolution mirrors the broader trend
in precision medicine, where multi-targeted approaches are increasingly investigated for complex metabolic conditions.
Semaglutide, tirzepatide, and retatrutide represent
three distinct generations of research peptides targeting metabolic
pathways. Understanding their differences –
receptor profiles, half-lives, signaling biases, and research applications –
is essential for designing rigorous preclinical studies.
This comprehensive comparison guide examines all three peptides available from Peptide Sciences™ , helping researchers
select the right tool for their specific experimental questions.
For additional context, commercial information on GLP-1-based therapies can be found at NovoWegovy , and other
research suppliers like Paramount Peptides also
offer similar compounds. However, as emphasized in our guide on where to buy research peptides , always
verify quality standards regardless of supplier.
Three Peptides, Three Mechanisms
At a Glance Comparison Table
Feature Semaglutide Tirzepatide Retatrutide
Receptor targets GLP-1 only GLP-1 + GIP GLP-1 + GIP + glucagon
Number of agonists Single Dual (two) Triple (three)
Half-life (animal models) ~7 days ~5 days ~6 days
Molecular weight (Da) 4,113.6 4,813.4 ~4,900
Amino acid length 31 39 ~40
Peptide Sciences™ purity ≥99% ≥98.5% ≥98%
Primary research use Selective GLP-1 studies Dual pathway mapping Triple-receptor signaling
Fatty acid modification C18 at Lys26 C20 at Lys20 C18/C20 hybrid
DPP-4 resistance Yes (Aib substitutions) Yes (Aib substitutions) Yes (Aib substitutions)
SKU PS-SEMA-5mg PS-TIRZ-10mg PS-RETA-10mg
The Incretin System: Background for Researchers
Before diving into each peptide, a brief overview of the incretin system is helpful.
Incretins are gut-derived hormones that potentiate insulin secretion in response to meals.
The two primary incretins are:
Hormone Receptor Primary Effects Secreted By
GLP-1 (Glucagon-Like Peptide-1) GLP-1R Insulin secretion, satiety, gastric emptying L-cells
(ileum, colon)
GIP (Glucose-dependent Insulinotropic Polypeptide) GIP-R Insulin secretion, fat
metabolism,
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