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7. Ανθρώπινες Σχέσεις - ώρα: 10.30 – 12.00

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Συντονίστριες: Κατερίνα Δημητρίου & Ευγενία Ζήση

Βιβλίο: Θα σε καταλάβω αν με καταλάβεις, Έρικ Μπλούμενταλ (εκδ. Φιλίστωρ)


8. Ανθρώπινες σχέσεις - ώρα: 18.00 – 19.30

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Βιβλίο: Υπάρχω, αλλάζζω - Πέγκυ Πελώνη

Last modified on Tuesday, 23 Σεπτεμβρίου 2025 14:07
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    Peptide Sciences Tirzepatide vs Semaglutide vs Retatrutide – A Research Comparison
    The incretin peptide science tirzepatide family has
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    from selective GLP-1 agonism to dual and triple receptor activation. This
    evolution mirrors the broader trend in precision medicine, where multi-targeted approaches
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    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
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    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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