Tirzepatide 5mg

Tirzepatide is a 39-amino-acid synthetic peptide that functions as a dual agonist of both the glucose-dependent insulinotropic polypeptide (GIP) receptor and the glucagon-like peptide-1 (GLP-1) receptor. It is the first compound in its class — a "twincretin" — designed to simultaneously activate both incretin pathways. The molecule incorporates a C-20 fatty diacid moiety that binds serum albumin, conferring a half-life of approximately 5 days and enabling once-weekly administration. Tirzepatide shows approximately 5-fold selectivity for the GIP receptor over GLP-1 receptor, a pharmacological distinction that differentiates its metabolic profile from pure GLP-1 agonists like semaglutide.

The dual mechanism of tirzepatide produces metabolic effects that exceed what either receptor pathway achieves alone. GLP-1 receptor activation delivers the established benefits of appetite suppression, delayed gastric emptying, and glucose-dependent insulin secretion. The addition of GIP receptor agonism introduces complementary pathways: GIP signaling enhances adipose tissue lipid metabolism, improves insulin sensitivity in adipocytes, and may promote energy expenditure through effects on brown adipose tissue thermogenesis. The combined activation creates a synergistic metabolic environment in which caloric intake decreases while energy utilization improves. At the pancreatic level, dual receptor activation enhances beta-cell function more robustly than GLP-1 activation alone.

Research data for tirzepatide have been groundbreaking. Phase III trials demonstrated mean weight reductions of up to 22.5% over 72 weeks — significantly exceeding semaglutide's benchmark. A substantial proportion of participants achieved 25% or greater body weight reduction, approaching the efficacy previously seen only with bariatric surgery. Concurrent improvements in HbA1c, triglycerides, blood pressure, inflammatory markers, and hepatic fat content have been documented. The compound has also shown reductions in obstructive sleep apnea severity and improvement in physical function scores in participants with obesity-related functional limitations.

Tirzepatide is suited for researchers investigating advanced metabolic optimization, dual-pathway incretin biology, body composition remodeling, and next-generation weight management protocols. Researchers who have plateaued with single-agonist approaches may find the dual mechanism provides additional efficacy.

Reconstitute the 5mg vial with 1-2ml bacteriostatic water. Administer via once-weekly subcutaneous injection. Research protocols follow a dose-escalation approach: 2.5mg weekly for 4 weeks, increasing in 2.5mg increments every 4 weeks, with maximum research dosing at 15mg weekly. Escalation is critical for gastrointestinal tolerability. Store reconstituted solution at 2-8C and use within 28 days. Lyophilized powder should be stored refrigerated. The 5mg vial supports the initial weeks of dose escalation.