Tirzepatide Pen
$199.99 – $399.99Price range: $199.99 through $399.99
Buy your tirzepatide dual agonist weight loss pen online.
Tirzepatide Pen – Dual GIP/GLP-1 Receptor Agonist Delivery System for Advanced Metabolic Research
The Tirzepatide Pen is a convenient, research-grade pre-filled injection pen containing tirzepatide, a groundbreaking synthetic dual agonist that simultaneously targets glucose-dependent insulinotropic polypeptide (GIP) and glucagon-like peptide-1 (GLP-1) receptors. This 39-amino-acid peptide features a C20 fatty diacid acylation for extended half-life, enabling once-weekly subcutaneous administration with sustained receptor activation.
Engineered for precision in laboratory settings, the pen eliminates reconstitution steps, offering researchers an easy-to-use, accurate dosing system. Tirzepatide’s unique dual agonism provides synergistic effects that often surpass single-receptor incretin therapies, making it a powerful tool for investigating appetite regulation, glucose homeostasis, energy balance, lipid metabolism, and body composition in obesity, type 2 diabetes, and cardiometabolic models.
Key Research Applications & Observed Effects
Superior Weight Loss and Body Composition Improvements Tirzepatide drives substantial, dose-dependent weight reduction. In the SURMOUNT-1 trial (obesity without diabetes), doses of 5–15 mg produced mean weight loss of 15–22.5% over 72 weeks, with many participants achieving ≥15% or ≥20% reductions. SURMOUNT-2 (obesity with type 2 diabetes) showed up to 15.7% mean weight loss at 15 mg, while SURMOUNT-3 demonstrated additional profound loss following lifestyle intervention, reaching total reductions of ~26.6%. Reductions primarily target visceral and total fat mass while supporting relative lean mass preservation in multiple analyses.
Enhanced Glycemic Control and Insulin Dynamics The peptide promotes glucose-dependent insulin secretion, suppresses inappropriate glucagon release, slows gastric emptying, and improves insulin sensitivity. In the SURPASS program, tirzepatide reduced HbA1c by up to 2.0–2.6% across doses at 40–52 weeks, with high rates of participants reaching normoglycemia (A1C <5.7%). These effects make it ideal for diabetes mechanism studies, β-cell function research, and metabolic syndrome investigations.
Appetite Suppression and Satiety Enhancement Dual GIP/GLP-1 activation powerfully reduces food intake through central and peripheral signaling, increases satiety, and delays gastric emptying. This supports detailed exploration of eating behavior, reward pathways, and long-term energy intake regulation.
Cardiometabolic and Hepatic Benefits Research highlights improvements in lipid profiles (reduced triglycerides and LDL), blood pressure, inflammatory markers, and liver fat content. These outcomes position tirzepatide as a valuable agent for NAFLD/MASH, cardiovascular risk, and overall metabolic health models.
Product Highlights
- Ready-to-Use Pre-Filled Pen Format — Premixed solution in ergonomic single-dose or multi-dose research pens; simply dial, prime if needed, and inject subcutaneously—no mixing or syringes required.
- High-Purity Formulation — ≥98% purity (HPLC-verified), sterile, low-endotoxin, stability-optimized aqueous solution.
- Available Configurations — Research capacities supporting common titration strengths (2.5 mg, 5 mg, 7.5 mg, 10 mg, 12.5 mg, 15 mg per 0.5 mL equivalents), with adjustable micro-dosing options for precise protocols.
- Extended Pharmacokinetics — Once-weekly dosing maintains steady receptor engagement for chronic metabolic studies.
Recommended Dosage in Research Protocols
Standard research dosing begins with a low initiation dose to improve tolerability: 2.5 mg subcutaneously once weekly for the first 4 weeks. This starting dose minimizes gastrointestinal effects and is not intended for therapeutic endpoints.
After 4 weeks, increase to 5 mg once weekly. For additional effects in glucose control or weight-related endpoints, escalate in 2.5 mg increments after a minimum of 4 weeks on the current dose. The maximum recommended dose in research settings is 15 mg once weekly.
Administer at any time of day, with or without meals, via subcutaneous injection in the abdomen, thigh, or upper arm. Rotate injection sites. If a dose is missed, administer within 4 days if possible; otherwise, resume the regular schedule. Gradual titration is essential to optimize participant tolerance in experimental models.
Why Choose the Tirzepatide Peptide Pen for Metabolic Research
Tirzepatide’s dual-receptor mechanism delivers more comprehensive metabolic rewiring than single GLP-1 agonists, enabling deeper interrogation of incretin physiology, synergistic hormone signaling, and multi-organ effects on energy homeostasis. The pen format ensures workflow efficiency, dosing accuracy, and reproducibility—critical for dose-escalation, long-term, and head-to-head studies.
Common transient side effects include mild-to-moderate gastrointestinal events (nausea, diarrhea, vomiting, constipation) that typically diminish with time and proper titration. Heart rate increases and injection-site reactions may occur. As an investigational research compound in this context, comprehensive monitoring of safety parameters is recommended. Tirzepatide continues to generate excitement in phase 3 programs for its potential to address the complex interplay of obesity, diabetes, and cardiometabolic disease.
For laboratories advancing next-generation metabolic therapeutics, the Tirzepatide Peptide Pen provides a sophisticated, user-friendly platform to explore cutting-edge dual-agonist pharmacology and its profound impact on body weight, glycemic dynamics, and overall endocrine health.
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