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GROWTH HORMONE RELEASING PEPTIDE

Tesamorelin

A 44-amino GHRH analog that stimulates pituitary GH secretion, studied for visceral adipose tissue reduction in clinical research.

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Key Statistics

Statistic Value Detail
Visceral Fat Reduction 18.2% Abdominal fat loss at 26 weeks
IGF-1 Increase 117% Growth factor elevation
Liver Fat Reduction 37% NAFLD improvement at 12 months
NAFLD Resolution 35% Complete fatty liver reversal
Executive Function P=0.005 Significant cognitive improvement

Mechanism of Action

GHRH Receptor-Mediated GH Release

Tesamorelin binds to GHRH receptors on pituitary somatotrophs, stimulating pulsatile GH release that maintains physiological feedback mechanisms and circadian rhythms. It promotes selective lipolysis in visceral adipose tissue while preserving subcutaneous fat and muscle mass.

Biological Pathways

GHRH Receptor Activation (Primary)

Growth Hormone Releasing Hormone

  • Binds pituitary somatotrophs
  • Stimulates pulsatile GH release
  • Maintains physiological feedback

IGF-1 Mediated Lipolysis (Mediator)

Insulin-like Growth Factor 1

  • Stimulates hepatic IGF-1 production
  • Promotes selective visceral lipolysis
  • Preserves muscle mass

Metabolic Modulation (Supportive)

Metabolic Flexibility Enhancement

  • Reduces ectopic fat deposition
  • Improves insulin sensitivity
  • Enhances metabolic flexibility

Key Mechanism

Pulsatile GH Stimulation

Tesamorelin preserves natural GH pulsatility unlike exogenous growth hormone. It stimulates the body’s own GH production, maintaining circadian rhythms and feedback mechanisms for a physiologically superior approach.

Metric Value
VAT Reduction (26wk) 15.4%
VAT Reduction (52wk) 17.5%
Placebo Change -5%
Participants Achieving >8% VAT Reduction 73%

Clinical Findings

Metric Value Context
Visceral Fat Reduction 18.2% Phase 3, 816 patients, 26 weeks
IGF-1 Increase 117% Mean elevation from baseline
Liver Fat Reduction 37% MRI-PDFF measurement

FDA-approved for HIV-associated lipodystrophy. Results from two Phase 3 trials (LIPO-010 & CTR-1011) with 816 HIV-infected patients.

Preclinical Effects

Effect Model Value
Treatment Well Tolerated Phase 3 trials 91.2%
Effects Maintained Continued use 52 weeks
Triglyceride Reduction VAT responders 20-50 mg/dL
Trunk Muscle Density Body composition +4.86 HU

Research Areas

Visceral Fat Reduction — Primary FDA-approved indication

18.2% average VAT reduction at 26 weeks in HIV lipodystrophy patients

Liver Health — NAFLD/NASH treatment potential

37% hepatic fat reduction, 35% NAFLD resolution. Only FDA-approved agent for HIV-associated NAFLD

Cognitive Function — Executive function improvement

Significant improvements in executive function (P=0.005) and response inhibition in older adults

Body Composition — Muscle quality enhancement

Improvements in muscle density and lean mass area without loss of lean tissue

Dosing Protocols

Standard FDA Protocol

Dose: 2mg daily subcutaneous | Frequency: Once daily | Duration: Continuous (effects reverse on discontinuation)

  • Inject in abdomen, rotate sites
  • Same time each day recommended
  • Effects reverse if discontinued

Cognitive Support Protocol

Dose: 1mg daily | Frequency: 30 min before bedtime | Duration: 20+ weeks, then assess response

  • Lower dose than standard lipodystrophy protocol
  • Bedtime administration studied
  • Based on MCI/aging study

Pharmacokinetics

Parameter Value
Half-Life 26-38 minutes
Peak Concentration 0.15 hours (9 minutes)
Bioavailability <4% (typical for peptides)
Stability Requires reconstitution
Excretion Renal (peptide fragments)
Metabolism Peptide hydrolysis

Safety Profile

Issue Incidence Severity
Injection site reactions 13.3% mild
Arthralgia 7.5% mild
Peripheral edema 5.7% mild
  • Generally well-tolerated with predictable GH-related side effects
  • Anti-tesamorlin antibodies detected but no impact on efficacy
  • Well-tolerated long-term (52+ weeks)

Compound Information

Property Value
Type Synthetic GHRH analog
CAS Number 218949-48-5
Molecular Weight 5,135.9 g/mol
Amino Acids 44
Sequence Modified GHRH(1-44)
Formula C221H366N72O67S1

Frequently Asked Questions

Q: How long does it take to see results?

A: IGF-1 levels increase within 2-4 weeks. Visible reduction in abdominal fat typically begins around 8-12 weeks, with maximal effects at 26 weeks. Clinical trials show 15-18% visceral fat reduction at 6 months.

Q: What happens if I stop taking Tesamorelin?

A: Effects are not sustained after discontinuation. Clinical studies show visceral fat returns to near baseline levels within 26 weeks of stopping treatment.

Q: Is Tesamorelin the same as HGH?

A: No. Tesamorelin stimulates your body’s own growth hormone production while preserving natural pulsatility and feedback mechanisms, which is physiologically superior to exogenous HGH.

Q: Can Tesamorelin improve cognitive function?

A: Research shows promising cognitive benefits. A controlled trial demonstrated significant improvements in executive function (P=0.005) in both healthy older adults and those with mild cognitive impairment, using 1mg daily.

References

  1. Falutz J, et al. (2010) “Effects of tesamorelin in HIV-infected patients with abdominal fat accumulation” Journal of Clinical Endocrinology & Metabolism PMID: 20554713
  2. Stanley TL, et al. (2019) “Effects of tesamorelin on non-alcoholic fatty liver disease in HIV” Lancet HIV PMID: 31611038
  3. Baker LD, et al. (2012) “Effects of GHRH on cognitive function in adults with MCI and healthy older adults” Archives of Neurology PMID: 22869065
  4. Adrian S, et al. (2019) “Tesamorelin Decreases Muscle Fat and Increases Muscle Area in Adults with HIV” Journal of Clinical Endocrinology and Metabolism PMID: 31050749
  5. Fourman LT, et al. (2020) “Effects of tesamorelin on hepatic transcriptomic signatures in HIV-associated NAFLD” JCI Insight PMID: 32780726
  6. Theratechnologies Inc. (2025) “Tesamorelin Prescribing Information” EGRIFTA Prescribing Information
FOR RESEARCH USE ONLY. Not for human consumption. All compounds are sold strictly for in vitro research and laboratory use. © Forto Labs

FOR RESEARCH USE ONLY. Not for human consumption. All compounds are sold strictly for in vitro research and laboratory use. The information on this page is compiled from published peer-reviewed studies and is provided for educational purposes only. It does not constitute medical advice. © 2026 Forto Labs