Compound Reference

Tesamorelin

DPP-IV Stabilized GHRH Analogue

Tesamorelin molecular structure
Molecular structure — illustrative reference.

Class

DPP-IV Stabilized GHRH Analogue

Molecular Weight

5,135.8 Da

Half-life

26–38 minutes

Purity

≥98% (HPLC)

Form

Lyophilized powder

Storage

Lyophilized: 2–8°C; Reconstituted: 2–8°C

Reconstitution

Sterile water for injection

Mechanism of action

Tesamorelin is a synthetic GHRH analogue with a trans-3-hexenoic acid modification at the N-terminus, which enhances stability against dipeptidyl peptidase IV (DPP-IV) degradation while preserving GHRH receptor binding. It stimulates endogenous GH secretion with preserved physiological pulsatility — a key distinction from exogenous GH administration, which suppresses the HPG axis feedback.

⚠️ For Research Use Only — described exclusively for in vitro and laboratory research by qualified researchers. Not for human or veterinary use. Informational only; does not constitute medical advice or imply efficacy in humans.

Research highlights

~15%

Visceral adipose tissue reduction (HIV-lipodystrophy trial)

FDA

Egrifta — approved for HIV-associated lipodystrophy

Pulsatile

Preserves physiological GH pulse pattern

Cognitive

Emerging data on GH axis and memory in older adults

Research notes

  • FDA approval: Tesamorelin (Egrifta) approved for HIV-associated lipodystrophy — significant visceral fat reduction in controlled trials.
  • VAT: ~15–18% reduction in visceral fat observed over 26 weeks in clinical research.
  • Cognitive: Emerging research on GHRH/GH axis and working memory function in older adults.
  • Lipid effects: Improvements in triglycerides and trunk fat distribution observed in multiple studies.
  • HPG preservation: Does not suppress the hypothalamic-pituitary-GH axis feedback, unlike exogenous GH.

For Qualified Researchers

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