Informational only. Not medical advice.INFORMATIONAL PLATFORM ONLY — NOT MEDICAL ADVICE, DIAGNOSIS, OR TREATMENT
Head-to-head comparison of GHRP-6 and Hexarelin — mechanism, side effects, legal status, and pricing.
GHRP-6 is a synthetic hexapeptide (His-D-Trp-Ala-Trp-D-Phe-Lys-NH2) growth hormone secretagogue and ghrelin receptor agonist. Developed by Bowers and Momany and first described in 1984, it was the first synthetic GHRP characterized and is defined by its pronounced appetite-stimulating effect — the strongest of any clinically studied GHRP. It has never been approved by the FDA or any regulatory agency and remains a research-only compound used off-label in the grey market.
Hexarelin (His-D-2MeTrp-Ala-Trp-D-Phe-Lys-NH2) is a synthetic hexapeptide growth hormone secretagogue developed by Mediolanum (Italy) in the 1990s. It is a potent ghrelin-receptor (GHSR-1a) agonist that also binds the CD36 scavenger receptor, giving it a cardioprotective signal distinct from other GHRPs. It is not FDA-approved for any indication and remains a research-only compound; its clinical development for GH deficiency and cardiac indications did not reach approval. A defining feature versus other GHRPs is rapid, pronounced tachyphylaxis with chronic daily dosing.
GHRP-6
Hexarelin
Category
Legal Status
Mechanism
Half-life
COA-verified vendors · trust score ≥70 required · single-vial price — bulk/bundle deals may be lower
GHRP-6
Hexarelin
COA corpus from Disclosed Labs — independently tested batches only.
GHRP-6
13
COAs
99.4%
Avg purity
4
Labs
Hexarelin
10
COAs
99.4%
Avg purity
4
Labs
GHRP-6 is among peptides under FDA review for the Category 1 (503A) list; if added, it would require a prescription to be compounded by registered 503A/503B pharmacies — not yet authorized. Hexarelin remains research-only. In April 2026 the FDA removed 12 peptides from Category 2, which does not place them on the Category 1 list or authorize compounding. The FDA's Pharmacy Compounding Advisory Committee is advisory and meets July 23–24, 2026 to review nominations and make recommendations to the FDA.
GHRP-6 was first characterized by Bowers, Momany, Reynolds, and Hong in Endocrinology (1984, PMID 6714155), establishing it as the first synthetic peptide to specifically release GH via a non-GHRH mechanism — a key tool in the later discovery of the ghrelin receptor. Ghigo et al. (European Journal of Endocrinology, 1997, PMID 9186261) reviewed the GHRP class and confirmed GH, ACTH/cortisol, and prolactin co-stimulation in humans. Berlanga et al. (Clinical Science, 2007, PMID 16989643) demonstrated ~78% infarct-mass reduction in a porcine myocardial infarction model via antioxidant mechanisms, and Berlanga-Acosta et al. (Clinical Medicine Insights: Cardiology, 2017, PMID 28469491) reviewed the cytoprotective GHRP literature across cardiac, neuronal, and hepatic tissues. GHRP-6 has never been approved for any clinical indication; its intense appetite stimulation and cortisol/prolactin co-release limit its clinical utility compared with ipamorelin.
Key references
Ghigo et al. (1994, PMID 8126144, JCEM) characterized hexarelin's GH-releasing activity across IV, SubQ, intranasal, and oral routes in healthy men, establishing it as a potent GH secretagogue. Rahim & Shalet (1998, PMID 10990150, Growth Horm IGF Res) demonstrated that twice-daily SubQ hexarelin in healthy elderly subjects caused ~45% attenuation of the GH AUC over 16 weeks, with partial recovery 4 weeks after discontinuation — the canonical human tachyphylaxis study. Bodart et al. (2002, PMID 11988484, Circulation Research) showed that hexarelin's cardiovascular action in perfused hearts is mediated by CD36 rather than GHSR-1a and is absent in CD36-null animals. Hexarelin has never been FDA-approved; grey-market use for body composition, recovery, or cardiac benefit is not clinically validated.
GHRP-6 (Performance) and Hexarelin (Hormone) are in different categories and target different biological pathways. This is a common pattern in multi-compound research protocols. Researchers should monitor the biomarkers from both profiles and watch for interactions listed in each compound’s contraindications. Consult a licensed healthcare provider before combining any research compounds.
This platform provides informational tools only, not medical advice. This comparison is for educational purposes only. Consult a licensed provider.
Side Effects
Contraindications
Lab Testing
Key references