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Hexarelin

Examorelin, HEX

Quick Stats
Studies 233
Trials 61
Score 3
1997 pubmed

Effect of long-term administration of Hexarelin on the somatotrophic axis in aged rats.

Cattaneo. L L; Luoni. M M; Settembrini. B B; Müller. E E EE; Cocchi. D D

Key Findings

  • Chronic hexarelin (80 µg/kg s.c.) maintains GH release in aged rats for 30‑60 days
  • A single hexarelin dose after chronic treatment triggers a larger GH surge than in untreated rats
  • Somatostatin mRNA in the hypothalamus of old rats drops to youthful levels with hexarelin, but circulating IGF‑1 stays unchanged

Practical Outcomes

  • Hexarelin may help older individuals boost their GH response, but human data are missing, so any self‑experiment should start with very low doses and monitor GH/IGF‑1 levels. The rat dose translates to roughly 0.08 mg/kg daily, which is far higher than typical human research doses, so dose‑scaling and safety need careful consideration. Expect possible GH spikes without guaranteed IGF‑1 increases, and watch for side‑effects.

Summary

In older rats, giving the peptide hexarelin every day for up to two months kept the growth‑hormone (GH) system working better, leading to bigger GH spikes after a single dose, and it lowered a brain hormone (somatostatin) that normally blocks GH. However, it didn’t raise the downstream hormone IGF‑1, and the study was done in rats, not people.

Abstract

The growth hormone-releasing peptide Hexarelin (Hexa; 80 micrograms/kg-1, s.c.) was administered for 30 and 60 days to old rats. The GH-releasing effect of Hexa was maintained during chronic treatment. At the end of the treatment, old rats were administered once with Hexa which elicited a greater GH response in rats chronically treated with the peptide than in those receiving a placebo. Pituitary GHmRNA concentrations were significantly lower in the older rats than in the younger animals, irrespective of Hexa treatment, while the GH protein content was similar in all the groups studied. The same was true for hypothalamic GHRH, whose synthesis was reduced in all the older animals but not in the young, in the presence of maintained concentrations of the peptide. Somatostatin mRNA concentrations were significantly higher in the hypothalami of older rats and administration of Hexa for 30 or 60 days brought the concentrations of somatostatin mRNA of aged rats to 'young' levels. Treatments with Hexa failed to alter the circulating levels of IGF-1. The data reported in this article indicate that long-term treatment with Hexa normalized some biological indices of somatotrophic function in aged rats.

Study Information

Provider

pubmed

Year

1997

DOI

10.1006/phrs.1997.0203