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Written by Kim Callender, NP, FNP-BC·Reviewed by Jonathan Snipes, MD·Published July 12, 2026·Last reviewed July 12, 2026·Prices verified July 12, 2026·Methodology v1.0

Sermorelin: what the human evidence actually shows

Direct answer

Sermorelin is a synthetic fragment of growth hormone-releasing hormone. It stimulates the pituitary to produce and release the body's own growth hormone, rather than supplying growth hormone directly. It is prescribed off-label through telehealth and longevity clinics for adult growth-hormone optimisation, body composition, sleep and recovery.

What the evidence actually shows

Sermorelin does what it says mechanistically: it raises endogenous growth hormone and IGF-1. That is measurable and reasonably well-documented. What is much weaker is evidence that this translates into the outcomes it is sold for in healthy adults — fat loss, muscle gain, better sleep, slower ageing. The trials that exist are small, short, often uncontrolled, and frequently conducted in people with genuine growth-hormone deficiency, which is a different population from a healthy 45-year-old seeking optimisation. Extrapolating from deficiency treatment to healthy-adult enhancement is not a supported inference.

Three ways evidence gets overstated hereThree moves recur constantly in this category, and once you can name them you will see them everywhere. Mouse-to-human transfer: a striking longevity result in mice, presented as though it applies to you. Biomarker-for-outcome substitution: a study shows a blood level rose, and the marketing implies you will feel better or live longer. Deficiency-to-enhancement transfer: a treatment that helps people with a diagnosed deficiency is sold to healthy people seeking optimisation. None of these are valid inferences.

Absolute versus relative: reading the number correctly

Trial results are usually reported as relative figures, because relative figures are larger and therefore more persuasive. A "20% reduction in cardiovascular events" sounds transformative. The absolute reduction in SELECT was from 8.0% to 6.5% — about 1.5 percentage points over roughly three years. Both statements describe the same result honestly; only one of them tells you what to expect for yourself.

The same applies to weight-loss figures. A mean reduction of 20.9% is a mean. Individual results in these trials ranged from substantial loss to none at all, and a mean tells you nothing about where you personally would land. Anyone quoting a trial average as a promise is misusing it.

Funding and conflicts of interest

Every pivotal trial in this field was funded by the company that manufactures the drug it tested. That is normal in pharmaceutical research and it does not make the results false — these are large, well-conducted, peer-reviewed studies. It does mean the funding belongs in the citation every time, particularly for head-to-head trials where the funder makes the winning drug. SURMOUNT-5 was funded by Eli Lilly and found Lilly's drug superior. The result is plausible and consistent with the separate trial programmes; the disclosure still belongs beside it.

Where this sits against the other evidence

No single trial should be read alone. The strength of the GLP-1 evidence base is that multiple independent trial programmes — SURMOUNT for tirzepatide, STEP for semaglutide, SCALE for liraglutide, SELECT for cardiovascular outcomes — point in a consistent direction across tens of thousands of participants. That consistency is what makes the class credible.

What that consistency does not do is extend to products the trials never tested. Every one of those programmes studied an FDA-approved subcutaneous injection. None studied a compounded preparation, a microdose regimen, or an orally disintegrating tablet. The evidence is strong exactly where it was collected and silent everywhere else, and the gap between those two things is where most of the marketing in this industry operates.

Frequently asked questions

What does Sermorelin cost through telehealth?

We have not verified a price and will not publish one we cannot substantiate. This page gives you the method to evaluate any quote you are given.

Is Sermorelin FDA-approved?

Sermorelin was formerly FDA-approved (as Geref) for the diagnosis and treatment of growth hormone deficiency in children, but that product was withdrawn from the US market in 2008 — for commercial reasons, not safety. Sermorelin available today is a compounded preparati

Does Sermorelin work?

Sermorelin does what it says mechanistically: it raises endogenous growth hormone and IGF-1. That is measurable and reasonably well-documented. What is much weaker is evidence that this translates into the outcomes it is sold for in healthy adults — fat loss, muscle gain,

Sources

  1. U.S. Food and Drug Administration — approved labels and compounding guidance for this molecule.
  2. PubMed / NIH — indexed human clinical literature.
  3. ClinicalTrials.gov — registered trials, where they exist.
  4. Our source hierarchy and pricing-verification methodology.

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