Growth Hormone AxisCompounded · Rx Only

SermorelinPulsatile GH release

Understand the mechanism, the current regulatory status, and the evidence — then decide your next step with a clinician who knows these compounds. The information below is educational reference only.

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Mechanism

Pulsatile GH release from pituitary, modest IGF-1 rise

Researched For

Sleep quality, Enhanced recovery, Modest body composition

The essentials

At a Glance

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Dosage

200–300 mcg subcutaneous, nightly.

Protocol

8–12 weeks on, 2–4 weeks off. 30–60 min before bed, at least 2 h fasted.

Results timeline

Sleep improvements possibly within 1–2 weeks; GH/IGF-1 elevation measurable within the first month; body-composition changes typically 8–12 weeks.

Side effects

Transient facial flushing (most common), mild injection-site reactions, occasional peripheral tingling that resolves with dose reduction.

Best stacked with

Tesamorelin (more potent GHRH analog if stronger stimulation is needed); GLP-1 agonists (metabolic synergy during caloric restriction).

Regulatory status

Sermorelin was FDA-approved in 1997 under the brand name Geref for diagnosis and treatment of idiopathic growth hormone deficiency in children, and was commercially withdrawn by EMD Serono in 2008 for manufacturing/business reasons — explicitly not a safety action, and its prior approval was never revoked. This gives it the most defensible compounding position of any GH secretagogue: under Section 503A, previously-approved compounds have the clearest legal pathway, unlike CJC-1295 no-DAC (no FDA history) or ipamorelin (PCAC declined to recommend it for the 503A Bulks List in October 2024). FDA enforcement against compounded peptides tightened in late 2024. Sermorelin is available through compounding pharmacies by prescription, is otherwise classified as a research compound, and is prohibited by WADA for competitive athletes.

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Sermorelin is GRF(1-29) — the active core of GHRH, produced synthetically. It earned FDA approval in 1997 (Geref), the first synthetic GH secretagogue to clear the bar; EMD Serono pulled it in 2008 for manufacturing economics, not safety. That history gives it the most defensible legal position of any GH secretagogue in compounding today. But adult evidence is thin: the entire clinical case rests on Khorram et al. (1997) — 19 elderly subjects, 16 weeks, single-blind — showing +1.26 kg lean mass in men (not women), no significant fat loss, no bone-density change. Compared with tesamorelin's 816-patient Phase III program, the gap is not subtle. Where it earns its place: clean selectivity, preserved somatostatin feedback, and a gentler GH stimulus suited to recovery support during caloric restriction.

What Is Sermorelin?

The first 29 amino acids of GHRH (GRF 1-29) — the minimum fragment to fully activate the GHRH receptor and trigger GH release. ~3,358 Da, structurally unmodified, with a short IV half-life of 10–20 min; it clears within ~4 h though GH effects persist ~3 h after activation. The brevity is a feature — a crisp GH pulse mimicking what the pituitary does during deep sleep.

How Sermorelin Works

It activates the GHRH receptor on pituitary somatotrophs via the cAMP/PKA cascade — the same one endogenous GHRH uses. Like ringing the doorbell the hypothalamus rings each night during deep sleep.

The somatostatin brake (safety advantage): when GH/IGF-1 rise, the hypothalamus releases somatostatin telling the pituitary to stop — so sermorelin can't easily drive supraphysiological GH levels. Exogenous rhGH bypasses this feedback entirely, which is why rhGH risks supraphysiological GH while sermorelin makes overdose difficult. It preserves the natural pulsatile pattern. Clean selectivity: at physiological doses it doesn't elevate cortisol, ACTH, or prolactin — distinguishing it from older ghrelin-receptor agonists (GHRP-2, GHRP-6).

The FDA Story

1997 approval: Geref, for diagnosis/treatment of idiopathic GH deficiency in children, based on trials showing significant height-velocity increases over 12 months (data to 36 months). Less potent than rhGH at equivalent doses, but offering physiological regulation. 2008 commercial withdrawal: EMD Serono pulled it for manufacturing economics against entrenched rhGH products — not a safety action; prior approval was never revoked. Why it matters: under Section 503A, previously-FDA-approved compounds have the clearest compounding pathway. Sermorelin checks that box unambiguously, unlike CJC-1295 no-DAC (no human trials, no FDA history) or ipamorelin (Phase II for a different indication, never approved) — both briefly on the FDA Category 2 list in 2024.

Clinical Evidence

Pediatric: adequate for approval — significant height-velocity increases over 12 months (to 36 months), consistently less effective than rhGH at equivalent doses (the trade-off is physiological regulation vs raw potency). Adult: essentially one trial — Khorram et al. (1997), 19 subjects (ages 55–71), 16 weeks, single-blind. Improved: nocturnal GH, IGF-1, IGFBP-3, and lean mass in men only (~1.26 kg). No change: total body fat, BMI, bone density, or lean mass in women. Limitations: tiny sample, single-blind, gender-discordant, short duration, no functional endpoints. This single trial is the source of virtually every "sermorelin builds lean mass" claim; whether it generalizes to today's typical 35–55-year-old users is unknown.

Compound	Best adult evidence	Sample	Duration	Key outcome
Tesamorelin	Phase III RCTs (LIPO-010/1011)	N=816	26–52 wks	15–20% VAT reduction vs placebo
MK-677	2-year RCT (Nass 2008)	N=65	2 years	+1.1 kg lean mass, no strength gain
Sermorelin	Single trial (Khorram 1997)	N=19	16 weeks	+1.26 kg lean mass (men only), no fat/BMD change
Ipamorelin	PK/PD characterization only	—	8–12 wks	No body-composition RCT
CJC-1295 no-DAC	No human trials	—	8–16 wks	No published efficacy data

Benefits: Evidence vs Marketing

Supported by direct evidence: reliable GH and IGF-1 elevation; limited lean-mass gain (Khorram, men only). Mechanism but not direct trial data: sleep quality (GH is tied to slow-wave sleep; MK-677 raised Stage 4 sleep ~50%, but sermorelin's sleep outcomes aren't directly measured), recovery/tissue repair. Claimed but unsupported: independent fat loss (Khorram found no change in body fat/BMI), and broad "anti-aging" — the GH-secretagogue class repeatedly raises lean mass without improving strength or function (MK-677, anamorelin).

Side Effects

Mild and well-characterized from its years as an approved product: transient facial flushing and injection-site reactions are most common; mild peripheral edema and tingling are less frequent than with tesamorelin. No cortisol/ACTH/prolactin elevation at standard doses. The somatostatin feedback provides an extra safety margin. Periodic IGF-1 testing is prudent during extended use.

Sermorelin vs Tesamorelin

Both are GHRH-receptor agonists. Structure: sermorelin is GRF(1-29), unmodified; tesamorelin keeps the full 44-aa sequence plus a trans-3-hexenoic acid group protecting against DPP-IV, giving modestly better stability. Evidence: tesamorelin has two Phase III RCTs (N=816, CT-measured visceral fat) vs sermorelin's one 19-subject adult trial. Regulatory: tesamorelin is currently FDA-approved (Egrifta) for HIV-associated lipodystrophy; sermorelin was approved but commercially withdrawn — both legally compoundable. Why choose sermorelin: better tolerability in edema-sensitive people, lower cost via compounding, and a gentler stimulus when maximal potency isn't the goal.

Legal Status and Compounding

Sermorelin's position is the clearest of any GH secretagogue in compounding: its 1997 FDA approval and non-safety withdrawal fit the 503A pathway cleanly, unlike CJC-1295 no-DAC and ipamorelin (regulatory uncertainty; PCAC declined to recommend ipamorelin for the 503A Bulks List in October 2024). FDA enforcement against compounded peptides tightened in late 2024 (warning letters, 40+ state AGs), primarily targeting GLP-1s but with broader implications; sermorelin's prior approval offers some insulation. Available by prescription through compounding pharmacies; a research compound otherwise; WADA-prohibited for competitive athletes.

Straight answers

Frequently asked

Is sermorelin FDA-approved?

It was approved in 1997 (Geref) for pediatric GH deficiency, then commercially withdrawn by EMD Serono in 2008 for manufacturing/business reasons, not safety. It's now available through compounding pharmacies by prescription.

How long does it take to work?

Acute GH-stimulating effects occur within hours. Clinicians report sleep improvements within 1–2 weeks and body-composition changes over 8–12 weeks, though these timelines come from practice rather than controlled studies.

What's the difference between sermorelin and HGH?

Sermorelin stimulates your pituitary to release its own GH, preserving natural pulsatility and somatostatin feedback; rhGH is the hormone itself and bypasses the pituitary, which is why rhGH can reach supraphysiological levels while sermorelin's effect is self-limiting.

What's the difference between sermorelin and tesamorelin?

Both are GHRH-side peptides but not interchangeable. Tesamorelin is stronger for visceral fat, waist/liver phenotype, GLP-1 lean-mass support, or a robust GH signal (with IGF-1 monitoring). Sermorelin is the gentler/access-driven fallback — shorter-acting, more pituitary-reserve-dependent, often used when tesamorelin is too expensive, too strong, or unavailable.

Can you take sermorelin long-term?

Long-term adult data are limited (longest trial 16 weeks). IGF-1 stayed above baseline two weeks after stopping in elderly men (no immediate rebound). Practice commonly uses 8–12 weeks on, 2–4 weeks off, derived from experience rather than dose-duration studies.

Keep exploring

References

DrugBank. Sermorelin (DB00010). DrugBank DB00010
Walker RF. Sermorelin: a better approach to management of adult-onset GH insufficiency? Clin Interv Aging 2006;1(4):307-308. PMC2699646
Keating GM, Wellington K. Sermorelin: a review of its use in diagnosis and treatment of children with idiopathic GHD. BioDrugs 2004;18(5):339-354. PubMed 18031173
Frier Levitt. Regulatory Status of Peptide Compounding in 2025. Frier Levitt
Khorram O et al. Endocrine and metabolic effects of long-term administration of [Nle27]GHRH-(1-29)-NH2 in age-advanced men and women. J Clin Endocrinol Metab 1997;82(5):1472-1479. PubMed 9141536
Falutz J et al. Effects of tesamorelin in HIV-infected patients with excess abdominal fat: pooled Phase 3 analysis. J Clin Endocrinol Metab 2010;95(9):4291-4304. PubMed 20554713
Nass R et al. Effects of an oral ghrelin mimetic on body composition in healthy older adults. Ann Intern Med 2008. PMC2757071
Sinha DK et al. Beyond the androgen receptor: GH secretagogues in body composition. Transl Androl Urol 2020;9(Suppl 2):S149-S159. PMC7108996
Sigalos JT, Pastuszak AW. The safety and efficacy of growth hormone secretagogues. Sex Med Rev 2018;6(1):45-53. PMC5632578
Wakabayashi H et al. The regulatory approval of anamorelin for cachexia in Japan. 2021. PMC7890143
FDA Egrifta Prescribing Information (2025 label). FDA Label
Falutz J et al. Metabolic effects of a growth hormone-releasing factor in patients with HIV. N Engl J Med 2007;357(23):2359-2370. PubMed 18057338
Alba-Roth J, Muller OA et al. Sermorelin: a review of its pharmacology and efficacy in GH deficiency. Drugs 1988. PMID 2545260

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