Growth hormone axis peptides

Peptides that influence growth-hormone release (GHRH analogs and ghrelin-receptor agonists) and the IGF-1 axis.

Tier fingerprint · 11 compounds

S is approval-grade evidence; F is documented harm or near-zero human data. Each bar is how many peptides on this page land in that tier — a fast read on how much of this category sits in approval-grade evidence versus thin or vendor-driven claims.

S
1
A
1
B
0
C
1
D
3
F
5

The category at a glance

Every compound here ranked S–F by its weighted evidence score — strongest human / approval-grade evidence at the top, thin or vendor-driven claims at the bottom. Tap any row for the evidence read. Popularity never raises a tier.

Receipts, not vendor theater. Every tier here is computed from published evidence and regulatory status — not vendor marketing or influencer claims. See how we score.

S
human-growth-hormone
Strong human evidenceLow overstatementFDA-approved
90
/ 100

Recombinant hGH (somatropin) is an FDA-approved biologic identical to pituitary GH, with a large body of controlled-trial evidence for growth-hormone deficiency (pediatric and adult) and conditions such as Turner and Noonan syndromes. Unlike the research analogues, it has a defined approval and safety profile.

Tier read: strong human evidence · low overstatement risk · low search interest · Approved use. Why not A: supported by human evidence, preclinical depth, mechanism confidence, safety clarity, regulatory clarity, practical relevance.

Read the full human-growth-hormone profile →
A
tesamorelin
Strong human evidenceLow overstatementFDA-approved
87
/ 100

The most clinically validated compound in this group. A pivotal 412-patient randomized, placebo-controlled trial (Falutz, NEJM 2007) showed ~15% reduction in visceral fat in HIV-associated lipodystrophy, and it is FDA-approved as EGRIFTA for that indication. Caveats: benefits aren't sustained after stopping, and approval is narrow — not general anti-aging or body-composition use.

Tier read: strong human evidence · low overstatement risk · low search interest · Approved use. Why not B: supported by human evidence, preclinical depth, mechanism confidence, safety clarity, regulatory clarity, practical relevance. Why not S: held back by remaining gaps and limited replication.

Read the full tesamorelin profile →
C
sermorelin
Moderate human evidenceLow overstatementResearch-use-only
58
/ 100

A GHRH(1-29) analogue that stimulates endogenous GH release. It was FDA-approved (brand Geref) for growth-hormone-deficiency use in children, but the manufacturer voluntarily withdrew it from the US market in 2008 for commercial reasons — so no active FDA label governs current use, which is mainly compounded and off-label.

Tier read: moderate human evidence · low overstatement risk · low search interest · Early human. Why not D: supported by mechanism confidence. Why not B: held back by remaining gaps and limited replication.

Read the full sermorelin profile →
D
hexarelin
Early human evidenceMedium overstatementResearch-use-only
38
/ 100

A hexapeptide GH secretagogue that potently stimulates GH release in small human studies; its much-discussed cardioprotective effects are shown mainly in animal models. Human evidence is short-term and small-scale, and it is not FDA-approved.

Tier read: early human evidence · medium overstatement risk · low search interest · Early human. Why not F: supported by mechanism confidence. Why not C: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full hexarelin profile →
D
ghrp-2
Early human evidenceMedium overstatementResearch-use-only
38
/ 100

A ghrelin-receptor agonist (pralmorelin) used mainly as a GH-deficiency diagnostic and a probe of ghrelin biology; small human studies show it raises GH and increases appetite. Evidence is short-term and mechanistic, with no long-term outcome trials; not FDA-approved for general use.

Tier read: early human evidence · medium overstatement risk · low search interest · Early human. Why not F: supported by mechanism confidence. Why not C: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full ghrp-2 profile →
D
ghrp-6
Early human evidenceMedium overstatementResearch-use-only
38
/ 100

A synthetic GH-releasing peptide / ghrelin-receptor agonist. Human data come largely from small pharmacokinetic and GH-stimulation studies; broader cytoprotective claims rest mostly on preclinical work. No large human outcome trials, not FDA-approved.

Tier read: early human evidence · medium overstatement risk · low search interest · Early human. Why not F: supported by mechanism confidence. Why not C: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full ghrp-6 profile →
F
cjc-1295
Early human evidenceMedium overstatementResearch-use-only
33
/ 100

A long-acting GHRH analogue. In a real placebo-controlled trial in healthy adults (Teichman, JCEM 2006) it produced dose-dependent, sustained increases in GH (~2–10×) and IGF-1 (~1.5–3×) lasting days. Despite that verified human pharmacology, it is not FDA-approved and is used as a research chemical, with no long-term outcome data.

Tier read: early human evidence · medium overstatement risk · low search interest · Animal. Why not D: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full cjc-1295 profile →
F
ipamorelin
Early human evidenceMedium overstatementResearch-use-only
33
/ 100

A selective pentapeptide GH secretagogue that raises growth hormone without meaningfully changing prolactin, ACTH, or cortisol. Human data are limited to small, short-term pharmacology studies in healthy volunteers; it has no FDA approval and no large or long-term efficacy/safety trials — a research compound.

Tier read: early human evidence · medium overstatement risk · low search interest · Animal. Why not D: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full ipamorelin profile →
F
igf-1-lr3
Early human evidenceMedium overstatementResearch-use-only
33
/ 100

A synthetic IGF-1 analogue engineered for higher potency and reduced binding-protein affinity, studied almost exclusively in animal and cell models. Essentially no controlled human outcome trials; not an approved human drug.

Tier read: early human evidence · medium overstatement risk · low search interest · Animal. Why not D: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Read the full igf-1-lr3 profile →
F
cjc-1295-dac
Early human evidenceMedium overstatementResearch-use-only
29
/ 100

CJC-1295 with DAC is a long-acting GHRH analogue that binds albumin to extend its half-life to ~6–8 days. A small placebo-controlled trial in healthy adults showed sustained, dose-dependent rises in GH and IGF-1. Investigational, not FDA-approved; evidence is early-phase only.

Tier read: early human evidence · medium overstatement risk · low search interest · Mechanism. Why not D: held back by human evidence, preclinical depth, safety clarity, regulatory clarity, practical relevance.

Read the full cjc-1295-dac profile →
F
mod-grf-1-29
Early human evidenceMedium overstatementResearch-use-only
29
/ 100

Modified GRF 1-29 (CJC-1295 without DAC) is a DPP-IV-resistant GHRH(1-29) fragment with a short half-life and pulsatile GH-releasing action. Evidence is largely preclinical; rigorous controlled human data for the no-DAC form are lacking. A research analogue, not approved.

[1]Once-daily CJC-1295 normalizes growth in the GHRH-knockout mouseAm J Physiol Endocrinol Metab, 2006 (PMID 16822960)

Tier read: early human evidence · medium overstatement risk · low search interest · Mechanism. Why not D: held back by human evidence, preclinical depth, safety clarity, regulatory clarity, practical relevance.

Read the full mod-grf-1-29 profile →

Growth-hormone-axis peptides are a crowded, confusing category. The key is the mechanism split: GHRH analogs (sermorelin, CJC-1295, tesamorelin) and ghrelin-receptor agonists (ipamorelin, the GHRPs) push GH through two different levers — and only a couple of members are FDA-approved for narrow indications.

Beginner reading path

Start with the best-supported options first: tesamorelin, human-growth-hormone. Then compare them before exploring research-only compounds.

Read these in order
  1. This growth hormone axis overview (you're here)
  2. tesamorelin
  3. human-growth-hormone
  4. tesamorelin vs human-growth-hormone
  5. Safety & quality guide
Best supportedApproved or strong human evidence — read these first.
tesamorelinA
FDA-approved
human-growth-hormoneS
FDA-approved
Worth watchingPromising; meaningful evidence with gaps remaining.
sermorelinC
Research-use-only
Too earlyMostly preclinical or early-stage; human support is thin.
cjc-1295F
Research-use-only
cjc-1295-dacF
Research-use-only
mod-grf-1-29F
Research-use-only
ipamorelinF
Research-use-only
hexarelinD
Research-use-only
ghrp-2D
Research-use-only
ghrp-6D
Research-use-only
igf-1-lr3F
Research-use-only
Not proven for this goal
Safe long-term muscle buildingAnti-aging via raised GHPerformance gains without risk

What the evidence actually supports

Tesamorelin (a GHRH analog) is FDA-approved for a specific indication (HIV-associated visceral fat). Recombinant human growth hormone itself is approved for diagnosed deficiency. The secretagogues (ipamorelin, CJC-1295, sermorelin, GHRPs) reliably raise GH release mechanistically, but human safety/benefit data for the popular anti-aging and muscle uses is limited and research-only.

Where the hype outruns the data

“Safe anti-aging via raised GH” and “muscle without risk” aren't supported. Sustained GH elevation differs physiologically from natural pulses; raising IGF-1 carries theoretical long-term risks. These are not free upside.

FAQ

What's the difference between CJC-1295 and ipamorelin?

CJC-1295 is a GHRH analog (GHRH receptor); ipamorelin is a ghrelin-receptor agonist — two separate levers on the same GH axis, which is why they're often discussed together.

Is any GH peptide FDA-approved?

Tesamorelin is approved for a narrow indication; recombinant hGH is approved for deficiency. Most secretagogues are research-only.

Is this dosing advice?

No — research reference only, no protocols.

← All goalsFull tier boardCompare top two →

Research reference only. Not medical advice, dosing, or a recommendation to use any compound. “Worth watching” ≠ proven or safe.

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