Compound comparison

CJC-1295 + Ipamorelin vs Tesamorelin

CJC-1295 + Ipamorelin is one of the most discussed peptide stacks in online fitness and anti-aging communities, combining a growth hormone-releasing hormone (GHRH) analog with a growth hormone secretagogue (GHS) for theoretical synergistic GH release. Tesamorelin (Egrifta) is the only GHRH/GHS-class peptide with FDA approval — indicated specifically for reduction of excess visceral abdominal fat in HIV-infected patients with lipodystrophy. This comparison frames the differences in mechanism, evidence, regulatory status, and access paths without recommending either option.

Last reviewed 2026-07-08 Next review 2026-08-08

At a glance

Attribute CJC-1295 + Ipamorelin Tesamorelin (Egrifta)
Compound class GHRH analog (CJC-1295) + GHS (ipamorelin) stack GHRH analog (stabilized)
Mechanism Dual pathway: GHRH receptor + ghrelin receptor agonism GHRH receptor agonism (single pathway)
FDA approval Neither compound is FDA-approved FDA-approved as Egrifta (2010)
Approved indication None Reduction of excess visceral abdominal fat in HIV-associated lipodystrophy
Clinical trial data CJC-1295: single pharmacokinetic study. Ipamorelin: preclinical pharmacology + very limited human data. Combination: no published trials. Phase 3 randomized trial published in NEJM (Falutz et al., 2010)
Development status CJC-1295 development discontinued by ConjuChem. Ipamorelin never advanced to late-stage trials. Approved and marketed as Egrifta
Regulatory channel Research-use-only (RUO) suppliers or compounded via telehealth Prescription drug (FDA-approved, pharmacy-dispensed)
Cost context Lower per-vial cost through RUO suppliers; no drug-grade manufacturing standards Higher branded-drug cost; may be covered by insurance for approved indication
Evidence level Pharmacokinetic / preclinical / community discussion Phase 3 trial + FDA regulatory approval

CJC-1295 + Ipamorelin

Open the CJC-1295 evidence page

CJC-1295 is a synthetic growth hormone-releasing hormone (GHRH) analog developed by ConjuChem Biotechnologies using drug affinity complex (DAC) technology to bind albumin and extend half-life from minutes to days. A published pharmacokinetic study (Teichman et al., 2006, Journal of Clinical Endocrinology & Metabolism) showed that CJC-1295 increased GH and IGF-1 levels in healthy subjects for up to 6 days after a single dose — this is the primary published human data. ConjuChem discontinued clinical development and the compound was never submitted to the FDA for approval.

Ipamorelin is a synthetic pentapeptide growth hormone secretagogue (GHS) identified in the late 1990s. The original pharmacology was published in the European Journal of Endocrinology (Raun et al., 1998), describing ipamorelin as a selective GH secretagogue with minimal effect on cortisol or prolactin release in animal models. Ipamorelin is not FDA-approved for any indication and has extremely limited published human clinical data.

The theoretical rationale for stacking CJC-1295 with ipamorelin is pathway complementarity: CJC-1295 stimulates the GHRH receptor while ipamorelin activates the ghrelin receptor (GHS-R1a), potentially producing greater combined GH release than either compound alone. No published clinical trial has tested this specific combination for safety or efficacy.

Both compounds are individually unapproved and the combination has no regulatory approval in any jurisdiction. The stack's popularity is driven by community protocol sharing, telehealth prescribing patterns, and research-chemical marketplace availability — not by clinical evidence. Products marketed as 'research use only' are subject to FDA enforcement, including warning letters to suppliers who make implied human-use claims.

Tesamorelin (Egrifta)

Open the Tesamorelin evidence page

Tesamorelin (brand name Egrifta) received FDA approval in 2010 for the reduction of excess visceral abdominal fat in HIV-infected patients with lipodystrophy. It is the only GHRH or GHS-class peptide with current FDA approval. The FDA drug label documents the approved indication, administration route (subcutaneous injection), and safety profile.

The pivotal Phase 3 trial was published in the New England Journal of Medicine (Falutz et al., 2010; PMID 20879920), showing significant reduction in visceral adipose tissue (VAT) over 26 weeks in HIV patients with lipodystrophy. The trial population was HIV patients with lipodystrophy — the approval is specifically for this indication, not for general obesity, cosmetic fat loss, or anti-aging.

Tesamorelin is a stabilized GHRH analog; its mechanism involves stimulating endogenous GH release, which in turn increases lipolysis and reduces visceral fat accumulation. It uses the same GHRH receptor pathway as CJC-1295 but was engineered for drug development, passed FDA review, and has published Phase 3 clinical trial data.

Tesamorelin is accessed through the prescription drug channel — a licensed provider, a pharmacy, and clinical records. Some telehealth platforms prescribe tesamorelin for its FDA-approved indication or, in some cases, off-label. Any use outside the approved HIV-associated lipodystrophy indication is off-label.

Summary verdict

Tesamorelin has the strongest evidence base in this comparison: a published Phase 3 randomized trial in a defined patient population (HIV lipodystrophy), FDA review and approval, and a labeled drug product. CJC-1295 has a single published pharmacokinetic study showing GH and IGF-1 increases in healthy volunteers, but no clinical outcomes trial and no regulatory approval. Ipamorelin has preclinical pharmacology data and extremely limited published human data. The CJC-1295 + ipamorelin combination has no published clinical trial data at all. This evidence hierarchy — FDA-approved drug with Phase 3 data vs research compounds with pharmacokinetic-only or preclinical data — is the core distinction this comparison documents. Neither option is recommended; this page exists to help readers understand the differences in access paths and evidence, not to choose a treatment.

Related compounds: CJC-1295 · Ipamorelin · Tesamorelin

Sources on this page

Source records are stored in the repo and linked from this comparison.

Egrifta (tesamorelin) — FDA Drug Label

U.S. Food and Drug Administration · Primary regulatory · 2010-06-18 · accessed 2026-07-01

FDA-approved drug label for Egrifta (tesamorelin for injection), indicated for the reduction of excess visceral abdominal fat in HIV-infected patients with lipodystrophy. The only GHRH/GHS-class peptide with FDA approval.

Tesamorelin Clinical Trial Registry Entries — ClinicalTrials.gov

ClinicalTrials.gov / U.S. National Library of Medicine · Primary regulatory · 2010-01-01 · accessed 2026-07-01

ClinicalTrials.gov registry entries for tesamorelin clinical trials, including the pivotal Phase 3 trials for HIV-associated lipodystrophy that supported FDA approval of Egrifta.

Pharmacokinetics and Pharmacodynamics of CJC-1295, a Long-Acting GHRH Analog

Journal of Clinical Endocrinology & Metabolism (PubMed) · Peer reviewed · 2006-05-01 · accessed 2026-07-01

Teichman et al. (2006) pharmacokinetic study (PMID 16569233) showing that CJC-1295 increased GH and IGF-1 levels in healthy subjects for up to 6 days after a single dose. The primary published human data for CJC-1295.

Ipamorelin, the First Selective Growth Hormone Secretagogue — Pharmacology

European Journal of Endocrinology (PubMed) · Peer reviewed · 1998-12-01 · accessed 2026-07-01

Raun et al. (1998) original pharmacology publication (PMID 9860070) describing ipamorelin as a pentapeptide growth hormone secretagogue with selectivity for GH release over cortisol and prolactin in animal models.

Warning Letter: Gram Peptides

U.S. Food and Drug Administration · Primary regulatory · 2026-03-31 · accessed 2026-06-30

FDA warning letter discussing peptide products marketed online and the limits of research-use-only positioning.