CJC-1295 NO DAC

⚠️ Structural Separation Notice

The Ageless Pep Academy is a clinical education property independent from any commerce operation. Any references in this profile to Ageless Peps product SKUs, pricing, or the agelesspeps.com domain are for completeness and transparency; they are not endorsements and do not form part of the clinical education content. Clinicians are responsible for independent verification of any product sourcing decision. The Academy's Medical Director provides editorial oversight only and does not endorse commercial products.

Modified GRF(1-29), a GHRH analog that stimulates pulsatile growth hormone release from the anterior pituitary while preserving physiological feedback regulation.

Quick Facts

Property	Value
Also Known As	Mod-GRF(1-29), Modified GRF(1-29), CJC-1295 without DAC, Tetrasubstituted GRF(1-29)
Category	GH Axis / Muscle Growth / Anti-Aging / Recovery
Sequence	Tyr-D-Ala-Asp-Ala-Ile-Phe-Thr-Gln-Ser-Tyr-Arg-Lys-Val-Leu-Ala-Gln-Leu-Ser-Ala-Arg-Lys-Leu-Leu-Gln-Asp-Ile-Leu-Ser-Arg-NH2 (29 aa, 4 substitutions for protease resistance)
Molecular Weight	~3367 Da
Molecular Formula	C₁₅₂H₂₅₂N₄₄O₄₂
PubChem CID	91976842
Administration	SubQ
Typical Dose Range	100-200 mcg per injection (from literature)
Half-Life	~30 minutes (NO DAC version; preserves pulsatile GH secretion)
Storage	Lyophilized: -20C for 1-2 years; Reconstituted: 2-8C, use within 2-4 weeks
FDA Status	Research only. Not approved for any indication. CJC-1295 with DAC reached Phase II clinical trials but development was halted.
WADA Status	Prohibited (S2 – Peptide Hormones, Growth Factors, Related Substances)

Mechanism of Action

CJC-1295 NO DAC (Mod-GRF 1-29) is a synthetic analog of the first 29 amino acids of endogenous growth hormone-releasing hormone (GHRH), modified at four positions (Ala2, Ala8, Ala15, Leu27 substitutions) to confer resistance to dipeptidyl peptidase IV (DPP-IV) cleavage and enzymatic degradation. These substitutions extend the functional half-life from approximately 7 minutes (native GHRH) to approximately 30 minutes while maintaining the short-acting pharmacokinetic profile critical for preserving pulsatile GH secretion (PMID 15817669).

The peptide binds to GHRH receptors on anterior pituitary somatotrophs, stimulating both synthesis and pulsatile release of growth hormone (GH1, UniProt P01241). Unlike CJC-1295 with DAC (Drug Affinity Complex), which conjugates to albumin for a half-life of approximately 6-8 days and produces sustained "tonic" GH elevation, the NO DAC variant produces discrete GH pulses that mirror endogenous physiology. This pulsatile pattern is essential because continuous GH elevation downregulates GH receptors and induces insulin resistance, while pulsatile release maintains receptor sensitivity and normal metabolic signaling (PMID 17018654).

The critical pharmacological feature of CJC-1295 NO DAC is its synergy with ghrelin receptor agonists (GHSR/GHS-R1a, UniProt Q92847) such as Ipamorelin. Because GHRH and ghrelin act on different receptor systems to stimulate GH release from somatotrophs, co-administration produces a supra-additive GH pulse — reported at 7-10x greater amplitude than either agent alone. The short half-life also preserves normal somatostatin negative feedback, preventing GH axis suppression during chronic use (PMID 16352683).

Downstream, the GH pulses stimulate hepatic IGF-1 synthesis, activating anabolic and tissue repair signaling cascades throughout the body. This GH-IGF-1 axis activation supports lean mass accretion, fat oxidation, connective tissue repair, and sleep architecture improvement.

Key Research Areas

GH-IGF-1 axis optimization – Prolonged stimulation of pulsatile GH and IGF-1 secretion in human subjects with single and multiple doses
Growth normalization – CJC-1295 restores normal growth patterns in GHRH knockout mouse models
Somatopause management – Age-related GH decline reversal via pituitary stimulation
Body composition – GH-mediated lipolysis and lean mass accretion
Anti-doping detection – Extensive work on immunoassay and mass spectrometry methods for GHRH analog detection
Sports medicine – Emerging interest in peptide therapies for musculoskeletal recovery and performance
Synergistic GH secretion – Combined GHRH + GHRP protocols for amplified GH release

Evidence Level Summary

Evidence Type	Count	Notes
Human RCTs	1	Single-dose and multi-dose PK/PD in healthy volunteers
Human observational	1	Netnography of female use patterns
Animal in vivo	2	GHRH knockout mice, serum protein changes
In vitro	2	Detection methodology studies
Systematic reviews	0	—
Narrative reviews	3	Anti-doping, sports medicine, body composition

Clinical Applications

Fat Loss — GH-mediated lipolysis via pulsatile GH release
Sarcopenia — Lean mass preservation and accretion through GH-IGF-1 signaling
Injury Recovery — IGF-1-driven tissue repair and connective tissue remodeling
Sleep Disorders — Amplification of natural slow-wave sleep GH pulse

Protocols Using This Peptide

GH Optimization Protocol

Ageless Peps Products

AP-CJC1295-Vial — CJC-1295 NO DAC Vial, $84 (WC 670)
AP-CJC-Ipam-Blend — CJC-1295 NO DAC / Ipamorelin Blend, $64 (WC 780)

Dosing Reference

Research Dosing Ranges (from literature)

Route	Dose Range	Frequency	Duration	Source
SubQ	100 mcg (with GHRP)	1-3x daily, fasted	8-12 weeks on / 4 weeks off	PMID 17018654; practitioner consensus
SubQ	100-200 mcg (standalone)	1-3x daily, fasted	8-12 weeks	Less effective than combination

Cycling

Standard cycling: 5 days on / 2 days off; 8-12 weeks on / 4 weeks off. MUST be administered in a fasted state (minimum 2 hours post-meal; food blunts GH response). Pre-sleep dosing is optimal to amplify the natural slow-wave sleep GH pulse. Fasting insulin and IGF-1 levels should be monitored periodically.

Contraindications & Safety

Contraindications: Active malignancy (GH/IGF-1 can stimulate tumor growth); acromegaly; diabetic retinopathy (IGF-1 elevation risk); active pituitary tumors
Common side effects: Transient fluid retention, head rush at injection, injection site reactions, carpal tunnel symptoms at high doses
Drug interactions: Insulin and oral hypoglycemics (GH can antagonize insulin sensitivity at supraphysiologic levels); glucocorticoids (GH effects may be blunted); somatostatin analogs (octreotide, etc. will block GH release)
Pregnancy/nursing: Contraindicated; no safety data
Special populations: Caution in diabetics (monitor glucose); renal/hepatic impairment data lacking; not studied in pediatrics outside of growth disorders

Cancer Considerations

CAUTION — IGF-1 axis cancer risk. GH secretagogues raise IGF-1 levels. The Lancet meta-analysis associates elevated IGF-1 with prostate cancer (OR 1.49) and premenopausal breast cancer (OR 1.65) (PMID-15110491). However, the largest observational study (15,809 GH-treated adults) found cancer incidence comparable to the general population (SIR 0.92) (PMID-35368070). Expert consensus states "no association with cancer recurrence" (PMID-35319491). Action: Contraindicated in active malignancy. Use with caution in cancer survivors; require oncologist clearance and IGF-1 monitoring.

Synergistic Combinations

Ipamorelin + CJC-1295 NO DAC — Primary benchmark combination; 7-10x supra-additive GH pulse via dual receptor activation (GHRH-R + GHS-R1a)
Tesamorelin — Alternative GHRH analog; FDA-approved for HIV lipodystrophy, may be substituted in clinical settings
BPC-157 + CJC-1295 NO DAC — Tissue repair + GH-mediated anabolic support
AOD-9604 + CJC-1295 NO DAC — GH axis + direct lipolysis for body composition
TB-500 + CJC-1295 NO DAC — Recovery stack with complementary repair mechanisms

Related Research

PMID	Title	Year	Study Type
PMID-15817669 – CJC-1295 Discovery and Identification	Discovery and identification of CJC-1295	2005	Preclinical
PMID-17018654 – CJC-1295 Pulsatile GH Secretion in Humans	CJC-1295 pulsatile GH secretion in humans	2006	Human PK/PD
PMID-16352683 – Prolonged stimulation of growth hormone (GH) and insulin-lik	Prolonged stimulation of GH and IGF-1 secretion by CJC-1295	2006	Human RCT
PMID-16822960 – CJC-1295 Normalizes Growth in GHRH Knockout Mice	CJC-1295 normalizes growth in GHRH knockout mice	2006	Animal in vivo
PMID-19386527 – CJC-1295 GH-IGF-1 Axis Serum Protein Changes	CJC-1295 GH-IGF-1 axis serum protein changes	2009	Animal in vivo
PMID-26771670 – Netnography of Female Use of the Synthetic Growth Hormone CJ	Netnography of female use of CJC-1295	2016	Observational
PMID-30489688 – An immuno polymerase chain reaction screen for the detection	Immuno-PCR screen for CJC-1295 and GHRH analog detection	2018	In vitro
PMID-34665524 – Advances in the detection of growth hormone releasing hormon	Advances in GHRH synthetic analog detection	2021	In vitro
PMID-41966639 – Peptide Therapies for Musculoskeletal and Athletic Performance	Peptide therapies for musculoskeletal and athletic performance	2024	Review
PMID-32257855 – Growth Hormone Secretagogues in Body Composition Management	Growth hormone secretagogues in body composition management	2020	Review
PMID-41476424 – Injectable Peptide Therapy Primer for Sports Medicine	Injectable peptide therapy primer for sports medicine	2024	Review
PMID-15110491 – IGF-1 Cancer Risk Systematic Review Meta-Analysis	IGF-1 and cancer risk: systematic review + meta-analysis (Lancet)	2004	Meta-Analysis
PMID-35319491 – GH Replacement Safety in Cancer Survivors Consensus	GH replacement safety in cancer survivors: consensus statement	2022	Consensus
PMID-35368070 – Long-term Safety of Growth Hormone in 15809 Adults	Long-term safety of growth hormone replacement in 15,809 adults	2022	Cohort

References

PMID 15817669 — Discovery and DAC technology
PMID 17018654 — Human PK/PD data on pulsatile GH secretion
PMID 16352683 — Prolonged GH/IGF-1 stimulation in humans
PMID 16822960 — Growth normalization in GHRH-KO mice
PMID 32257855 — GHS body composition review
PMID 15110491 — Renehan AG et al. IGF-1 cancer risk: systematic review and meta-analysis. Lancet. 2004.
PMID 35319491 — GH Replacement in Cancer Survivors Consensus Statement. 2022.
PMID 35368070 — Long-term safety of growth hormone replacement in 15,809 adults. 2022.

#peptide #gh-axis #subq