CJC-1295 (no DAC)vsGHRP-2

CJC-1295 (no DAC), also known as Mod GRF 1-29, is a synthetic analogue of the first 29 amino acids of growth hormone-releasing hormone (GHRH). Four amino acid substitutions (at positions 2, 8, 15, and 27) have been made to increase resistance to enzymatic degradation while preserving full biological activity at the GHRH receptor (GHRH-R), a G protein-coupled receptor expressed on somatotroph cells in the anterior pituitary.

When CJC-1295 binds the GHRH receptor, it activates the Gs alpha subunit, which stimulates adenylyl cyclase to produce cyclic AMP (cAMP). Rising cAMP levels activate protein kinase A (PKA), which phosphorylates CREB (cAMP response element-binding protein) and other transcription factors that drive GH gene expression and secretion. Importantly, this mechanism preserves the natural pulsatile pattern of GH release because it works within the existing hypothalamic-pituitary feedback loop — somatostatin still provides inhibitory regulation between pulses.

The key advantage of the no-DAC version over the DAC version is this preservation of pulsatility. Because its half-life is approximately 30 minutes, it produces a discrete GH pulse that rises and falls naturally, mimicking the body's own secretory pattern. This pulsatile pattern is believed to be physiologically superior to sustained elevation because GH receptor sensitivity is maintained between pulses, and the liver's IGF-1 production response is optimized by intermittent rather than continuous GH stimulation. This is why CJC-1295 (no DAC) is often preferred by practitioners despite requiring more frequent dosing.

GHRP-2 (Growth Hormone Releasing Peptide-2) is a synthetic hexapeptide that binds to the GHS-R1a receptor on pituitary somatotrophs with high affinity, making it the second most potent GHRP for GH release after hexarelin. It activates the canonical Gq/11-PLC-IP3-calcium pathway, triggering robust GH vesicle exocytosis.

Beyond direct pituitary action, GHRP-2 modulates GH release at the hypothalamic level through two complementary mechanisms. It stimulates GHRH-producing neurons in the arcuate nucleus, amplifying the endogenous GHRH signal, and simultaneously suppresses somatostatin release from periventricular neurons, removing the inhibitory brake on GH secretion. This dual hypothalamic action explains why combining GHRP-2 with a GHRH analogue produces synergistic rather than merely additive GH release — the GHRP removes somatostatin inhibition while the GHRH analogue directly activates somatotrophs.

GHRP-2 occupies a middle ground in the GHRP family regarding selectivity. It produces moderate cortisol and prolactin elevation — less than hexarelin but more than ipamorelin. Its ghrelin-mimetic activity also stimulates appetite through hypothalamic NPY/AgRP neurons, though this effect is less pronounced than GHRP-6. Some research suggests GHRP-2 may have gastroprotective properties, with studies showing protection against ethanol-induced gastric mucosal damage in animal models. The peptide has been most extensively studied in Japan, where clinical trials evaluated its potential for treating GH deficiency, and it remains one of the best-characterized GHRPs in terms of pharmacology and dose-response relationships.