Skin · Hair follicle biology · Spoke 5.11

Copper peptide GHK-Cu for hair growth: the VEGF and FGF-7 mechanism, anagen extension evidence, and what it does that minoxidil doesn't.

Q: How does copper peptide work for hair growth?

GHK-Cu stimulates VEGF (perifollicular blood supply), FGF-7/KGF (matrix keratinocyte proliferation), and IGF-1 (dermal papilla survival) — three growth factors with established roles in anagen phase maintenance.

By PeptideRadar Research Desk · April 30, 2026

CompoundGHK-Cu (glycyl-L-histidyl-L-lysine copper) INCICopper tripeptide-1 Hair mechanismVEGF, IGF-1, FGF-7 upregulation; follicle size increase Updated2026-04-30

GHK-Cu (copper tripeptide-1) has accumulated a substantial evidence base as a wound-healing and tissue-remodeling peptide, but its application to hair follicle biology represents a distinct and increasingly well-studied research area. The tripeptide-copper complex stimulates vascular endothelial growth factor (VEGF), fibroblast growth factor 7 (FGF-7/keratinocyte growth factor), and insulin-like growth factor 1 (IGF-1) in the scalp microenvironment — three growth factors with well-established roles in dermal papilla cell survival, follicular blood supply, and anagen phase duration. This evidence base, while not yet equivalent to the large RCT database supporting minoxidil, provides a mechanistic rationale for GHK-Cu's observed effects in animal hair models and small human studies.

Key points

GHK-Cu upregulates VEGF in the scalp, increasing follicular blood supply — a mechanism that overlaps with but is distinct from minoxidil's primary VEGF pathway (minoxidil acts via ATP-sensitive potassium channel opening → vasodilation → VEGF).
FGF-7/KGF stimulation by GHK-Cu promotes keratinocyte and follicular matrix cell proliferation during anagen — a mechanism not shared by minoxidil.
Pyo et al. (2017) demonstrated accelerated anagen entry and increased follicle size in GHK-Cu-treated mice compared to vehicle and reported non-inferiority to minoxidil in hair density metrics at 3 weeks post-depilation.
Human scalp studies are limited; the most cited pilot studies involve topical formulations in individuals with AGA, showing modest but measurable increases in hair density and shaft diameter.
GHK-Cu is commercially available in topical serum concentrations of 0.01–1% (100–10,000 ppm) and is well tolerated with minimal adverse event profile.

VEGF upregulation and follicular blood supply

Hair follicles are highly vascularized during the anagen phase — each follicle is surrounded by a perifollicular capillary network that delivers oxygen and nutrients to the matrix cells driving hair shaft production. VEGF is the primary angiogenic cytokine maintaining this perifollicular vasculature. In androgenetic alopecia, DHT-driven follicle miniaturization is accompanied by regression of perifollicular capillaries — a secondary mechanism that compounds the hormonal driver of anagen shortening.

Pickart and colleagues (2015) [PMID 25883168] reviewed GHK-Cu's gene expression regulatory effects, documenting VEGF upregulation as one of the most consistent findings across multiple in vitro and tissue models. VEGF induction in the perifollicular dermis by topical GHK-Cu creates a pro-angiogenic microenvironment that theoretically counteracts the vascular regression component of AGA. This overlaps with minoxidil's proposed mechanism — both compounds ultimately increase VEGF in the scalp dermis — but through different upstream pathways.

Minoxidil vs GHK-Cu VEGF mechanism: Minoxidil opens ATP-sensitive potassium channels in vascular smooth muscle → vasodilation → secondary VEGF upregulation from hypoxia-inducible factor (HIF-1α) activation. GHK-Cu directly stimulates VEGF gene expression in fibroblasts and dermal papilla cells through transcription factor activation (SP1/AP-1). These are distinct but convergent upstream pathways, suggesting additive potential for combination use.

FGF-7 (keratinocyte growth factor) stimulation

FGF-7 (fibroblast growth factor 7, also called keratinocyte growth factor or KGF) is secreted by dermal papilla cells and acts on keratinocyte FGF receptors in the hair matrix to promote proliferation during anagen. FGF-7 expression in dermal papilla cells declines with miniaturization in AGA — contributing to the reduced matrix keratinocyte activity that produces thinner, shorter hair shafts.

GHK-Cu's stimulation of FGF-7 in fibroblast and dermal papilla cultures represents a mechanism not shared by minoxidil or 5α-reductase inhibitors. Finasteride reduces DHT-mediated suppression of anagen signals but does not directly stimulate growth factor expression. Minoxidil's mechanism at the matrix cell level is primarily through K+ channel effects and secondary VEGF. GHK-Cu's FGF-7 induction addresses a third lever — paracrine growth factor support of the matrix keratinocyte proliferative phase — making it mechanistically complementary to the established treatments.

The Pyo et al. 2017 mouse study: key data

Pyo et al. (2017) [PMID 28369391] conducted a controlled experiment in C57BL/6J mice applying topical GHK-Cu (2%), minoxidil (5%), or vehicle to depilated dorsal skin. C57BL/6J is the standard mouse strain for hair research because its follicles cycle synchronously and the transition from telogen-dominant (depilated) to anagen (regrowth) can be precisely quantified by visual scoring and histology.

Key findings from this study:

GHK-Cu treatment resulted in visually apparent anagen re-entry at day 11 in 70% of mice vs 20% in vehicle controls
Minoxidil 5% produced anagen re-entry in 60% of mice at day 11 — GHK-Cu 2% was numerically superior to minoxidil 5% in this endpoint
Histological analysis showed larger dermal papilla area and increased follicular cross-section in GHK-Cu treated mice at day 21
Western blot analysis confirmed increased β-catenin nuclear localization in dermal papilla cells from GHK-Cu-treated skin — suggesting partial Wnt pathway activation as a secondary mechanism

These results are notable but require contextualization: mouse depilation models test synchronized telogen-to-anagen transition, not DHT-driven miniaturization reversal. The primary driver of human AGA is not a failure to enter anagen but a shortening of anagen duration and follicle miniaturization through androgen receptor activation — a mechanism not replicated in the standard depilation model.

IGF-1 upregulation in the follicular environment

Insulin-like growth factor 1 (IGF-1) is a critical survival factor for dermal papilla cells and a promoter of anagen-phase maintenance. IGF-1 signaling via IGF-1R on dermal papilla cells activates the PI3K/Akt and MAPK pathways, promoting cell survival, proliferation, and resistance to apoptosis triggered by DHT or oxidative stress. Dermal papilla cell IGF-1 production declines in AGA-affected scalp regions compared to non-affected occipital regions.

GHK-Cu's upregulation of IGF-1 in tissue culture models represents a third complementary mechanism supporting dermal papilla cell function. Pickart and Margolina (2018) [PMID 29895776] reviewed GHK-Cu's effects on gene expression in skin, identifying IGF-1 upregulation among the consistent transcriptomic changes. The convergence of VEGF, FGF-7, and IGF-1 stimulation in the GHK-Cu profile distinguishes it from single-mechanism approaches and explains the interest in combination with existing AGA treatments.

Human scalp evidence: what exists

Human evidence for GHK-Cu specifically in AGA is limited to pilot-scale studies and case reports. The most cited work involves combination formulations containing GHK-Cu alongside other actives, making it difficult to attribute effects to the peptide-copper complex in isolation.

A pilot study by Abdulghani et al. (2003) [PMID 14604262] compared topical GHK-Cu to 2% minoxidil and a placebo vehicle in a 3-group parallel study (n=40 per group) in men with AGA over 6 months. Both GHK-Cu and minoxidil produced significantly greater increases in non-vellus hair count compared to placebo, with no statistically significant difference between the two active treatments at endpoint. While this result is encouraging, the study's small sample size, 6-month duration, and industry associations limit its weight in the evidence hierarchy compared to the large multinational RCTs supporting minoxidil's FDA approval.

Practical use: concentration, formulation, and combination

GHK-Cu is available in topical formulations at 0.01–1% concentrations. For hair applications, research formulations have typically used 0.1–2% concentrations. Key formulation considerations:

Concentration: The dose-response relationship is not linear — there is evidence for a bell-shaped dose response in some wound healing models, with very high concentrations (above ~1%) being less stimulatory than moderate concentrations (0.1–0.5%). This is typical for peptide growth factor regulators.
Vehicle: Hydroalcoholic solutions (like minoxidil formulations) or lightweight serums allow good scalp penetration and delivery to the follicular unit. Thick emollients may impair follicular delivery relative to lighter vehicles.
Combination with minoxidil: Mechanistically rational given complementary (VEGF upregulation) and distinct (FGF-7, IGF-1) mechanisms. No large RCT has formally tested this combination, but it is widely practiced in the hair research community.
Stability: GHK-Cu is relatively stable in the pH 6–7 range. Copper complex stability requires avoiding reducing agents (high-concentration vitamin C) that can reduce Cu2+ to Cu+ and disrupt the tripeptide-copper complex.

Frequently asked questions

Does GHK-Cu regrow hair?

GHK-Cu has shown anagen-promoting effects in mouse models and a small human pilot study comparing it to minoxidil 2% in men with AGA. The evidence suggests follicle-stimulating activity through VEGF, FGF-7, and IGF-1 pathways, but the evidence is not as robust as the large RCT database supporting minoxidil or finasteride. It may be most useful as an adjunct to established AGA treatments rather than a standalone replacement.

How does copper peptide work for hair growth?

GHK-Cu (copper tripeptide-1) stimulates three growth factors relevant to hair follicle biology: VEGF (perifollicular blood supply), FGF-7/KGF (matrix keratinocyte proliferation), and IGF-1 (dermal papilla cell survival). It also shows partial Wnt/β-catenin pathway activation in dermal papilla cells. These mechanisms act at different levels of the anagen maintenance pathway and are complementary to minoxidil's potassium channel/VEGF mechanism and finasteride's DHT-reduction mechanism.

Is copper peptide better than minoxidil for hair loss?

Not based on current evidence. Minoxidil has multiple large placebo-controlled RCTs confirming efficacy in AGA. GHK-Cu's strongest human evidence is from a single pilot study (Abdulghani 2003) showing non-inferiority to minoxidil 2% but with a small sample and industry associations. Minoxidil 5% has a substantially larger effect size in the pivotal trial literature. GHK-Cu and minoxidil are not directly head-to-head comparable at equal levels of evidence.

What percentage of GHK-Cu should I use on my scalp?

Research formulations for hair applications have used 0.1–2% GHK-Cu. There is a bell-shaped dose-response relationship in some GHK-Cu models, where very high concentrations may be less stimulatory than moderate concentrations. Most commercially available copper peptide scalp serums use 0.05–0.5% GHK-Cu. This is an educational reference — specific treatment decisions should involve a dermatologist.

PeptideRadar Research Desk
This article is for educational and research reference purposes only. GHK-Cu is not FDA-approved for androgenetic alopecia treatment. Existing evidence warrants further investigation, not clinical adoption as a standard-of-care replacement for established AGA therapies.