House of Peptides · Educational Research Hub

The Science of
Women's Health Peptides

From HPG axis restoration and PCOS metabolic support to menopausal longevity and libido science — the cutting-edge peptide research addressing women’s most underserved health needs. 🌸
🧬9
Peptides Covered
3
FDA Approved
🌡️1B+
Peri/Post-Menopausal
⚖️6%
R&D Funding Gap
scroll down

⚠️ Educational Content Only: This page is for informational purposes only and does NOT constitute medical advice. Women's hormonal health is highly individual — never modify hormonal therapies, fertility treatments, or use research peptides without a licensed physician's guidance. Always consult your doctor.

The Scale of the Challenge

Women's Health: A Research & Funding Crisis

Women's health conditions affect billions globally yet receive only 6% of total pharma R&D funding (WEF 2026). Peptide science is emerging as a key bridge in this gap.

🔄
1 in 10

Women have PCOS

Most common female endocrine disorder globally

🌡️
1 Billion

Peri/Post-Menopausal

Women worldwide by 2025 — fastest-growing demographic

💗
43%

Report Low Desire (HSDD)

Women with hypoactive sexual desire disorder

🌸
1 in 6

Couples Face Infertility

Female-factor accounts for ~50% of cases

🧬
6%

Women with Endometriosis

~200 million women globally; median 7-yr diagnosis delay

📉
30%

Collagen Lost in 5 Years

Post-menopausal estrogen decline drives rapid skin aging

⚖️
70–80%

GH Decline Post-Menopause

Growth hormone amplitude reduction by age 60 vs 30

🔬
6%

Research Funding Share

Women's health gets only 6% of global pharma R&D (WEF 2026)

🔄

PCOS — The Silent Epidemic

Polycystic ovary syndrome affects 1 in 10 women globally — the most common endocrine disorder of reproductive age. Driven by insulin resistance and HPG axis dysregulation, PCOS is now one of the most active areas of peptide intervention research, with GLP-1/GIP agonists demonstrating 40–60% cycle restoration rates.

🌡️

Menopause: 34 Symptoms, 1 Billion Women

Over 1 billion women are peri- or post-menopausal globally. Beyond hot flashes, menopause drives 30% dermal collagen loss in 5 years, 70–80% GH amplitude decline, accelerating bone density loss, cardiovascular risk and cognitive vulnerability. Peptides target the upstream hormonal cascade and downstream consequences simultaneously.

💗

Female Sexual Dysfunction: Under-Diagnosed, Under-Treated

43% of women report low sexual desire (HSDD). Until 2015, there were zero FDA-approved treatments for female sexual dysfunction. PT-141 (Vyleesi® 2019) marks the beginning of a new era — targeting the CNS desire circuit rather than peripheral vascular mechanisms — a fundamentally different and more accurate model of female sexual response.

The Biology

The Female Hormonal Lifecycle

The HPG axis — regulated at its apex by kisspeptin — governs 40+ years of cyclical hormonal change. Each life stage creates distinct peptide intervention opportunities.

🌱
Stage 1

Puberty (9–16)

Kisspeptin surge triggers HPG axis activation; menarche; estradiol rises

🌸
Stage 2

Reproductive (17–39)

Cyclical LH/FSH/E2/P4 pulses govern 28-day cycle; peak fertility; GH-IGF axis active

🔄
Stage 3

Perimenopause (40–51)

Follicle count decline; erratic E2 & P4; FSH rises; GH amplitude falls; vasomotor symptoms begin

🍂
Stage 4

Menopause (avg 51)

Final menstrual period; E2 <30 pg/mL; bone density loss accelerates; collagen loss 30% in 5 years

Stage 5

Post-Menopause (52+)

Stable low-estrogen state; cardiovascular, bone, cognitive, skin risks elevate; peptide intervention most studied

The HPG Axis: Kisspeptin as Master Regulator

How the hypothalamic-pituitary-gonadal axis drives the female cycle — and where it can fail

Kisspeptin Neurons
(Hypothalamus)
🎯 Kisspeptin-10
GnRH Pulse
(Hypothalamus)
LH + FSH Release
(Anterior Pituitary)
Ovarian Follicle
(Ovaries)
Estradiol + Progesterone
(Systemic)
Ovulation + Cycle
(Target outcome)
🎯 GLP-1 (PCOS)

🛑 What disrupts the axis?

  • Chronic stress → elevated cortisol suppresses kisspeptin neurons
  • Low body weight / negative energy balance → leptin & insulin fall, signaling reproductive shutdown
  • PCOS → insulin excess creates upstream androgen overproduction
  • Endometriosis → systemic inflammation dysregulates feedback loops

💊 Where peptides intervene

  • Kisspeptin-10 → directly restores GnRH pulsatility at the apex
  • GLP-1/GIP agonists → reduce insulin resistance driving PCOS androgen excess
  • Selank → normalizes HPA cortisol reactivity protecting kisspeptin neurons
  • BPC-157 → repairs gut-immune axis feeding systemic inflammation

📊 Clinical outcomes

  • Kisspeptin: ovulation restored in hypothalamic amenorrhea Phase II trials
  • GLP-1RA in PCOS: 40–60% of anovulatory patients restore ovulatory cycles
  • Semaglutide PCOS: 17.1% age-standardized incidence by 2025
  • HRT + tirzepatide: 35% greater weight loss than tirzepatide alone (Mayo 2026)
Research Database

Women's Health Peptide Profiles

Research profiles for 9 compounds spanning FDA-approved treatments, clinical-stage candidates, and research-phase peptides addressing the full spectrum of women's hormonal health.

🌸

Kisspeptin-10

The HPG axis master switch

Clinical Trials
Neuropeptide / GnRH Regulator
Kisspeptin is the master upstream regulator of the hypothalamic-pituitary-gonadal (HPG) axis. It binds KISS1R receptors on GnRH neurons, triggering pulsatile GnRH release, which in turn drives LH and FSH secretion from the pituitary — the hormones that control ovulation, estradiol production, and the entire female reproductive cycle. In women with hypothalamic amenorrhea (loss of period due to stress, over-exercise, or low energy availability), kisspeptin signaling is suppressed. Research at Imperial College London shows kisspeptin-54 and kisspeptin-10 administration restores LH pulses and can trigger ovulation in these women.
💗

PT-141 (Bremelanotide)

Vyleesi® — FDA-approved for HSDD

FDA Approved
Melanocortin Receptor Agonist
PT-141 is a cyclic heptapeptide melanocortin receptor agonist (MC3R and MC4R) that acts centrally in the hypothalamus and limbic system to increase sexual desire — unlike PDE5 inhibitors which work peripherally. It activates dopaminergic reward pathways and reduces activity in the medial prefrontal cortex (an area associated with sexual inhibition). It was FDA-approved in 2019 as Vyleesi® for premenopausal women with hypoactive sexual desire disorder (HSDD) — the first non-hormonal, centrally-acting drug approved for female sexual dysfunction.
🛡️

BPC-157

Body Protection Compound — gut-hormonal axis

Research Only
Gastric Pentadecapeptide
BPC-157 modulates the gut-brain-hormonal axis through nitric oxide synthesis upregulation, VEGF receptor activation, and NF-κB suppression. In women, these pathways are particularly relevant: gut permeability (‘leaky gut’) drives systemic inflammation that disrupts HPG axis function, impairs insulin sensitivity in PCOS, and exacerbates the inflammatory component of endometriosis. BPC-157 restores intestinal tight junctions, reduces mesenteric and systemic inflammation, and shows regulatory effects on dopamine and serotonin pathways — neurotransmitters central to mood, pain perception (dysmenorrhea), and stress-induced cycle disruption.
🤝

Oxytocin

The bonding hormone — intimacy & stress modulator

FDA Approved
Hypothalamic Neuropeptide / Neurohormone
Oxytocin is a nine-amino-acid neuropeptide produced in the hypothalamic paraventricular nucleus and released from the posterior pituitary. In women, it mediates uterine contractions during labor, milk letdown during breastfeeding, pair bonding, social trust, and sexual arousal facilitation. Intranasal oxytocin bypasses the blood-brain barrier limitation of systemic delivery, directly modulating amygdala reactivity (reducing fear/anxiety responses), enhancing limbic reward system activation, and reducing cortisol stress responses. Research supports its role in HSDD, postpartum mood disorders, PTSD, and social anxiety — all disproportionately affecting women.

CJC-1295 + Ipamorelin

GH pulse restoration — metabolic & hormonal support

Research Only
GHRH Analogue + GHRP
CJC-1295 (a GHRH analogue) and Ipamorelin (a selective ghrelin receptor agonist) synergistically amplify pulsatile growth hormone secretion from the pituitary without suppressing natural GH feedback. In women, GH amplitude declines dramatically post-menopause (by ~70–80%), contributing to visceral fat accumulation, reduced bone density, impaired lean mass maintenance, and decreased IGF-1-dependent cellular repair. This combination restores youthful GH pulsatility, improving body composition, supporting thyroid and adrenal axis health indirectly via IGF-1 signaling, and potentially reducing menopausal metabolic disruption.
🧘

Selank

Anxiolytic neuropeptide — cortisol & cycle protection

FDA Approved
Synthetic Tuftsin Analogue / Anxiolytic Peptide
Selank (Тофизопам-like profile) is a synthetic heptapeptide analogue of tuftsin that modulates GABA-A receptor activity, increases BDNF expression, and normalizes the HPA axis (hypothalamic-pituitary-adrenal) cortisol stress response. In women, chronic HPA axis hyperactivation — from work stress, trauma, or autoimmune dysregulation — directly suppresses GnRH pulsatility, causing cycle irregularity, amenorrhea, and exacerbating perimenopausal symptoms. Selank reduces cortisol reactivity, improves serotonergic and dopaminergic tone, and enhances IL-6/TNF-α regulation without sedation or dependence risk.

GHK-Cu

Copper peptide — skin, hair & anti-inflammatory beauty

Research Only
Copper-Binding Tripeptide
GHK-Cu (glycine-histidine-lysine + copper) is the most clinically studied topical peptide for women’s aesthetic and systemic health goals. It activates over 4,000 human genes and modulates 31+ anti-inflammatory pathways. It stimulates collagen I, III, VI, decorin, and elastin synthesis while inhibiting collagen-degrading matrix metalloproteinases (MMP-1, -2, -3). Post-menopause, estrogen decline causes 30% of dermal collagen loss within 5 years — GHK-Cu directly compensates at the gene-expression level. Systemically, GHK-Cu reduces TGF-β1 and IL-6, relevant to inflammation-driven hormonal disruption, and shows BDNF-mimetic neurological effects.

Epithalon

Pineal tetrapeptide — telomere & menopausal longevity

Research Only
Synthetic Tetrapeptide / Pineal Bioregulator
Epithalon (Ala-Glu-Asp-Gly) is a synthetic tetrapeptide analogue of epithalamin, the natural pineal gland bioregulator. It activates telomerase (the enzyme that maintains telomere length) in lymphocytes and epithelial cells, restores circadian melatonin rhythm disrupted by aging and stress, and stimulates pineal function relevant to the photoperiodic hormonal cycle in women. Post-menopause, telomere attrition in granulosa cells and endometrial tissue contributes to ovarian decline and tissue aging. Epithalon also reduces oxidative stress via superoxide dismutase upregulation and has shown immunorestoration effects in long-term clinical trials.
🔄

Semaglutide / Tirzepatide

GLP-1/GIP agonists — PCOS & metabolic restoration

FDA Approved
GLP-1/GIP Receptor Agonist
GLP-1 receptor agonists have emerged as a paradigm shift in PCOS management — the most common endocrine disorder in women of reproductive age (affecting 10–15% globally). In PCOS, insulin resistance drives hyperinsulinemia, which stimulates ovarian theca cells to overproduce androgens (testosterone, DHEA-S), suppressing ovulation and causing anovulatory infertility, hirsutism, and acne. GLP-1/GIP agonists reduce insulin resistance directly, lowering androgen levels, restoring menstrual regularity, and improving ovulatory function. Multiple 2025–2026 trials confirm 35–40% greater weight loss in PCOS women on tirzepatide vs controls, with restoration of ovulatory cycles in 40–60% of previously anovulatory patients.
🌸

Kisspeptin-10

The HPG axis master switch

Clinical Trials
Neuropeptide / GnRH Regulator
Kisspeptin is the master upstream regulator of the hypothalamic-pituitary-gonadal (HPG) axis. It binds KISS1R receptors on GnRH neurons, triggering pulsatile GnRH release, which in turn drives LH and FSH secretion from the pituitary — the hormones that control ovulation, estradiol production, and the entire female reproductive cycle. In women with hypothalamic amenorrhea (loss of period due to stress, over-exercise, or low energy availability), kisspeptin signaling is suppressed. Research at Imperial College London shows kisspeptin-54 and kisspeptin-10 administration restores LH pulses and can trigger ovulation in these women.
🛡️

BPC-157

Body Protection Compound — gut-hormonal axis

Research Only
Gastric Pentadecapeptide
BPC-157 modulates the gut-brain-hormonal axis through nitric oxide synthesis upregulation, VEGF receptor activation, and NF-κB suppression. In women, these pathways are particularly relevant: gut permeability (‘leaky gut’) drives systemic inflammation that disrupts HPG axis function, impairs insulin sensitivity in PCOS, and exacerbates the inflammatory component of endometriosis. BPC-157 restores intestinal tight junctions, reduces mesenteric and systemic inflammation, and shows regulatory effects on dopamine and serotonin pathways — neurotransmitters central to mood, pain perception (dysmenorrhea), and stress-induced cycle disruption.
🤝

Oxytocin

The bonding hormone — intimacy & stress modulator

FDA Approved
Hypothalamic Neuropeptide / Neurohormone
Oxytocin is a nine-amino-acid neuropeptide produced in the hypothalamic paraventricular nucleus and released from the posterior pituitary. In women, it mediates uterine contractions during labor, milk letdown during breastfeeding, pair bonding, social trust, and sexual arousal facilitation. Intranasal oxytocin bypasses the blood-brain barrier limitation of systemic delivery, directly modulating amygdala reactivity (reducing fear/anxiety responses), enhancing limbic reward system activation, and reducing cortisol stress responses. Research supports its role in HSDD, postpartum mood disorders, PTSD, and social anxiety — all disproportionately affecting women.

CJC-1295 + Ipamorelin

GH pulse restoration — metabolic & hormonal support

Research Only
GHRH Analogue + GHRP
CJC-1295 (a GHRH analogue) and Ipamorelin (a selective ghrelin receptor agonist) synergistically amplify pulsatile growth hormone secretion from the pituitary without suppressing natural GH feedback. In women, GH amplitude declines dramatically post-menopause (by ~70–80%), contributing to visceral fat accumulation, reduced bone density, impaired lean mass maintenance, and decreased IGF-1-dependent cellular repair. This combination restores youthful GH pulsatility, improving body composition, supporting thyroid and adrenal axis health indirectly via IGF-1 signaling, and potentially reducing menopausal metabolic disruption.
🧘

Selank

Anxiolytic neuropeptide — cortisol & cycle protection

FDA Approved
Synthetic Tuftsin Analogue / Anxiolytic Peptide
Selank (Тофизопам-like profile) is a synthetic heptapeptide analogue of tuftsin that modulates GABA-A receptor activity, increases BDNF expression, and normalizes the HPA axis (hypothalamic-pituitary-adrenal) cortisol stress response. In women, chronic HPA axis hyperactivation — from work stress, trauma, or autoimmune dysregulation — directly suppresses GnRH pulsatility, causing cycle irregularity, amenorrhea, and exacerbating perimenopausal symptoms. Selank reduces cortisol reactivity, improves serotonergic and dopaminergic tone, and enhances IL-6/TNF-α regulation without sedation or dependence risk.

Epithalon

Pineal tetrapeptide — telomere & menopausal longevity

Research Only
Synthetic Tetrapeptide / Pineal Bioregulator
Epithalon (Ala-Glu-Asp-Gly) is a synthetic tetrapeptide analogue of epithalamin, the natural pineal gland bioregulator. It activates telomerase (the enzyme that maintains telomere length) in lymphocytes and epithelial cells, restores circadian melatonin rhythm disrupted by aging and stress, and stimulates pineal function relevant to the photoperiodic hormonal cycle in women. Post-menopause, telomere attrition in granulosa cells and endometrial tissue contributes to ovarian decline and tissue aging. Epithalon also reduces oxidative stress via superoxide dismutase upregulation and has shown immunorestoration effects in long-term clinical trials.
🔄

Semaglutide / Tirzepatide

GLP-1/GIP agonists — PCOS & metabolic restoration

FDA Approved
GLP-1/GIP Receptor Agonist
GLP-1 receptor agonists have emerged as a paradigm shift in PCOS management — the most common endocrine disorder in women of reproductive age (affecting 10–15% globally). In PCOS, insulin resistance drives hyperinsulinemia, which stimulates ovarian theca cells to overproduce androgens (testosterone, DHEA-S), suppressing ovulation and causing anovulatory infertility, hirsutism, and acne. GLP-1/GIP agonists reduce insulin resistance directly, lowering androgen levels, restoring menstrual regularity, and improving ovulatory function. Multiple 2025–2026 trials confirm 35–40% greater weight loss in PCOS women on tirzepatide vs controls, with restoration of ovulatory cycles in 40–60% of previously anovulatory patients.
🌸

Kisspeptin-10

The HPG axis master switch

Clinical Trials
Neuropeptide / GnRH Regulator
Kisspeptin is the master upstream regulator of the hypothalamic-pituitary-gonadal (HPG) axis. It binds KISS1R receptors on GnRH neurons, triggering pulsatile GnRH release, which in turn drives LH and FSH secretion from the pituitary — the hormones that control ovulation, estradiol production, and the entire female reproductive cycle. In women with hypothalamic amenorrhea (loss of period due to stress, over-exercise, or low energy availability), kisspeptin signaling is suppressed. Research at Imperial College London shows kisspeptin-54 and kisspeptin-10 administration restores LH pulses and can trigger ovulation in these women.

CJC-1295 + Ipamorelin

GH pulse restoration — metabolic & hormonal support

Research Only
GHRH Analogue + GHRP
CJC-1295 (a GHRH analogue) and Ipamorelin (a selective ghrelin receptor agonist) synergistically amplify pulsatile growth hormone secretion from the pituitary without suppressing natural GH feedback. In women, GH amplitude declines dramatically post-menopause (by ~70–80%), contributing to visceral fat accumulation, reduced bone density, impaired lean mass maintenance, and decreased IGF-1-dependent cellular repair. This combination restores youthful GH pulsatility, improving body composition, supporting thyroid and adrenal axis health indirectly via IGF-1 signaling, and potentially reducing menopausal metabolic disruption.

Epithalon

Pineal tetrapeptide — telomere & menopausal longevity

Research Only
Synthetic Tetrapeptide / Pineal Bioregulator
Epithalon (Ala-Glu-Asp-Gly) is a synthetic tetrapeptide analogue of epithalamin, the natural pineal gland bioregulator. It activates telomerase (the enzyme that maintains telomere length) in lymphocytes and epithelial cells, restores circadian melatonin rhythm disrupted by aging and stress, and stimulates pineal function relevant to the photoperiodic hormonal cycle in women. Post-menopause, telomere attrition in granulosa cells and endometrial tissue contributes to ovarian decline and tissue aging. Epithalon also reduces oxidative stress via superoxide dismutase upregulation and has shown immunorestoration effects in long-term clinical trials.
🔄

Semaglutide / Tirzepatide

GLP-1/GIP agonists — PCOS & metabolic restoration

FDA Approved
GLP-1/GIP Receptor Agonist
GLP-1 receptor agonists have emerged as a paradigm shift in PCOS management — the most common endocrine disorder in women of reproductive age (affecting 10–15% globally). In PCOS, insulin resistance drives hyperinsulinemia, which stimulates ovarian theca cells to overproduce androgens (testosterone, DHEA-S), suppressing ovulation and causing anovulatory infertility, hirsutism, and acne. GLP-1/GIP agonists reduce insulin resistance directly, lowering androgen levels, restoring menstrual regularity, and improving ovulatory function. Multiple 2025–2026 trials confirm 35–40% greater weight loss in PCOS women on tirzepatide vs controls, with restoration of ovulatory cycles in 40–60% of previously anovulatory patients.
🌸

Kisspeptin-10

The HPG axis master switch

Clinical Trials
Neuropeptide / GnRH Regulator
Kisspeptin is the master upstream regulator of the hypothalamic-pituitary-gonadal (HPG) axis. It binds KISS1R receptors on GnRH neurons, triggering pulsatile GnRH release, which in turn drives LH and FSH secretion from the pituitary — the hormones that control ovulation, estradiol production, and the entire female reproductive cycle. In women with hypothalamic amenorrhea (loss of period due to stress, over-exercise, or low energy availability), kisspeptin signaling is suppressed. Research at Imperial College London shows kisspeptin-54 and kisspeptin-10 administration restores LH pulses and can trigger ovulation in these women.
💗

PT-141 (Bremelanotide)

Vyleesi® — FDA-approved for HSDD

FDA Approved
Melanocortin Receptor Agonist
PT-141 is a cyclic heptapeptide melanocortin receptor agonist (MC3R and MC4R) that acts centrally in the hypothalamus and limbic system to increase sexual desire — unlike PDE5 inhibitors which work peripherally. It activates dopaminergic reward pathways and reduces activity in the medial prefrontal cortex (an area associated with sexual inhibition). It was FDA-approved in 2019 as Vyleesi® for premenopausal women with hypoactive sexual desire disorder (HSDD) — the first non-hormonal, centrally-acting drug approved for female sexual dysfunction.
🤝

Oxytocin

The bonding hormone — intimacy & stress modulator

FDA Approved
Hypothalamic Neuropeptide / Neurohormone
Oxytocin is a nine-amino-acid neuropeptide produced in the hypothalamic paraventricular nucleus and released from the posterior pituitary. In women, it mediates uterine contractions during labor, milk letdown during breastfeeding, pair bonding, social trust, and sexual arousal facilitation. Intranasal oxytocin bypasses the blood-brain barrier limitation of systemic delivery, directly modulating amygdala reactivity (reducing fear/anxiety responses), enhancing limbic reward system activation, and reducing cortisol stress responses. Research supports its role in HSDD, postpartum mood disorders, PTSD, and social anxiety — all disproportionately affecting women.
🛡️

BPC-157

Body Protection Compound — gut-hormonal axis

Research Only
Gastric Pentadecapeptide
BPC-157 modulates the gut-brain-hormonal axis through nitric oxide synthesis upregulation, VEGF receptor activation, and NF-κB suppression. In women, these pathways are particularly relevant: gut permeability (‘leaky gut’) drives systemic inflammation that disrupts HPG axis function, impairs insulin sensitivity in PCOS, and exacerbates the inflammatory component of endometriosis. BPC-157 restores intestinal tight junctions, reduces mesenteric and systemic inflammation, and shows regulatory effects on dopamine and serotonin pathways — neurotransmitters central to mood, pain perception (dysmenorrhea), and stress-induced cycle disruption.

CJC-1295 + Ipamorelin

GH pulse restoration — metabolic & hormonal support

Research Only
GHRH Analogue + GHRP
CJC-1295 (a GHRH analogue) and Ipamorelin (a selective ghrelin receptor agonist) synergistically amplify pulsatile growth hormone secretion from the pituitary without suppressing natural GH feedback. In women, GH amplitude declines dramatically post-menopause (by ~70–80%), contributing to visceral fat accumulation, reduced bone density, impaired lean mass maintenance, and decreased IGF-1-dependent cellular repair. This combination restores youthful GH pulsatility, improving body composition, supporting thyroid and adrenal axis health indirectly via IGF-1 signaling, and potentially reducing menopausal metabolic disruption.
🔄

Semaglutide / Tirzepatide

GLP-1/GIP agonists — PCOS & metabolic restoration

FDA Approved
GLP-1/GIP Receptor Agonist
GLP-1 receptor agonists have emerged as a paradigm shift in PCOS management — the most common endocrine disorder in women of reproductive age (affecting 10–15% globally). In PCOS, insulin resistance drives hyperinsulinemia, which stimulates ovarian theca cells to overproduce androgens (testosterone, DHEA-S), suppressing ovulation and causing anovulatory infertility, hirsutism, and acne. GLP-1/GIP agonists reduce insulin resistance directly, lowering androgen levels, restoring menstrual regularity, and improving ovulatory function. Multiple 2025–2026 trials confirm 35–40% greater weight loss in PCOS women on tirzepatide vs controls, with restoration of ovulatory cycles in 40–60% of previously anovulatory patients.
🛡️

BPC-157

Body Protection Compound — gut-hormonal axis

Research Only
Gastric Pentadecapeptide
BPC-157 modulates the gut-brain-hormonal axis through nitric oxide synthesis upregulation, VEGF receptor activation, and NF-κB suppression. In women, these pathways are particularly relevant: gut permeability (‘leaky gut’) drives systemic inflammation that disrupts HPG axis function, impairs insulin sensitivity in PCOS, and exacerbates the inflammatory component of endometriosis. BPC-157 restores intestinal tight junctions, reduces mesenteric and systemic inflammation, and shows regulatory effects on dopamine and serotonin pathways — neurotransmitters central to mood, pain perception (dysmenorrhea), and stress-induced cycle disruption.
🧘

Selank

Anxiolytic neuropeptide — cortisol & cycle protection

FDA Approved
Synthetic Tuftsin Analogue / Anxiolytic Peptide
Selank (Тофизопам-like profile) is a synthetic heptapeptide analogue of tuftsin that modulates GABA-A receptor activity, increases BDNF expression, and normalizes the HPA axis (hypothalamic-pituitary-adrenal) cortisol stress response. In women, chronic HPA axis hyperactivation — from work stress, trauma, or autoimmune dysregulation — directly suppresses GnRH pulsatility, causing cycle irregularity, amenorrhea, and exacerbating perimenopausal symptoms. Selank reduces cortisol reactivity, improves serotonergic and dopaminergic tone, and enhances IL-6/TNF-α regulation without sedation or dependence risk.

GHK-Cu

Copper peptide — skin, hair & anti-inflammatory beauty

Research Only
Copper-Binding Tripeptide
GHK-Cu (glycine-histidine-lysine + copper) is the most clinically studied topical peptide for women’s aesthetic and systemic health goals. It activates over 4,000 human genes and modulates 31+ anti-inflammatory pathways. It stimulates collagen I, III, VI, decorin, and elastin synthesis while inhibiting collagen-degrading matrix metalloproteinases (MMP-1, -2, -3). Post-menopause, estrogen decline causes 30% of dermal collagen loss within 5 years — GHK-Cu directly compensates at the gene-expression level. Systemically, GHK-Cu reduces TGF-β1 and IL-6, relevant to inflammation-driven hormonal disruption, and shows BDNF-mimetic neurological effects.

Epithalon

Pineal tetrapeptide — telomere & menopausal longevity

Research Only
Synthetic Tetrapeptide / Pineal Bioregulator
Epithalon (Ala-Glu-Asp-Gly) is a synthetic tetrapeptide analogue of epithalamin, the natural pineal gland bioregulator. It activates telomerase (the enzyme that maintains telomere length) in lymphocytes and epithelial cells, restores circadian melatonin rhythm disrupted by aging and stress, and stimulates pineal function relevant to the photoperiodic hormonal cycle in women. Post-menopause, telomere attrition in granulosa cells and endometrial tissue contributes to ovarian decline and tissue aging. Epithalon also reduces oxidative stress via superoxide dismutase upregulation and has shown immunorestoration effects in long-term clinical trials.

GHK-Cu

Copper peptide — skin, hair & anti-inflammatory beauty

Research Only
Copper-Binding Tripeptide
GHK-Cu (glycine-histidine-lysine + copper) is the most clinically studied topical peptide for women’s aesthetic and systemic health goals. It activates over 4,000 human genes and modulates 31+ anti-inflammatory pathways. It stimulates collagen I, III, VI, decorin, and elastin synthesis while inhibiting collagen-degrading matrix metalloproteinases (MMP-1, -2, -3). Post-menopause, estrogen decline causes 30% of dermal collagen loss within 5 years — GHK-Cu directly compensates at the gene-expression level. Systemically, GHK-Cu reduces TGF-β1 and IL-6, relevant to inflammation-driven hormonal disruption, and shows BDNF-mimetic neurological effects.
💗

PT-141 (Bremelanotide)

Vyleesi® — FDA-approved for HSDD

FDA Approved
Melanocortin Receptor Agonist
PT-141 is a cyclic heptapeptide melanocortin receptor agonist (MC3R and MC4R) that acts centrally in the hypothalamus and limbic system to increase sexual desire — unlike PDE5 inhibitors which work peripherally. It activates dopaminergic reward pathways and reduces activity in the medial prefrontal cortex (an area associated with sexual inhibition). It was FDA-approved in 2019 as Vyleesi® for premenopausal women with hypoactive sexual desire disorder (HSDD) — the first non-hormonal, centrally-acting drug approved for female sexual dysfunction.
🤝

Oxytocin

The bonding hormone — intimacy & stress modulator

FDA Approved
Hypothalamic Neuropeptide / Neurohormone
Oxytocin is a nine-amino-acid neuropeptide produced in the hypothalamic paraventricular nucleus and released from the posterior pituitary. In women, it mediates uterine contractions during labor, milk letdown during breastfeeding, pair bonding, social trust, and sexual arousal facilitation. Intranasal oxytocin bypasses the blood-brain barrier limitation of systemic delivery, directly modulating amygdala reactivity (reducing fear/anxiety responses), enhancing limbic reward system activation, and reducing cortisol stress responses. Research supports its role in HSDD, postpartum mood disorders, PTSD, and social anxiety — all disproportionately affecting women.
🧘

Selank

Anxiolytic neuropeptide — cortisol & cycle protection

FDA Approved
Synthetic Tuftsin Analogue / Anxiolytic Peptide
Selank (Тофизопам-like profile) is a synthetic heptapeptide analogue of tuftsin that modulates GABA-A receptor activity, increases BDNF expression, and normalizes the HPA axis (hypothalamic-pituitary-adrenal) cortisol stress response. In women, chronic HPA axis hyperactivation — from work stress, trauma, or autoimmune dysregulation — directly suppresses GnRH pulsatility, causing cycle irregularity, amenorrhea, and exacerbating perimenopausal symptoms. Selank reduces cortisol reactivity, improves serotonergic and dopaminergic tone, and enhances IL-6/TNF-α regulation without sedation or dependence risk.

GHK-Cu

Copper peptide — skin, hair & anti-inflammatory beauty

Research Only
Copper-Binding Tripeptide
GHK-Cu (glycine-histidine-lysine + copper) is the most clinically studied topical peptide for women’s aesthetic and systemic health goals. It activates over 4,000 human genes and modulates 31+ anti-inflammatory pathways. It stimulates collagen I, III, VI, decorin, and elastin synthesis while inhibiting collagen-degrading matrix metalloproteinases (MMP-1, -2, -3). Post-menopause, estrogen decline causes 30% of dermal collagen loss within 5 years — GHK-Cu directly compensates at the gene-expression level. Systemically, GHK-Cu reduces TGF-β1 and IL-6, relevant to inflammation-driven hormonal disruption, and shows BDNF-mimetic neurological effects.
By the Numbers

Data Visualizations

Hormonal decline trajectories, research evidence strength, and peptide target coverage — visualized.

Hormonal Decline Across the Female Lifecycle

Indexed to age 20s = 100%. Estrogen, progesterone, GH amplitude, and dermal collagen all decline with age — each driving distinct symptoms that peptides can target.

EstrogenProgesteroneGH AmplitudeDermal Collagen
  • Estrogen %
  • Progesterone %
  • GH Amplitude %
  • Collagen %
⚠️ Indicative trends from published research. Individual variation is high. Menopausal transition (typically 48–55) drives the steepest declines.

Research Evidence Strength by Compound

Human trial, animal study, and mechanistic evidence scores (0–100). GLP-1 agonists and PT-141 lead on human data; kisspeptin leads on mechanism clarity.

Human TrialsAnimal StudiesMechanistic Data
```
⚠️ Evidence scores are editorial assessments based on published literature. Not a clinical recommendation.

Peptide Target Coverage Map

Which peptide addresses which women’s health target? Green = strong evidence, Yellow = emerging.
CompoundHormonalFertilityMenopauseLibidoPCOSAnti-Inflam.CollagenMood
GLP-1/GIP⚠️⚠️⚠️
PT-141⚠️
Oxytocin⚠️
Kisspeptin-10⚠️
CJC+Ipa⚠️⚠️
GHK-Cu⚠️⚠️
Selank⚠️
BPC-157⚠️⚠️
Epithalon⚠️
✅ Strong evidence   ⚠️ Emerging/limited   ❌ Not applicable

The Research Gap

Women's health R&D funding6%

of total pharma R&D (WEF 2026)

Female representation in trials38%

in pre-2000 clinical studies

Male-female dosing parity22%

of drugs have sex-specific dosing

The opportunity: Women live longer than men but spend more years in poor health. Closing the research and treatment gap in women’s health is one of the highest-impact areas in modern medicine. Peptide science is accelerating this progress.

History of Science

Women's Health Peptide Research Timeline

From oxytocin's 1953 synthesis to the 2019 FDA approval of PT-141 — seven decades of science addressing women's most underserved health needs.

🧬
1953

Oxytocin becomes first peptide hormone to be sequenced and synthesized — by Vincent du Vigneaud, earning the 1955 Nobel Prize. First clinical use as Pitocin® for labor induction.

🔬
1984

GHK-Cu (glycine-histidine-lysine copper complex) isolated from human plasma by Loren Pickart. Initial research focuses on wound healing and liver regeneration.

🌸
1996

Kisspeptin gene (KISS1) identified as a metastasis suppressor. Its central role in reproductive axis regulation not yet recognized.

💡
2003

Kisspeptin identified as the endogenous ligand for GPR54 (now KISS1R). Two independent research groups (UK/US) simultaneously discover its critical role in triggering puberty and LH secretion — a paradigm shift in reproductive endocrinology.

🌡️
2005

KISS1R loss-of-function mutations confirmed to cause idiopathic hypogonadotropic hypogonadism — establishing kisspeptin as the essential gatekeeper of the HPG axis.

💗
2008

PT-141 (bremelanotide) completes Phase II trials demonstrating central activation of desire in women with HSDD — the first peptide to target CNS sexual circuits rather than peripheral vascular mechanisms.

🔄
2012

First GLP-1 agonist (liraglutide) shows significant androgen reduction and menstrual cycle restoration in PCOS women — opening the GLP-1 era in female metabolic and reproductive health.

📊
2015

Imperial College London Phase I/II: kisspeptin-54 and kisspeptin-10 successfully trigger ovulation in women with hypothalamic amenorrhea — proof-of-concept for peptide-based fertility restoration.

2019

PT-141 (bremelanotide / Vyleesi®) FDA-approved for premenopausal HSDD — first non-hormonal, centrally-acting drug approved for female sexual dysfunction in the US.

🧪
2022

Tirzepatide Phase III SURMOUNT-1 data: 22.5% body weight reduction in women with obesity — highest efficacy data for any peptide in female metabolic health. PCOS subset analyses show dramatic androgen reduction.

📈
2025

GLP-1/GIP agonist use in PCOS rises 7-fold (2021–2025). Mayo Clinic data: HRT + tirzepatide combination produces 35% greater weight loss in postmenopausal women vs tirzepatide alone.

🚀
2026+

Emerging frontiers: kisspeptin antagonists for endometriosis; GLP-1 + kisspeptin combinations for PCOS fertility; Epithalon / GHK-Cu in perimenopausal longevity protocols; intranasal oxytocin for postpartum depression FDA review.

Common Questions

Frequently Asked Questions

Expert answers on women's health peptides, PCOS, menopause, and the science behind the treatments.

GLP-1/GIP receptor agonists (semaglutide, tirzepatide) have the strongest and most consistent evidence for PCOS. They directly reduce insulin resistance — the root driver of androgen excess in PCOS — restoring menstrual cycles, reducing testosterone/DHEA-S, and improving ovulatory function. Clinical data (2024–2025) shows GLP-1RA use in PCOS increased 7-fold in 4 years, with 40–60% of previously anovulatory PCOS patients restoring ovulatory cycles. Kisspeptin-10 is promising for the subset of PCOS with hypothalamic dysfunction, and BPC-157 addresses the gut-inflammation axis that worsens insulin resistance. All require physician supervision — especially given the contraindication of GLP-1 agonists in pregnancy.

The HPG (hypothalamic-pituitary-gonadal) axis operates as a precise pulse generator. The hypothalamus releases GnRH in pulses (the frequency determines whether LH or FSH is preferentially stimulated), driven by kisspeptin neurons. Low kisspeptin = GnRH pulses stop = LH/FSH drop = estradiol and progesterone collapse = cycle stops.

The three most common disruptors in reproductive-age women are:
(1) chronic stress — elevated cortisol directly suppresses kisspeptin and GnRH neurons (functional hypothalamic amenorrhea);
(2) low body weight or negative energy balance — leptin and insulin fall, signaling reproductive shutdown;
(3) PCOS — where insulin excess creates a different type of HPG dysregulation.

Selank and BPC-157 address the stress axis; GLP-1 agonists address the insulin-driven PCOS pattern; kisspeptin directly restores the pulse generator.

No — there are two FDA-approved pharmacological options for HSDD in women:

(1) Addyi® (flibanserin) — approved 2015, a daily oral 5-HT1A agonist / 5-HT2A antagonist that increases dopamine and norepinephrine in the prefrontal cortex; and

(2) Vyleesi® (bremelanotide / PT-141) — approved 2019, a subcutaneous melanocortin agonist used on-demand.

They work by completely different mechanisms. Addyi requires daily dosing and cannot be combined with alcohol; PT-141 is used 45 minutes before activity. PT-141 is generally preferred for its on-demand profile and faster onset, but has a higher nausea burden. Both are for premenopausal women specifically, and neither addresses the root hormonal causes of low desire — making kisspeptin, oxytocin, and hormonal optimization complementary considerations.

GH secretion declines dramatically with age — by approximately 14% per decade in women after 30 — and the menopause transition accelerates this decline. By age 60, most women have 70–80% less GH pulse amplitude than at age 30.

This matters because GH/IGF-1 drives lean mass maintenance, bone density, dermal collagen synthesis, fat metabolism (especially visceral fat clearance), and cellular repair.

CJC-1295 + Ipamorelin restores youthful GH pulsatility by stimulating the pituitary’s own GH release — rather than replacing GH externally (which suppresses natural production).

For post-menopausal women, this combination is studied alongside HRT as a way to address the metabolic and aesthetic consequences of hormonal decline without the risks of supraphysiological exogenous HGH.

Peptides and HRT address different biological targets and can be complementary rather than competing. HRT (estrogen, progesterone, sometimes testosterone) replaces the depleted hormones directly — addressing vasomotor symptoms, bone loss, cardiovascular risk, and cognitive protection.

Peptides work upstream or in parallel: GLP-1 agonists improve insulin sensitivity (making HRT more effective metabolically); CJC-1295 + Ipamorelin restores the GH axis that HRT doesn't address; GHK-Cu provides direct dermal collagen support beyond what estrogen restoration alone can achieve; Selank and oxytocin address the neurological and stress dimensions of menopause.

The Mayo Clinic 2026 data showing 35% greater weight loss with tirzepatide + HRT vs tirzepatide alone suggests meaningful synergy. However, all combinations require physician oversight — hormone-peptide interactions are complex and individual responses vary significantly.

Epithalon has a favorable safety profile across multiple long-term human studies — primarily Khavinson et al.'s research in elderly populations. No serious adverse events have been reported in published clinical data. The mechanistic evidence (telomerase activation in lymphocytes and epithelial cells, melatonin rhythm restoration, antioxidant gene upregulation) is compelling.

For women specifically, the most relevant effects are:
(1) restoration of circadian melatonin rhythm — particularly important for perimenopausal sleep disruption, which accelerates biological aging;
(2) telomere preservation in ovarian and endometrial cells, potentially slowing reproductive aging; and
(3) immune restoration.

The key caveat: most human data comes from Russian studies that haven't been independently replicated in large-scale Western RCTs. It should be approached as a promising longevity compound with strong preclinical data and preliminary positive human signals, not as a proven therapeutic.

Legal & FDA Disclaimers

Women's hormonal health is complex, highly individual, and carries specific risks. Please read this carefully.

Educational Content Only

All content on this page is for educational and informational purposes. Nothing here constitutes medical advice, diagnosis, or treatment recommendations. Women's hormonal conditions require individual evaluation by a qualified physician, gynecologist, or reproductive endocrinologist.

FDA Status Summary

FDA-approved: Oxytocin (Pitocin®, injectable), PT-141 (Vyleesi®), Semaglutide (Ozempic®, Wegovy®), Tirzepatide (Mounjaro®, Zepbound®). Clinical trials: Kisspeptin. Research only: BPC-157, GHK-Cu (systemic), Epithalon, Selank (outside Russia), CJC-1295 + Ipamorelin.

Pregnancy & Fertility Warning

GLP-1/GIP agonists (semaglutide, tirzepatide) are CONTRAINDICATED in pregnancy — discontinue at least 2 months before attempting conception. Kisspeptin protocols require specialist fertility clinic supervision. Never attempt to self-manage ovulation induction with peptides — ovarian hyperstimulation syndrome (OHSS) is a life-threatening risk.

Hormonal Interaction Risk

Peptides that affect the HPG axis (kisspeptin, CJC-1295, GHK-Cu) can interact with HRT, oral contraceptives, IVF protocols, and thyroid medications. Always disclose all peptide use to your prescribing physician. Do not combine research peptides with active fertility treatment without specialist oversight.

Full Disclaimer

House of Peptides provides this page for educational awareness of women's health peptide research. All information is for research and educational purposes only. The FDA has not evaluated any claims made about research-phase peptides on this page. PT-141 (Vyleesi®), oxytocin (Pitocin®), and GLP-1/GIP agonists are FDA-approved medications requiring a valid prescription. BPC-157, kisspeptin, CJC-1295, ipamorelin, epithalon, selank, and GHK-Cu (systemic) are not FDA-approved for any therapeutic use in the United States. References to approval in other countries (Russia, etc.) do not imply US legality or safety endorsement. All clinical study data cited reflects published peer-reviewed research as available to early 2026. Individual results vary significantly; published outcomes do not predict individual response. House of Peptides accepts no liability for actions taken based on information on this educational page.

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