CosmeticFDA-Approved

Melanotan IMC1R-selective photoprotector (FDA-approved)

Q: What is the difference between Melanotan I and Melanotan II?

MT-I (afamelanotide) is a linear 13-amino-acid peptide that selectively activates MC1R — skin pigmentation and DNA repair. MT-II is a cyclic 7-amino-acid peptide that activates four of five melanocortin receptors non-selectively, including brain receptors producing appetite suppression and sexual arousal. MT-I is FDA-approved (Scenesse); MT-II has never completed clinical development.

Q: What is Scenesse used for?

Scenesse (afamelanotide) is FDA-approved for increasing pain-free light exposure in adults with erythropoietic protoporphyria (EPP), a rare inherited phototoxicity condition. It's given as a subcutaneous implant every 60 days. Phase III vitiligo trials (CUV105) are enrolling.

Q: Does melanotan cause melanoma?

The weight of evidence indicates MC1R activation is photoprotective, not oncogenic. The Addison's cohort (3,299 patients, 40-year follow-up) shows melanoma incidence below expected, and afamelanotide reports zero melanomas across 1,000+ patients over 10+ years.

Q: What is bremelanotide and how does it relate to melanotan?

Bremelanotide (Vyleesi) derives from the MT-II program — when MT-II unexpectedly produced erections in Phase I, the sexual-arousal mechanism was isolated into an MC4R agonist, FDA-approved in 2019 for hypoactive sexual desire disorder in premenopausal women.

Understand the mechanism, the current regulatory status, and the evidence — then decide your next step with a clinician who knows these compounds. The information below is educational reference only.

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Mechanism

Selective MC1R agonist, eumelanin synthesis activation, DNA repair enhancement

Benefits

UV-independent tanning, Photoprotection, DNA repair support

Typical Dose

0.1-0.25mg

Cycle Length

4 weeks loading, then maintenance

Frequency

Daily (loading) -> 1-2x/week

Stacks With

GHK-Cu

The essentials

At a Glance

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Dosage

16 mg subcutaneous implant every 60 days (physician-administered).

Protocol

Up to 6 implants per year, continuous. Prescribed and implanted by a specialist.

Results timeline

Pigmentation within days, full effect by week 2, persisting weeks beyond implant depletion.

Side effects

Nausea, headache, localised darkening at the implant site — no serious events across 1,000+ patients over 10+ years.

Receptor selectivity

MC1R-selective — skin pigmentation and DNA repair. Does not cross the blood-brain barrier.

Regulatory status

Melanotan I (afamelanotide, brand name Scenesse) is FDA-approved (October 2019) and EMA-authorized (2014) for increasing pain-free light exposure in adults with erythropoietic protoporphyria (EPP). In September 2025 the EMA removed its 4-implant-per-year cap, harmonizing with US labeling for year-round treatment. It holds orphan drug designation, and Phase III trials in vitiligo (CUV105) are actively enrolling, with exploration in photodermatoses and acute stroke. It is administered only as a physician-implanted subcutaneous implant. This is the fully approved, MC1R-selective member of the melanotan pair — in sharp contrast to Melanotan II, which is banned from compounding and illegal to sell.

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Melanotan I and II are two synthetic analogs of alpha-melanocyte-stimulating hormone (alpha-MSH) developed in the same University of Arizona laboratory, with radically different fates. MT-I became afamelanotide (Scenesse) — FDA/EMA-approved for erythropoietic protoporphyria with 10+ years of safety data across 1,000+ patients. The divergence traces to a single structural decision: MT-I is a linear peptide selective for MC1R (the skin-pigmentation receptor), whereas MT-II is a cyclic peptide that activates four of five melanocortin receptor subtypes indiscriminately. MT-I is a single-purpose key; MT-II is a master key that opens doors you may not want opened.

What MT-I Is

Alpha-MSH degrades in minutes, making it impractical as a drug. In 1980, Sawyer, Hruby, and Hadley synthesized a modified version with two changes: norleucine at position 4 (preventing oxidative degradation) and D-phenylalanine at position 7 (increasing receptor binding ~1,000-fold and conferring protease resistance). This linear tridecapeptide — [Nle4, D-Phe7]-alpha-MSH — became Melanotan I, developed clinically as afamelanotide. It preserves the full 13-residue alpha-MSH sequence and retains ~10-fold selectivity for MC1R over other melanocortin receptors. Its linear architecture does not meaningfully cross the blood-brain barrier, which accounts for the absence of CNS effects in clinical use. Neither MT-I nor MT-II activates MC2R (the ACTH/cortisol receptor) — an important safety boundary.

Pharmacokinetics

Parameter	MT-I (16 mg implant)
Tmax	~36 h
Intrinsic half-life	~30 min
Apparent half-life	~15 h (implant-driven flip-flop kinetics)
Cmax	3.7 ng/mL
BBB penetration	Minimal
Duration of effect	Weeks post-depletion

Afamelanotide is a 16 mg bioresorbable subcutaneous implant every 60 days, providing controlled release (median Tmax ~36 h, >90% liberated by day 5, undetectable by day 10). Melanogenic effects persist for weeks beyond detectable drug levels, reflecting epidermal melanin turnover. No late effects reported in volunteers followed 25 years after first exposure.

Receptor Pharmacology

MT-I preferentially activates MC1R on melanocytes, driving eumelanin synthesis (the brown-black pigment that absorbs UV and scavenges reactive oxygen species) and enhancing nucleotide excision repair of UV-induced DNA damage — a photoprotective mechanism independent of pigment production. Loss-of-function MC1R variants (common in fair-skinned populations) are established melanoma risk factors precisely because they impair both eumelanin production and DNA repair. MT-I's limited CNS penetration confines its actions to the periphery.

Clinical Evidence — EPP and Vitiligo

Afamelanotide's EPP program is the most rigorous investigation of any melanocortin agonist: three Phase III RCTs enrolling 244 patients. The pivotal US trial (CUV039, n=93) showed patients spent a median 64.1 hours in pain-free direct sunlight over 180 days vs 40.5 hours for vehicle (P=0.04); the European trial (CUV029, n=74) showed 6.0 vs 0.75 hours pain-free sunlight (P<0.05). Long-term data (Biolcati, 115 patients up to 8 years) documented quality-of-life scores rising from 31% to 74% of maximum. The FDA approved Scenesse in October 2019; the EMA authorized it in 2014 and in September 2025 removed the 4-implant-per-year cap. A Phase II vitiligo trial (n=55) with narrowband UV-B achieved 48.6% repigmentation vs 33.3% with NB-UVB alone; Phase III CUV105 (200+ patients) is enrolling — the first systemic non-immunosuppressive agent trialed for repigmentation. Afamelanotide has also entered a Phase IIa stroke trial (early data n=6: median NIHSS improvement 6 to 2 by day 7).

Safety — The Melanoma Question

The weight of evidence indicates MC1R activation is photoprotective rather than oncogenic. The Addison's disease cohort (3,299 patients with chronic MC1R activation, 40-year follow-up) shows a standardized melanoma incidence ratio of 0.7 — numerically below expected rates. Afamelanotide's program reports zero melanoma events across 1,000+ patients over 10+ years, made more meaningful because many EPP patients substantially increased sun exposure after treatment. Adverse events are predominantly mild: nausea, headache, and localized hyperpigmentation at the implant site. No formal animal carcinogenicity studies have been conducted (a gap acknowledged in the Scenesse FDA label).

The Emerging Melanocortin Frontier

Next-generation agents pursue defined receptor targets through defined routes: bivamelagon (oral MC4R agonist, positive Phase 2 in hypothalamic obesity), PL-8177 (locally acting oral MC1R agonist, Phase 2 in ulcerative colitis), and setmelanotide/Imcivree (MC4R-selective, FDA-approved for genetic obesity). The lesson of MT-I vs MT-II is that receptor selectivity is the difference between a viable therapeutic and an uncontrollable polypharmacological agent — and afamelanotide is the selective, approved end of that spectrum.

Straight answers

Frequently asked

What is the difference between Melanotan I and Melanotan II?

MT-I (afamelanotide) is a linear 13-amino-acid peptide that selectively activates MC1R — skin pigmentation and DNA repair. MT-II is a cyclic 7-amino-acid peptide that activates four of five melanocortin receptors non-selectively, including brain receptors producing appetite suppression and sexual arousal. MT-I is FDA-approved (Scenesse); MT-II has never completed clinical development.

What is Scenesse used for?

Scenesse (afamelanotide) is FDA-approved for increasing pain-free light exposure in adults with erythropoietic protoporphyria (EPP), a rare inherited phototoxicity condition. It's given as a subcutaneous implant every 60 days. Phase III vitiligo trials (CUV105) are enrolling.

Does melanotan cause melanoma?

The weight of evidence indicates MC1R activation is photoprotective, not oncogenic. The Addison's cohort (3,299 patients, 40-year follow-up) shows melanoma incidence below expected, and afamelanotide reports zero melanomas across 1,000+ patients over 10+ years.

What is bremelanotide and how does it relate to melanotan?

Bremelanotide (Vyleesi) derives from the MT-II program — when MT-II unexpectedly produced erections in Phase I, the sexual-arousal mechanism was isolated into an MC4R agonist, FDA-approved in 2019 for hypoactive sexual desire disorder in premenopausal women.

Keep exploring

References

Langendonk JG et al. Afamelanotide for Erythropoietic Protoporphyria. NEJM 2015;373(1):48-59. PMID: 26132941
Biolcati G et al. Long-term observational study of afamelanotide in 115 EPP patients. Br J Dermatol 2015;172(6):1601-1612. PMID: 25494545
Bohm M et al. Benefits and risks of chronic MC1R activation. JEADV 2025;39:39-51. PMID: 39082868
Sawyer TK et al. [Nle4, D-Phe7]-alpha-MSH: a highly potent alpha-melanotropin. PNAS 1980;77(10):5754-5758. PMID: 6777774
Mun Y, Kim W, Shin D. MC1R: pharmacological and therapeutic aspects. Int J Mol Sci 2023;24(15):12152. PMID: 37569558
Minder EI et al. Pharmacokinetics and pharmacodynamics of afamelanotide. Clin Pharmacokinet 2017;56(8):815-823.
Lim HW et al. Afamelanotide and NB-UVB for vitiligo. JAMA Dermatol 2015;151(1):42-50. PMID: 25230094
FDA SCENESSE Label (revised August 2024); FDA NDA 210797 clinical pharmacology review.
Stanislaus V et al. Feasibility and safety of afamelanotide in acute stroke. BMC Neurol 2023;23(1):281.

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