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01 · the file

Melanotan II.

D
Research-use-onlyMelanocortin & sexual-health peptides
DMelanotan IIVerdict: Mostly animal evidenceHuman evidence: limitedStatus: Research-use-onlyReceiptsCalculatorReferences
💡 Explain this simply
What this is

Melanotan II is a research compound in the melanocortin & sexual-health peptides.

Why people care

It draws interest for melanocortin & sexual-health peptides.

What's actually supported

D-tier evidence: human evidence is limited; most support is preclinical.

What's not proven

General anti-aging / longevity; Human injury recovery; Muscle growth or fat loss claims.

What to be cautious about

Interesting on paper, but not a clinically proven option. The internet narrative is stronger than the human evidence.

What to compare next

Before you decide, compare Melanotan II with Pt 141, Kisspeptin, Oxytocin. See all →

Research-onlyAnimal-data heavySafety unclearRegulatory friction highMechanism-first
What it is

Melanotan II is a research compound in the melanocortin & sexual-health peptides.

What it does

Engaging melanocortin receptors, relevant to pigmentation and sexual function.

Why people use it

It draws interest for melanocortin & sexual-health peptides.

Does it work?

D-tier evidence: human evidence is limited; most support is preclinical.

Bottom lineMelanotan II is D-tier: scientifically interesting in preclinical models, but human evidence is minimal and the online narrative tends to run ahead of it.
What the published evidence shows

A synthetic non-selective melanocortin agonist used unapproved for tanning and erectile effects, with no approved medical indication. Documented safety concerns include priapism, nausea/flushing, and changes to moles with melanoma case reports.

[1]Melanotan-induced priapism: a hard-earned tan (case report)BMJ Case Rep, 2019 (PMID 30796078)

Verified citations resolve to PubMed / FDA. See how we score.

Melanotan II: the research file

What it is

Melanotan II (MT-II) is a synthetic, cyclic heptapeptide analog of the natural hormone alpha-melanocyte-stimulating hormone (alpha-MSH). It was developed at the University of Arizona in the late 1980s and 1990s as part of a program designing protease-resistant "superpotent" melanotropins; the related linear analog melanotan I became the approved drug afamelanotide (Scenesse). Unlike afamelanotide, Melanotan II itself was never approved as a medicine and today circulates almost exclusively as an unlicensed product sold online for cosmetic "tanning" and as a libido agent.

How it works

Melanotan II is a non-selective agonist of the melanocortin receptor family, binding MC1R, MC3R, MC4R and MC5R rather than selectively targeting MC1R. Activation of MC1R on cutaneous melanocytes stimulates the cAMP pathway and shifts melanin synthesis toward darker eumelanin, producing skin darkening that, unlike a UV tan, can occur with reduced sun exposure. Its central effects on sexual arousal and appetite are attributed mainly to MC4R (with possible MC3R contribution) in the hypothalamus and related circuits, while nausea, flushing and yawning also arise from this broad central melanocortin activation. The cyclic lactam structure makes it markedly more resistant to enzymatic degradation and more potent and longer-acting than native alpha-MSH.

What the evidence shows

Human data on Melanotan II is limited to small, early-phase academic studies and a large body of case reports; no Phase 2/3 program was ever completed and it has never been tested in large controlled trials. The best-documented human work is on erectile function: a 1998 double-blind, placebo-controlled crossover study in men with psychogenic erectile dysfunction (Wessells et al., J Urol) and a 2000 study in men with organic erectile dysfunction (Urology) reported that subcutaneous Melanotan II initiated erections, accompanied by frequent nausea and yawning. Its tanning rationale rests on MC1R pharmacology and on the broader melanotan development program (Hadley et al., 1998), but rigorous controlled efficacy/safety data for cosmetic tanning in humans is essentially absent. Most contemporary human evidence comes from adverse-event case reports — including systemic toxicity with rhabdomyolysis (Clinical Toxicology, 2012) and dermatologic changes — so claims of benefit substantially outrun the controlled-trial evidence.

Safety considerations

Commonly reported short-term effects in humans include nausea, vomiting, facial flushing, spontaneous yawning and stretching, appetite suppression, darkening of existing moles, and spontaneous erections or priapism in men. More serious documented harms from unregulated use appear in case reports: rhabdomyolysis and systemic toxicity, and a recurring concern about changes to melanocytic naevi (new and darkening moles, atypical naevi) with multiple published cases of melanoma reported in users — though causality has not been established and confounding by concurrent UV/tanning-bed exposure is a major limitation. Because the product is unlicensed and typically self-injected from non-pharmaceutical sources, contamination, mislabeling, dosing errors and sterility problems are additional, poorly quantified risks. This entry intentionally gives no doses or protocols; anyone considering use should consult a clinician, and dermatology bodies advise against use.

Regulatory status

Melanotan II is not approved by the FDA or any major regulator for any indication and is not legally marketed as a medicine; products sold online are unlicensed. Regulators including the US FDA, the UK MHRA and Australia's TGA have issued consumer warnings against it. The distinct linear analog melanotan I (afamelanotide, Scenesse) is separately FDA- and EMA-approved, but only for erythropoietic protoporphyria — not for tanning.

Key facts
  • Synthetic cyclic analog of alpha-MSH; non-selective agonist at MC1R, MC3R, MC4R and MC5R
  • Developed alongside melanotan I (afamelanotide); only afamelanotide gained regulatory approval (for erythropoietic protoporphyria, not tanning)
  • Never completed Phase 2/3 trials; human data limited to small early studies and case reports
  • Unlicensed worldwide for human use; FDA, MHRA and TGA have warned consumers against it
  • Documented effects include nausea, flushing, yawning, appetite loss, priapism, and mole darkening
  • Case reports link unregulated use to rhabdomyolysis and to melanoma, though causality is unproven
Sources
  1. [1]Synthetic melanotropic peptide initiates erections in men with psychogenic erectile dysfunction: double-blind, placebo controlled crossover studyThe Journal of Urology, 1998, PMID 9679884
  2. [2]Effect of an alpha-melanocyte stimulating hormone analog on penile erection and sexual desire in men with organic erectile dysfunctionUrology, 2000, PMID 11018622
  3. [3]Melanotan II injection resulting in systemic toxicity and rhabdomyolysisClinical Toxicology (Philadelphia), 2012, PMID 23121206
  4. [4]Melanotan II (DermNet) — unlicensed alpha-MSH analog: uses, regulatory warnings and adverse effectsDermNet NZ, dermatology reference
Evidence maturity
Anecdote
Mechanism
Animal
Early human
Clinical trials
Approved use

Currently sits at Early humanSome early human evidence exists but isn't definitive.

Online hypeLowvsActual evidenceEarlyGapBalanced

Jargon, decoded: · ·

02 · benefits people research this for

Areas this compound is studied or discussed for — not guaranteed effects.

Libido / sexual health
Evidence: Early human evidence
Status: Research-use-only
Caution: Response, eligibility, and tolerability still vary.
03 · evidence receipts

Marketing claim vs what the data actually shows. Tap a row for detail.

Claim
Verdict
What the data says
Safe way to tan
! Safety caveat
Unapproved; carries notable safety concerns and is not a sanctioned tanning method.
Evidence typeSafety not established

What this does not mean: It doesn't mean it's confirmed safe — long-term human safety is unknown.

Verdicts describe the state of the evidence, not invented study results. Open References for the underlying citations.

0 of 1 claims checked
04 · stack fit

Stack fit

Decision clarity: Unknown

Not enough indexed evidence to assess.

Best fitResearch interest in melanocortin & sexual-health peptides and melanocortin receptor activation.
Not a good fit forAnyone expecting proven human outcomes — the human evidence isn't there yet.
Evidence confidenceLow
Risk profileUnclear
Regulatory frictionHigh
Hype riskMedium

Stack verdict: Interesting on paper, but not a clinically proven option. The internet narrative is stronger than the human evidence.

Not proven for

Melanotan II is not established for:

General anti-aging / longevityHuman injury recoveryMuscle growth or fat loss claimsDisease treatmentAny use as a proven therapy

Tier ranking

D

A weighted evidence score of 38/100 places melanotan-ii in D tier — based on published evidence, not popularity.

Weighted evidence score 38/100

Why not C: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Why not F: supported by mechanism confidence.

What would move it up: Larger controlled human trials, clearer long-term safety, replicated findings, and regulatory progress.

What would move it down: Failed confirmatory trials, new safety signals, or evidence that popular claims don't translate.

Hype vs evidence (shown separately — does not affect the tier)
Internet hype: LowEvidence strength: EarlyRisk of overstatement: Medium
05 · safety / status
Evidence gap alert. Most support comes from animal, cell, or early research — high-quality human clinical evidence is limited.
Regulatory alert. This compound is not FDA-approved for the uses commonly discussed online.
Safety alert. Long-term human safety is not well established. Quality and purity from non-pharmaceutical sources is an additional risk.
Can it legally be used?Research-use-only
EMA / internationalVerify by region
Sport (WADA)Check the current WADA prohibited list
Known side effectsNot well characterized in humans
Biggest unknownsLong-term safety, broad off-label use, rare events
Main cautionResearch-only; human evidence limited; sourcing & purity risk
What we know
  • Melanotan II is not FDA-approved for human use; it is discussed in a research context.
  • It belongs to the Melanocortin & sexual-health peptides class.
  • Its principal mechanism is characterized in the literature.
What we don't know
  • Whether observed effects reliably translate to humans at large.
  • Long-term safety in healthy users, and full drug-interaction risk.
  • Optimal studied parameters outside any approved indication.
  • Claim-by-claim verdicts — these are authored against verified sources and shown when complete.
  • Quality and purity of material from non-pharmaceutical sources.
Caution if you're researching
Pregnancy / fertilityPsychiatric conditionsHormonal therapiesResearch-only compoundsCompetitive sports (anti-doping)Diabetes / glucose regulation

This is not medical advice. These are areas where professional guidance and better evidence matter most.

06 · compare before you decide

See it next to its closest alternatives.

Melanotan II vs Pt 141Melanotan II vs KisspeptinMelanotan II vs OxytocinBuild a comparison →
07 · the read

Full brief

A deeper, chapter-by-chapter research briefing. Tap any chapter to expand.

In this brief
  1. What it is
  2. The Melanocortin receptor activation mechanism
  3. The preclinical evidence lane
  4. Why Preliminary, and not higher or lower
  5. Proven lane vs speculative lane
  6. What people report
  7. Regulatory status
  8. What changed recently
01What it is

Simple takeaway: Melanotan II is a research compound in the melanocortin & sexual-health peptides.

Peptides acting on melanocortin and reproductive-hormone pathways, including an approved agent for a specific indication. It is not approved for human use; it is discussed here in a research context only.

02The Melanocortin receptor activation mechanism

Simple takeaway: Engaging melanocortin receptors, relevant to pigmentation and sexual function.

Melanocortin agonists act on melanocortin receptors. Depending on receptor subtype, effects studied include pigmentation and central pathways relevant to sexual arousal. One agent in this space is approved for a specific indication.

What this does not prove. A characterized mechanism explains how an effect could occur — it does not prove the effect reliably occurs in humans.
03The preclinical evidence lane

Simple takeaway: Support is mainly preclinical; 0 registered trials and 0 sources indexed.

The most defensible evidence comes from animal and mechanistic models. Human clinical evidence is limited.

What this does not prove. Preclinical or early-stage evidence does not establish reliable human outcomes.
04Why Preliminary, and not higher or lower

Simple takeaway: Composite maturity 2.2/5.

What holds it back: human evidence, safety clarity, regulatory clarity, practical relevance. What supports its placement: mechanism confidence. Stronger human trials, clearer long-term safety data, and regulatory progress would move it up; a safety signal or failure to replicate would move it down.

05Proven lane vs speculative lane

Simple takeaway: The research interest is real; most popular claims remain speculative.

What's supported is the preclinical/mechanistic research. What's speculative is the broad human benefit frequently claimed online, which the indexed human evidence does not establish.

06What people report

Simple takeaway: Community reports are not clinical evidence.

Online reports can surface expectation patterns and possible safety signals, but they are shaped by placebo effects, selection bias, confounders, and uncertain product quality and sourcing. We don't treat anecdotes as proof and we don't publish dosing or protocols.

What this does not prove. Anecdotes cannot establish efficacy or safety.
07Regulatory status

Simple takeaway: Research-use-only

Not approved by the FDA for human use; studied in research contexts. Regulatory status can change and differs by country; several peptides are also prohibited in sport (WADA). Verify current status before relying on it.

08What changed recently

Simple takeaway: No major evidence-changing update was identified in this review window.

The current profile reflects the existing body of indexed evidence. Material changes — new trials, approvals, or safety findings — are noted here when an editor logs them.

0 of 8 brief sections read
08 · community call

How the community sees this vs the evidence.

Your call on D-tier?

Evidence tier is D. Do you agree?

Community votes reflect user perception, not scientific proof — the evidence tier comes from our Research Maturity Index. Aggregate community sentiment will appear here once enough votes are collected.

Aggregate community sentiment will appear here once enough votes are in — we don't show invented numbers.

09 · follow updates
Follow updates on Melanotan II

Get notified when new studies, safety updates, regulatory changes, or the tier ranking change.

· New human study· Safety update· Regulatory change· Tier change· New claim check
10 · FAQ

FAQs

Is Melanotan II FDA-approved?

No. Melanotan II is not FDA-approved for the uses commonly discussed online. Not approved by the FDA for human use; studied in research contexts.

What is Melanotan II studied for?

Melanotan II is studied mainly for libido. Peptides acting on melanocortin and reproductive-hormone pathways, including an approved agent for a specific indication.

What does the research say about Melanotan II?

Mostly animal evidence. Human data is limited; most support comes from preclinical research.

Is Melanotan II safe?

Long-term human safety is not well established for Melanotan II. Quality and purity from non-pharmaceutical sources is an added risk.

🧮 Reconstitution calculator (educational)

Educational reconstitution math from your own values — not medical advice or a dose recommendation. Open the full calculator →

Medication (optional — 30+ in library)
Peptide in vial (mg)
Reconstitution water (mL)
Target amount per draw
Syringe
Draw to
10
units
Volume to draw
0.1
mL
At this amount
20
draws / vial
After one draw
4.75
mg left
Syringe · draw to 10 of 100 units
0
10
20
30
40
50
60
70
80
90
100

Each unit on a 100u · 1.0 mL syringe ≈ 25 mcg of this solution.

Concentration
2.5
mg / mL
Concentration
2,500
mcg / mL
Per U-100 unit
25
mcg / unit
Show the math
5 mg × 1000 = 5,000 mcg in the vial
2 mL × 100 = 200 U-100 units of liquid
5,000 mcg ÷ 200 units = 25 mcg per unit
250 mcg ÷ 25 mcg/unit = 10 units
10 units ÷ 100 = 0.1 mL
5,000 mcg ÷ 250 mcg = 20 draws per vial
Compare reconstitution volumes (5mg vial)
Water
mcg / unit
units for 250mcg
1 mL505
2 mL2510
2.5 mL2012.5
3 mL16.6715
5 mL1025

More water → lower concentration → more units for the same amount.

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Keep exploring
Compare nextMelanotan II vs Pt 141See the evidence side by side.Outcome pathLibido / sexual healthWhere Melanotan II sits vs. the alternatives.ToolConcentration calculatorHow vial size & water change concentration.
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Class
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