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Melanotan-2: Melanocortin MC1R Signaling & Melanogenesis Pathway Research

Last updated: July 2, 2026 · peer-reviewed receptor pharmacology literature referenced

Melanotan-2 (MT-2, also written Melanotan II) is a synthetic cyclic heptapeptide analog of α-melanocyte-stimulating hormone (α-MSH), first developed at the University of Arizona in the 1980s. In the published literature it is studied as a non-selective agonist of the melanocortin receptor family — the five G-protein-coupled receptors (MC1R–MC5R) that transduce melanocortin signals — with especially prominent activity at the MC1R subtype expressed on pigment-producing melanocytes. Its broad-spectrum receptor profile has made it a widely used reference compound in melanocortin receptor pharmacology and in the cell biology of the melanogenesis pathway.

What makes MT-2 valuable as a research tool is its combination of stability and breadth. The endogenous α-MSH hormone is a linear peptide degraded within seconds, whereas MT-2 incorporates a lactam bridge that constrains the molecule into a rigid, enzymatically resistant ring. This gives researchers a durable α-MSH mimetic for interrogating melanocortin receptor signaling in cultured cells and receptor-expression systems.

Research Use Only. Melanotan-2 is not a drug, dietary supplement, cosmetic, or medical device. It has not been approved by the FDA for any purpose. The information below summarizes published research on melanocortin receptor signaling and melanogenesis-pathway cell biology. Available for in vitro research purposes only.

Chemical Profile

Full NameMelanotan II
Also Known AsMT-2, MT-II, Melanotan-2
CAS Number121062-08-6
Molecular FormulaC50H69N15O9
Molecular Weight1024.2 g/mol
StructureCyclic (lactam-bridged) heptapeptide α-MSH analog
Receptor ProfileNon-selective melanocortin agonist (MC1R–MC5R)
Prominent TargetMC1R (melanocyte receptor)
Receptor ClassMelanocortin (Gs-coupled GPCR) family

A broad-spectrum reference ligand: Because MT-2 activates all five melanocortin receptor subtypes rather than a single one, researchers use it as a pan-melanocortin reference agonist. In pigment-cell studies its prominent MC1R activity provides a robust, reproducible readout of the cAMP-driven melanogenesis pathway, while its broader activity makes it a useful benchmark against which more subtype-selective research ligands are compared.

Primary Mechanisms of Action

1. MC1R Agonism on Melanocytes

The most extensively studied action of MT-2 is its agonism at the melanocortin-1 receptor (MC1R), the Gs-coupled receptor expressed on cutaneous and hair-follicle melanocytes. A foundational study in Endocrinology demonstrated that binding of melanotropic hormones to MC1R on human melanocytes stimulates both cell proliferation and melanogenesis — establishing the pigment-cell model in which α-MSH analogs like MT-2 are characterized.

Peer-Reviewed Study
Binding of melanotropic hormones to the melanocortin receptor MC1R on human melanocytes stimulates proliferation and melanogenesis
Endocrinology, 1996 · PubMed ↗

2. The cAMP / MITF / Tyrosinase Cascade

The signaling pathway downstream of MC1R is one of the best-characterized in pigment-cell biology. Agonist binding activates adenylyl cyclase, raising intracellular cAMP; cAMP in turn induces the microphthalmia-associated transcription factor (MITF), the master regulator of the melanocyte gene program. MITF upregulates tyrosinase and the tyrosinase-related proteins that carry out melanin biosynthesis, biasing output toward eumelanin. A review in Pigment Cell & Melanoma Research details the MC1R–cAMP axis and its signaling reach.

Peer-Reviewed Review
MC1R, the cAMP pathway, and the response to solar UV: extending the horizon beyond pigmentation
Pigment Cell & Melanoma Research, 2014 · PubMed ↗

3. MC1R Receptor Structure and Regulation

Understanding how MT-2 engages MC1R requires understanding the receptor itself. MC1R is a highly polymorphic G-protein-coupled receptor whose variants strongly influence its signaling output. A review in Frontiers in Genetics summarizes MC1R structure, function, and regulation, providing the receptor-level context in which melanocortin agonist pharmacology is interpreted.

Peer-Reviewed Review
Melanocortin 1 Receptor: Structure, Function, and Regulation
Frontiers in Genetics, 2016 · PubMed ↗

4. Structure-Activity of Cyclic Melanocortin Analogs

The lactam bridge that defines MT-2 is central to its pharmacology. By cyclizing the peptide, the bridge pre-organizes the conserved His-Phe-Arg-Trp core — the segment identified as essential for melanocortin receptor recognition — into a bioactive conformation and confers resistance to enzymatic degradation. Structural biology studies of potent cyclic and linear melanocortin analogues examine how this conformational constraint translates into receptor affinity and functional potency.

Peer-Reviewed Study
Structure and function of the potent cyclic and linear melanocortin analogues
Journal of Structural Biology, 2005 · PubMed ↗

Research Applications

Melanogenesis Pathway Cell Biology

MT-2 is a standard agonist for driving the melanogenesis pathway in cultured melanocytes and melanoma cell lines. Because it produces a strong, reproducible cAMP response at MC1R, researchers use it to study the transcriptional and enzymatic steps of eumelanin synthesis — from MITF induction through tyrosinase activation — and to test compounds that modulate this pathway.

MC1R Signaling and Structure-Function Research

MT-2 serves as a probe in structure-function studies of the MC1R binding pocket. Nuclear magnetic resonance (NMR) work on the binding of melanocortin analogues to MC1R has used cyclic α-MSH mimetics to map how ring size and conformation influence receptor affinity, informing the design of MC1R-targeted research ligands.

Peer-Reviewed Study
NMR Insights into the Structure-Function Relationships in the Binding of Melanocortin Analogues to the MC1R Receptor
Molecules, 2017 · PubMed ↗

Melanocyte Regulation Research

Beyond acute signaling, MT-2 is used to study longer-term melanocyte regulation — including receptor desensitization, the balance between eumelanin and pheomelanin output, and the influence of MC1R polymorphisms on agonist response. A review of MC1R structure and functional regulation in Pigment Cell Research frames how agonist stimulation intersects with these regulatory layers.

Peer-Reviewed Review
Melanocortin-1 receptor structure and functional regulation
Pigment Cell Research, 2005 · PubMed ↗

Comparison with Other Melanocortin Research Compounds

Within melanocortin research, compounds are distinguished mainly by receptor-subtype selectivity. MT-2 is a broad, non-selective agonist across MC1R–MC5R, which makes it a useful pan-melanocortin reference but also means effects observed in a mixed-receptor system cannot be attributed to a single subtype without additional controls. This contrasts with more selective research ligands and with its own derivative PT-141 (bremelanotide), a structurally related cyclic analog whose activity is weighted toward the centrally expressed MC4R and MC3R rather than MC1R.

This makes the MT-2 / PT-141 pair a recurring comparison in the literature: two closely related cyclic α-MSH analogs whose modest structural differences redistribute activity across a homologous receptor family, allowing researchers to study how melanocortin signaling partitions between peripheral pigment-cell receptors and central receptors.

Research Limitations

MT-2's principal interpretive limitation is its lack of receptor selectivity. Because it engages all five melanocortin subtypes, findings in systems that co-express multiple receptors require selective antagonists or receptor-knockout models to assign effects to a specific subtype. Its prominent MC1R activity is well suited to melanogenesis studies, but broader physiological readouts can reflect simultaneous activation of several receptors.

In addition, MC1R signaling output is strongly shaped by the receptor's many natural polymorphisms, so agonist responses measured in one melanocyte model may not generalize to cells carrying different MC1R variants. This receptor heterogeneity is an active consideration in the design of MC1R pharmacology experiments using MT-2.

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Frequently Asked Questions

What is Melanotan-2 (MT-2)?

Melanotan-2 (MT-2) is a synthetic cyclic heptapeptide analog of alpha-melanocyte-stimulating hormone that acts as a non-selective agonist across the melanocortin receptor family, with prominent activity at the MC1R subtype. In the published literature it is used as a reference compound for melanocortin receptor pharmacology and melanogenesis-pathway cell biology.

How does Melanotan-2 activate the MC1R signaling pathway in research models?

In pigment-cell models, MT-2 binds MC1R on melanocytes and activates the Gs / adenylyl cyclase / cAMP cascade. Elevated cAMP induces the transcription factor MITF, which upregulates tyrosinase and related enzymes in the eumelanin biosynthesis pathway. This makes MT-2 a standard agonist for studying MC1R receptor signaling and melanogenesis biology in vitro.

Is Melanotan-2 approved for human or therapeutic use?

No. Melanotan-2 is a research compound supplied strictly for in vitro laboratory study. It is not a drug, dietary supplement, or medical device and has not been evaluated or approved by the FDA for safety or efficacy in humans. NST Research makes no therapeutic, diagnostic, cosmetic, or health claims about it.