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Melanotan-I

Afamelanotide, MT-I, [Nle4-D-Phe7]-α-MSH, Scenesse, CUV-1647

Quick Stats
Studies 225
Trials 100
Score 3
1992 pubmed

The expression of functional MSH receptors on cultured human melanocytes.

Donatien. P D PD; Hunt. G G; Pieron. C C; Lunec. J J; Taïeb. A A; Thody. A J AJ

Key Findings

  • Human melanocytes bind alpha‑MSH with high affinity (Kd ≈5×10⁻ÂčÂč M) and about 700 receptors per cell
  • Keratinocytes and fibroblasts do not show specific MSH binding, indicating cell‑type specificity
  • cAMP‑elevating agents (dibutyryl cAMP) boost receptor binding by ~62%; cholera toxin modestly ↑ binding, while TPA reduces it

Practical Outcomes

  • For biohackers, this confirms that melanotan‑I has a real receptor target in human pigment cells, suggesting it can work as intended. Compounds that raise intracellular cAMP (e.g., forskolin) might enhance the tanning effect, but the data are from cultured cells, so real‑world results may vary and safety should be considered.

Summary

The study shows that human skin cells that make pigment (melanocytes) have specific receptors for alpha‑MSH, the natural hormone that melanotan‑I mimics, and that these receptors can be increased or decreased by certain chemicals. This confirms the basic target for melanotan‑I is present in human cells, but the work was done in a dish, not in living people.

Abstract

Although alpha-MSH increases skin darkening in humans, there are several reports that it fails to have melanogenic effects on human melanocytes in vitro. The purpose of this study was to see whether cultured human melanocytes express MSH receptors. Human melanocytes were grown in the absence of artificial mitogens such as 12-O-tetradecanoyl phorbol-13-acetate (TPA) and cholera toxin (CT) and incubated for 2 h at room temperature with increasing amounts of 125I-labelled Nle4DPhe7-alpha-MSH with and without excess cold peptide. Binding was saturable and specific: Scatchard analysis gave a Kd of 4.9 x 10(-11) M and approximately 700 binding sites/cell. Human keratinocytes and fibroblasts showed no specific binding. The addition of 1 mM dibutyryl cAMP to the culture medium caused a 62% increase in MSH binding to human melanocytes. A smaller increase (25%) was seen with 10(-9) M CT while 25 mM TPA caused a 24% decrease. These results show that human melanocytes in culture express MSH receptors and that this expression can be modulated by mitogens.

Study Information

Provider

pubmed

Year

1992

DOI

10.1007/bf00372074