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KPV

Lys-Pro-Val, α-MSH (11-13)

Quick Stats
Studies 104
Trials 57
Score 3
2019 pubmed 11 citations

Are melanocortin peptides future therapeutics for cutaneous wound healing?

Böhm. Markus M; Luger. Thomas T

Key Findings

  • Most skin cells have the MC1R receptor that binds α‑MSH and influences inflammation, protection, and collagen.
  • Short fragments such as KPV (Lys‑Pro‑Val) keep the anti‑inflammatory benefits but don’t trigger pigment production.
  • Pre‑clinical work (in silico, in vitro, ex vivo, animal) shows KPV can lower inflammation and may improve wound‑healing outcomes.

Practical Outcomes

  • For now, there’s no proven home‑use protocol for KPV. The peptide looks promising for faster, cleaner wound repair, but you’d need to wait for human safety and dosage studies before trying it. Keep an eye on future clinical trials if you’re interested in cutting‑edge wound‑care supplements.

Summary

Researchers think short peptides like KPV, which come from the hormone α‑MSH, could help skin wounds heal faster by reducing inflammation and protecting cells, without causing skin darkening. So far this is based on computer models, lab tests, and animal studies, not human trials.

Abstract

Cutaneous wound healing is a complex process divided into different phases, that is an inflammatory, proliferative and remodelling phase. During these phases, a variety of resident skin cell types but also cells of the immune system orchestrate the healing process. In the last year, it has been shown that the majority of cutaneous cell types express the melanocortin 1 receptor (MC1R) that binds α-melanocyte-stimulating hormone (α-MSH) with high affinity and elicits pleiotropic biological effects, for example modulation of inflammation and immune responses, cytoprotection, antioxidative defense and collagen turnover. Truncated α-MSH peptides such as Lys-Pro-Val (KPV) as well as derivatives like Lys-d-Pro-Thr (KdPT), the latter containing the amino acid sequence 193-195 of interleukin-1β, have been found to possess anti-inflammatory effects but to lack the pigment-inducing activity of α-MSH. We propose here that such peptides are promising future candidates for the treatment of cutaneous wounds and skin ulcers. Experimental approaches in silico, in vitro, ex vivo and in animal models are outlined. This is followed by an unbiased discussion of the pro and contra arguments of such peptides as future candidates for the therapeutic management of cutaneous wounds and a review of the so-far available data on melanocortin peptides and derivatives in wound healing.

Study Information

Provider

pubmed

Year

2019

Date

2019-02-12T00:00:00.000Z

DOI

10.1111/exd.13887

Citations

11

References

69