KPV (Lys-Pro-Val) is the C-terminal tripeptide of α-melanocyte-stimulating hormone (α-MSH, residues 11–13). At three residues, it is one of the smallest peptides documented to retain the parent hormone’s anti-inflammatory activity, making it a frequent reference compound in structure-activity studies of small anti-inflammatory peptides.
Published mechanism studies establish that KPV’s effects operate largely independently of melanocortin receptors. The dominant pathway is direct intracellular NF-κB inhibition: the tripeptide enters cells via passive diffusion or peptide-transporter-mediated uptake (PepT1 / SLC15A1), where it prevents p65-IκBα dissociation and blocks the transcription of pro-inflammatory cytokines (TNF-α, IL-1β, IL-6, IL-8) at the source.
Recent 2026 work (Lee et al., Cytotechnology, PMID 42064835) extended KPV’s mechanism profile from classical anti-inflammation into hepatic lipid metabolism, demonstrating ROS-dependent regulation of the PPARγ pathway in HepG2 cells. Active translational delivery research is developing targeted KPV systems for inflammatory bowel disease — hydrogel microsphere (Jeong et al., 2025, PMID 40030207) and temperature-sensitive hydrogel (Li et al., 2024, PMID 38289234) approaches.
Every Artemis Labs lot ships with a third-party Certificate of Analysis confirming identity (MS), purity (≥99% by reverse-phase HPLC), and endotoxin testing (≤0.5 EU/mg, LAL assay). Supplied as lyophilized white powder, 10 mg/vial, for in-vitro receptor, cell-culture, and pre-clinical research applications.
For research use only. Not for human or veterinary use.




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