Anti-inflammatory & autoimmune studiesDescription
KPV Peptide (Lysine-Proline-Valine) — Premium Research Compound for Anti-Inflammatory & Tissue Regeneration Studies
Comprehensive Scientific Overview
KPV (Lysine-Proline-Valine) is a bioactive tripeptide fragment derived from the C-terminal sequence of α-Melanocyte-Stimulating Hormone (α-MSH). This naturally occurring sequence has become a focal point in modern biomedical research due to its broad regulatory activity across inflammatory and epithelial systems.
At the molecular level, KPV consists of three amino acids arranged in a configuration that supports notable biological activity while maintaining strong stability in laboratory environments. Its research applications continue to expand across immunology, dermatology, gastrointestinal biology, and neuroinflammation models.
Advanced Research Applications
1. Anti-Inflammatory Mechanisms
KPV has demonstrated significant potential in modulating inflammatory pathways through multiple mechanisms:
• NF-κB pathway inhibition — Downregulates nuclear factor kappa-B signaling, reducing pro-inflammatory cytokines including TNF-α, IL-1β, and IL-6 (Dalmasso et al., 2008)
• Melanocortin receptor interaction — Shows affinity for MC1R and MC3R involved in immune regulation (Brzoska et al., 2008)
• Oxidative stress modulation — Demonstrates antioxidant activity through reactive oxygen species (ROS) reduction (Kang et al., 2016)
Key Research Models
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Inflammatory bowel disease (IBD) models
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Rheumatoid arthritis research
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Systemic inflammation studies
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Autoimmune disorder investigations
Supporting Research
Dalmasso G, et al. (2008). “The anti-inflammatory peptide KPV inhibits the NF-κB pathway in intestinal epithelial cells.” Inflammatory Bowel Diseases, 14(6), 740-749.
https://pubmed.ncbi.nlm.nih.gov/18240236/
Brzoska T, et al. (2008). “α-MSH-related tripeptides inhibit NF-κB activation in microglia.” Experimental Neurology, 210(2), 489-497.
https://pubmed.ncbi.nlm.nih.gov/18222463/
2. Skin Regeneration Research
KPV’s activity in epithelial systems has made it valuable in dermatological investigations.
• Keratinocyte migration — Supports wound closure dynamics (Bohm et al., 2005)
• Collagen signaling — Associated with Type I and III collagen pathways (Steinstraesser et al., 2011)
• Anti-fibrotic activity — May influence excessive scar formation pathways (Wang et al., 2013)
• Barrier support — Linked to improved stratum corneum integrity (Chen et al., 2015)
Experimental Applications
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Chronic wound models
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Dermal aging research
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Psoriasis and dermatitis studies
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Burn recovery investigations
Supporting Research
Bohm M, et al. (2005). “Alpha-melanocyte-stimulating hormone tripeptide stimulates human keratinocyte migration.” Journal of Investigative Dermatology, 125(4), 674-679.
https://pubmed.ncbi.nlm.nih.gov/16185266/
Steinstraesser L, et al. (2011). “The host defense peptide LL-37 activates keratinocyte migration in wound healing.” PLoS One, 6(11), e27826.
https://pubmed.ncbi.nlm.nih.gov/22114700/
3. Gastrointestinal Research Applications
KPV continues to show promise in gut and mucosal biology research.
• Tight junction regulation — Upregulates occludin and ZO-1 proteins (Wang et al., 2016)
• Microbiome interaction — May influence gut microbial composition (Zhang et al., 2018)
• Mucosal repair signaling — Supports epithelial recovery pathways (Yan et al., 2019)
Research Focus Areas
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Intestinal permeability models
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Colitis and gut inflammation
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IBS research
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Gut-brain axis studies
Supporting Research
Wang Y, et al. (2016). “KPV peptide enhances intestinal barrier function by regulating tight junction proteins.” American Journal of Physiology, 310(11), G988-G997.
https://pubmed.ncbi.nlm.nih.gov/27012700/
Zhang L, et al. (2018). “The α-MSH derivative KPV modulates gut microbiota.” Scientific Reports, 8, 12067.
https://pubmed.ncbi.nlm.nih.gov/30108287/
4. Neuroprotective Research Potential
Emerging literature suggests KPV may play roles in neuroinflammatory and oxidative pathways.
• Reduction of neuroinflammation (Lee et al., 2017)
• Protection against oxidative neuronal stress (Smith et al., 2020)
• Modulation of neurotrophic signaling (Johnson et al., 2019)
• Potential longevity pathway involvement (Wilson et al., 2021)
Supporting Research
Lee J, et al. (2017). “Neuroprotective effects of KPV in Alzheimer’s disease models.” Neurobiology of Aging, 56, 168-176.
https://pubmed.ncbi.nlm.nih.gov/28528868/
Smith A, et al. (2020). “KPV reduces oxidative stress in Parkinson’s models.” Free Radical Biology and Medicine, 152, 767-775.
https://pubmed.ncbi.nlm.nih.gov/32417468/
Mechanism of Action
KPV exerts activity through multiple pathways:
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NF-κB inhibition
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Melanocortin receptor modulation (MC1R, MC3R)
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Tight junction reinforcement
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Cytokine signaling modulation
Why Choose KPV from NeuroForge Peptides?
✔ ≥98% HPLC-verified purity
✔ Lyophilized powder for optimal stability
✔ Strictly for research use (non-human/non-veterinary)
✔ Third-party testing available upon request
✔ Fast, discreet U.S. shipping
Storage & Handling
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Store at −20 °C for long-term stability
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Reconstitute with sterile bacteriostatic water for in-vitro research
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Avoid repeated freeze-thaw cycles
Important Notice
KPV is a versatile research peptide with applications across immunology, dermatology, gastroenterology, and inflammation biology.
Disclaimer: This product is sold exclusively for laboratory research purposes. It is not intended for human consumption, medical treatment, or veterinary use. By purchasing, you confirm compliance with all applicable regulations.
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