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KPV
Inflammation Support

KPV

$135 retail

Chronic digestive inflammation, IBD/Crohn's/colitis markers, leaky gut, gut-skin-immune axis issues, inflammatory skin conditions, histamine-driven problems, immune modulation.

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Supplement Facts

Verified 2026-06-09 from product label (KPV_Facts.jpg).

  • Serving Size: 1 Capsule · Servings Per Container: 60
  • KPV - 500 mcg (naturally occurring acetylated and amidated form of KPV)
  • Other ingredients: Rice Flour, Silicon Dioxide, Timed Release Vegetable Capsule
  • Distributed for Haven Wellness, PO Box 1079, Pleasant Grove, UT 84062 (haven-health.co)

What it is

A tripeptide (Lys-Pro-Val) derived from the C-terminal of alpha-MSH (residues 11–13), formulated for oral delivery. Stripping the N-terminal portion of α-MSH removes melanocortin receptor binding (no pigmentation, no MC4R appetite effects) while concentrating anti-inflammatory function. The smallest known α-MSH-derived peptide with full anti-inflammatory function.

What it does (mechanism)

Primary action: intracellular blockade of NF-κB nuclear translocation.

  1. Enters cell via PepT1 / SLC15A1 (proton-coupled di/tripeptide transporter)
  2. Competes with NF-κB p65 (RelA) for importin-α3 binding (armadillo repeats 7-8)
  3. p65 stuck in cytoplasm → transcription of TNF-α, IL-1β, IL-6, IL-8, COX-2, iNOS sharply downregulated

Also suppresses MAPK (p38, JNK); inhibits NLRP3 inflammasome; stabilizes IκBα; shifts macrophages M1→M2. Largely MC-receptor-independent (Kannengiesser 2008) - anti-inflammatory effect persists in MC1R-null cells.

Why oral works: short tripeptide + proline imino-acid resists brush-border peptidases. Actively transported via **PepT1, which is upregulated in inflamed intestinal mucosa in IBD** - KPV literally concentrates in the tissue that needs it most (Dalmasso/Merlin 2007/2008, PMID 18061177).

Used for

Chronic digestive inflammation, IBD/Crohn's/colitis markers, leaky gut, gut-skin-immune axis issues, inflammatory skin conditions, histamine-driven problems, immune modulation.

Pairs well with

  • BPC-157 - gut healing stack (BPC for tissue repair, KPV for inflammation). Most-prescribed integrative protocol for IBS/IBD/leaky gut/post-antibiotic dysbiosis. [Practitioner]
  • Prebio Plus + Prospore - full gut-rebuild protocol. Sequence: reduce inflammation first (KPV ± BPC for 1–2 weeks) → layer prebiotic substrates → add spore-based probiotics. Throwing spores into hyperinflamed gut can transiently worsen symptoms. [Practitioner]
  • Ultromega - anti-inflammatory dual-pathway: KPV blocks NF-κB transcription (acute suppression); EPA/DHA-derived SPMs (resolvins, protectins, maresins) drive active resolution. Complementary, not redundant. [Clinical mechanism]
  • Thymogen Alpha 1 - immune modulation + inflammation. For chronic low-grade inflammation + immune underperformance (post-viral, long COVID, recurrent infections, MCAS with frequent infections). [Practitioner]

Dosing

Haven recommended (label protocol)

  • 1 capsule daily (500 mcg), oral, on an empty stomach (15–30 min pre-meal)
  • 4–8 weeks per course, then re-evaluate

Practitioner-directed [Practitioner]

  • 1 cap BID (1 mg/day) for active GI / dermatology / systemic inflammation, empty stomach AM + 30 min pre-dinner
  • Higher-end GI/autoimmune: 2–4 caps/day total (1–2 mg/day) split BID
  • Empty-stomach rationale: KPV is absorbed via PepT1, which is competitively occupied by dietary di/tripeptides from a meal. Same logic as valacyclovir / cefadroxil (also PepT1 substrates).
  • Plasma t½ 1–2 hr → BID maintains continuous mucosal exposure
  • Cycle: 4–8 weeks on, 2–4 off
  • MCAS / histamine patients: start at ½ cap (≈250 mcg) and titrate over 2 weeks - see Cautions

Cautions / contraindications

  • Headache in <5% during first week, self-resolving (likely transient cytokine shift / Herxheimer-like)
  • MCAS / histamine intolerance: α-MSH is a known mast-cell stabilizer; most MCAS patients report KPV is helpful. A ~5–10% subset reports first-week flushing/itching/worsening. Start at ½ cap/day in MCAS and titrate over 2 weeks.
  • Pregnancy / lactation / pediatric - no data, avoid
  • Active malignancy - no mechanistic concern (anti-inflammatory, not mitogenic), but no human safety data - defer to oncology
  • Vitiligo / pigmentation: safe (no MC1R binding)
  • Drug interactions: theoretical - PepT1 is also the absorption route for cefadroxil, valacyclovir, enalapril. Space dosing by 1–2 hours.
  • [Caveat] No published human RCT for oral KPV alone in IBD or skin disease. Evidence is mechanistic + animal models + practitioner case series. Merlin group nanoparticle work is at investigational stages.

Key studies & references

  • Dalmasso G et al. 2008 - PepT1-mediated tripeptide KPV uptake reduces intestinal inflammation - Gastroenterology 134:166 - PMID 18061177
  • Kannengiesser K et al. 2008 - KPV in DSS + CD45RBhi T-cell transfer colitis - Inflamm Bowel Dis 14:324
  • Bettenworth D et al. 2011 - oral KPV in DSS + TNBS colitis; PepT1-KO confirms PepT1 mechanism
  • Xiao B et al. 2017 - orally targeted KPV via HA-functionalized nanoparticles, alleviates UC - Mol Ther 25:1628 - PMID 28143741
  • Haycock JW et al. 2001 - KPV ameliorates LPS NF-κB translocation in alveolar epithelium - J Biol Chem - PMID 11256945
  • Brzoska T, Luger TA et al. 2008 - α-MSH peptides as new class of anti-inflammatory drugs - PMC2095288
  • Cutuli M et al. 2000 - direct antimicrobial activity against Candida albicans + S. aureus - J Leukoc Biol 67:233

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For practitionersThis page is general product education, not a treatment protocol. Dosing tiers above include practitioner-directed ranges for clinical context. For individualized recommendations, refer patients to Dr. Porter at integrativemedutah.com.