BPC-157

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BPC-157

Gastric pentadecapeptide BPC-157 researched for pleiotropic regenerative signaling via VEGFR2, GHR sensitization, and NO homeostasis

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Title	Quantity	Discounted Price
Bulk Discount	3 - 5	5% $32.30
Bulk Discount	6 - 8	7% $31.62
Bulk Discount	9 +	10% $30.60

Certificate of Analysis

Pentadecapeptide 5MG Pentadecapeptide 500MCG Pentadecapeptide 10MG

BPC-157 Overview

Mechanism of Action: The Pleiotropic Regulator

BPC-157 is an experimental pentadecapeptide, a synthetic fragment derived from an endogenous protein found in mammalian gastric juice. Preclinical analysis indicates it does not function through a single, high-affinity receptor but rather acts as a pleiotropic regulator, modulating a complex network of signaling pathways integral to tissue repair, cytoprotection, and the systemic response to injury.

The observed effects of BPC-157 stem from key pathway modulations documented in preclinical models:

Vascular Signaling and Angiogenesis: The compound upregulates the expression of Vascular Endothelial Growth Factor Receptor 2 (VEGFR2), sensitizing endothelial cells to naturally present growth factors. This activation of the VEGFR2-Akt-eNOS signaling axis promotes new blood vessel formation (angiogenesis) and endothelial cell proliferation/migration.
Growth Factor Sensitization: In models utilizing tendon fibroblasts, BPC-157 exposure enhanced the expression of the Growth Hormone Receptor (GHR). This sensitization subsequently potentiated the proliferative response of these cells to Growth Hormone (GH) stimulation, activating the downstream JAK2-STAT signaling cascade that drives cell growth.
Cellular Migration and Adhesion: The compound influences the physical reconstruction of tissue by activating the Focal Adhesion Kinase (FAK)-paxillin pathway. This is critical for promoting the migration, spreading, and adhesion of reparative cells, leading to enhanced wound closure kinetics observed in in vitro models.
Nitric Oxide (NO) Homeostasis: BPC-157 exhibits a stabilizing, homeostatic effect on the NO system, promoting beneficial localized vasodilation while concurrently mitigating the tissue damage caused by both NO deficiency and NO excess. This contributes to its overall cytoprotective profile.

Summary of Observed Human Study Outcomes

Rigorous, large-scale, randomized controlled trials (RCTs) necessary to establish definitive efficacy and safety are critically lacking, resulting in an overwhelming reliance on preclinical animal models. The limited human studies reported in the literature are primarily small-scale and/or unpublished, and their results are considered anecdotal and scientifically unproven.

Study/Trial Type	Compound Measured	Objective/Setting	Key Observed Outcomes
Retrospective Study	BPC-157 (Intra-articular injection)	Small, retrospective evaluation involving 16 subjects with unspecified chronic knee pain.	14 out of 16 subjects reported subjective pain relief that was sustained for over six months.
Phase II Trial	BPC-157 (PL 14736, administered via enema)	Investigated in rats with active ulcerative colitis (a subtype of Inflammatory Bowel Disease).	Results reportedly indicated safety and efficacy in inducing remission. Full, peer-reviewed data remains unavailable.
Pilot Study	BPC-157 (Intravesical injection)	Investigated in 12 subjects diagnosed with interstitial cystitis.	Reportedly led to symptom resolution in a majority of the participants.
Phase I Trial	BPC-157 (Oral tablet formulation)	Registered on ClinicalTrials.gov (NCT02637284) as a phase I clinical trial in healthy volunteers to study safety and pharmacokinetics of BPC-157, a pentadecapeptide from gastric source.	No results have been posted or published. The status of this trial is unclear.

Comparison to General Peptide Pharmacology

BPC-157 exhibits characteristics that represent a significant divergence from typical therapeutic peptides, primarily concerning its stability and unique pharmacological mechanism, as highlighted by preclinical analysis.

Feature	BPC-157 (Gastric Pentadecapeptide)	Conventional Therapeutic Peptides (Generally)
Physicochemical Stability	Demonstrates exceptional resilience; highly resistant to enzymatic degradation and hydrolysis, remaining intact in acidic environments.	Typically fragile and rapidly degraded by proteases in the digestive system and bloodstream.
Delivery Consideration	High stability allows for the possibility of oral research administration while still achieving systemic effects.	Poor oral bioavailability, generally necessitating parenteral (injection) administration to bypass the gastrointestinal tract.
Pharmacological Action	Acts as a biological “trigger” or initiator; brief exposure is sufficient to activate sustained downstream cellular processes (e.g., upregulating receptor gene expression).	Rapidly cleared, generally only interacting with fast-acting cell surface receptors, often requiring continuous presence.

Research References

Pentadecapeptide BPC 157 Enhances the Growth Hormone Receptor Expression in Tendon Fibroblasts. View Study
The promoting effect of pentadecapeptide BPC 157 on tendon healing involves tendon outgrowth, cell survival, and cell migration. View Study
Stable Gastric Pentadecapeptide BPC 157: Novel Therapy in Gastrointestinal Tract. View Study
Multifunctionality and Possible Medical Application of the BPC 157 Peptide—Literature and Patent Review. View Study

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