Vesugen: The Vascular Endothelium Bioregulator Tripeptide
Résumé Rapide
- What it is: Vesugen (Lys-Glu-Asp) is a synthetic tripeptide bioregulator targeting vascular endothelial tissue, developed from the Khavinson bioregulator series.
- Proposed mechanism: Like other Khavinson peptides, it is hypothesized to modulate gene expression in endothelial cells through direct DNA/histone interactions, influencing vascular wall integrity and endothelial function.
- Research claims: Published studies report improved endothelial cell proliferation, enhanced nitric oxide pathway gene expression, and favorable effects on vascular tone in aged animal models.
- Limitations: Research is confined to a single group; no independent replication; no controlled clinical trials by international standards.
- Status: Not FDA-approved. Not EMA-approved. Investigational with limited evidence base.
For informational purposes only. This article does not constitute medical advice. Consult a qualified healthcare provider for any health-related decisions.
What Is Vesugen?
Vesugen is a synthetic tripeptide with the amino acid sequence Lys-Glu-Asp (lysine-glutamic acid-aspartic acid). It is a member of the Khavinson bioregulator peptide family, designed to target vascular endothelial tissue. The name derives from the Latin "vas" (vessel), reflecting its intended specificity for blood vessel biology. Like other bioregulators in this series, Vesugen was developed at the Saint Petersburg Institute of Bioregulation and Gerontology under the direction of Professor Vladimir Khavinson.
The vascular endothelium — the single-cell layer lining all blood vessels — plays critical roles in vascular tone regulation, coagulation balance, inflammatory modulation, and angiogenesis. Age-related endothelial dysfunction is recognized as a key contributor to cardiovascular disease, and maintaining endothelial health is a significant area of medical research. For an overview of the entire bioregulator class, see our guide to bioregulator peptides.
| Property | Detail |
|---|---|
| Peptide Name | Vesugen |
| Sequence | Lys-Glu-Asp |
| Amino Acids | 3 (tripeptide) |
| Molecular Weight | ~376 Da |
| Target Tissue | Vascular endothelium |
| Origin | Khavinson bioregulator series |
| FDA Status | Not approved; not evaluated |
Mechanism of Action
Vesugen is proposed to operate through the same epigenetic mechanism attributed to other Khavinson bioregulators. The tripeptide is hypothesized to cross cell membranes, enter the nucleus, and interact with DNA and/or histone proteins in a sequence-specific manner to modulate gene transcription in endothelial cells.
Proposed Targets
- eNOS expression: Published studies suggest that Vesugen may upregulate endothelial nitric oxide synthase (eNOS) gene expression, potentially enhancing nitric oxide production — a key molecule for vasodilation, anti-thrombotic protection, and anti-inflammatory signaling.
- Adhesion molecule regulation: Some reports indicate modulation of endothelial adhesion molecule expression (ICAM-1, VCAM-1), which could influence leukocyte recruitment and inflammatory processes at the vascular wall.
- Endothelial proliferation: Cell culture studies have reported enhanced endothelial cell proliferation and migration with Vesugen treatment, suggesting potential effects on vascular repair and angiogenesis.
Research Findings
In Vitro Studies
Published cell culture experiments from the Khavinson group report that Vesugen treatment of human umbilical vein endothelial cells (HUVECs) enhances proliferation rates, increases eNOS protein expression, and modulates the expression of genes involved in vascular homeostasis. Some studies have used confocal microscopy with fluorescent-labeled peptides to demonstrate nuclear localization of the tripeptide, supporting the proposed mechanism of direct nuclear activity.
Animal Studies
Preclinical studies in aged rats have reported that Vesugen administration improved endothelium-dependent vasodilation, reduced markers of endothelial dysfunction, and partially restored vascular reactivity toward levels observed in younger animals. Some studies combined Vesugen with other bioregulators (such as Cardiogen) and reported synergistic cardiovascular effects.
Critical Assessment
The same methodological limitations that apply to the Khavinson bioregulator series broadly apply to Vesugen specifically. The evidence base consists primarily of publications from affiliated Russian laboratories, with limited independent validation. The proposed mechanism of a tripeptide directly modulating gene expression through DNA interaction remains controversial and unconfirmed by independent structural biology research. No randomized controlled clinical trials have been published.
Safety and Tolerability
As a simple tripeptide composed of common dietary amino acids, Vesugen is expected to have low intrinsic toxicity and rapid metabolic degradation. Published studies report no significant adverse effects in animal models. However, formal toxicology studies meeting international regulatory standards (GLP-compliant studies) have not been published or made publicly available. The safety profile cannot be considered established by Western pharmaceutical standards.
Regulatory Status
Vesugen is not approved by the FDA, EMA, or any major Western regulatory agency. It has been marketed in Russia and some Eastern European countries as a dietary supplement. As with all Khavinson bioregulators, regulatory status varies by jurisdiction, and the compound has not undergone the clinical trial process required for pharmaceutical approval in the United States or European Union.
Avertissement : Cet article est uniquement à des fins d'information et d'éducation. Il ne constitue pas un avis médical, un diagnostic ou un traitement. Consultez toujours des professionnels de santé qualifiés avant de prendre des décisions concernant l'utilisation de peptides ou tout protocole lié à la santé.
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