Vesugen is a small molecule made from three amino acids linked together into a tripeptide. It is studied for its association with vascular biology and endothelial cellular function. Blood vessels contain an inner endothelial layer that regulates circulation, vascular tone, and vessel flexibility. Over time, endothelial cells may exhibit reduced regenerative and adaptive signaling capacity due to aging-associated or stress-related factors. Vesugen is studied for its interaction with endothelial cellular pathways associated with proliferation, renewal, and vascular homeostasis. Research in laboratory cell cultures and animal models demonstrates associations with increased proliferative activity in vascular endothelial systems. Human observational research involving aging-associated vascular models has explored changes in circulation-related parameters and microvascular function. Experimental findings also suggest links between vascular support pathways and broader neurovascular signaling systems. Vesugen is part of ongoing research into peptide-based approaches targeting vascular aging and endothelial regulation.
Vesugen is the synthetic tripeptide Lys-Glu-Asp (KED), a short-chain bioregulator peptide designed to act selectively on vascular endothelial cells. Its molecular structure, consisting of a positively charged lysine residue flanked by two acidic residues (glutamic and aspartic acid), confers specific physicochemical properties that enable cellular uptake, nuclear translocation, and targeted interactions with chromatin components. At the molecular level, Vesugen functions primarily as an epigenetic regulator of gene expression without altering the underlying DNA sequence. It penetrates the nuclear compartment of endothelial cells and binds within the minor groove of double-stranded DNA at specific promoter regions, forming hydrogen bonds and electrostatic interactions with base pairs in a sequence-selective manner. This binding modulates chromatin accessibility and transcription factor recruitment, leading to upregulation of key genes involved in cellular proliferation and vascular homeostasis.
A central target is the promoter region of the MKI67 gene, which encodes the Ki-67 protein, a nuclear marker expressed during active phases of the cell cycle (G1, S, G2, and M) but absent in quiescent G0 cells. Age-related decline in endothelial proliferative capacity is associated with reduced Ki-67 levels, contributing to altered vessel repair signaling, senescence-associated pathways, and endothelial dysfunction. Vesugen’s interaction with the core promoter sequence (near the transcription start site, including motifs such as CATC) enhances MKI67 transcription, restoring Ki-67 expression particularly in cells from aged tissues. This promotes endothelial cell division, migration, and renewal of the vascular intima while counteracting accumulation of senescent cellular phenotypes associated with pro-inflammatory and pro-thrombotic signaling. Molecular docking analyses confirm stable complex formation in the minor groove, where the tripeptide’s side chains align to stabilize DNA conformation without intercalation or covalent modification, a mechanism shared with other short peptide bioregulators but tuned to vascular-specific gene sets.
Beyond Ki-67, Vesugen influences a network of interconnected pathways. It normalizes expression of endothelin-1, a potent vasoconstrictor and mitogen whose upregulation in atherosclerosis-associated or injured endothelium contributes to smooth muscle proliferation, fibrosis-associated remodeling, and vessel stiffening. By modulating excessive endothelin-1 signaling, Vesugen supports balanced vascular tone and vascular remodeling pathways associated with ischemic stress environments. Concurrently, it upregulates sirtuin 1 (SIRT1), a NAD+-dependent deacetylase central to cellular stress resistance, mitochondrial biogenesis, and metabolic regulation. SIRT1 activation enhances endothelial nitric oxide synthase (eNOS) activity, boosting nitric oxide bioavailability associated with vasodilation, inflammatory signaling modulation, and platelet-signaling balance. Through SIRT1, Vesugen also modulates downstream targets including PGC-1α and ERR-α, linking vascular signaling systems to insulin sensitivity pathways and cellular energy homeostasis.
Additional epigenetic effects include modulation of genes governing apoptosis and senescence (such as p16 and p21), neuronal differentiation markers (NES, GAP43, nestin), and pathways relevant to oxidative stress resistance (SOD2) and lipid handling (APOE, PPAR family members). In senescent fibroblast and endothelial models, Vesugen restores differentiation-associated markers and reduces oxidative DNA damage (measured by 8-OHdG levels), while exerting no adverse impact on mitochondrial membrane potential or lysosomal function at studied concentrations.
These molecular actions translate into broader cellular and tissue-level effects associated with vascular architecture and endothelial communication systems. Endothelial cells maintain the blood-brain barrier, regulate permeability, and orchestrate angiogenesis via VEGF signaling; Vesugen’s proliferative effects support these functions and may contribute to preservation of microcirculation integrity. Gap junction proteins such as connexins are indirectly supported through improved intercellular communication, facilitating coordinated endothelial responses to shear stress and hypoxia. In the context of peptide synthesis and biochemistry, Vesugen’s design exemplifies how minimal sequence length (three residues) achieves tissue selectivity: its amphipathic character and charge distribution favor nuclear entry in endothelial lineages while minimizing off-target interactions in non-vascular cells. As a short oligomer, it resembles endogenous signaling fragments released during matrix remodeling and cellular adaptation processes.
Potential research applications stem directly from endothelial signaling regulation and vascular homeostasis pathways. In atherosclerosis-associated models, where endothelial injury contributes to plaque formation and vascular remodeling, Vesugen’s effects on endothelial proliferation and endothelin-1 signaling are studied in relation to lesion progression and vascular integrity pathways involving coronary, cerebral, and peripheral arterial systems. In peripheral vascular research models, enhanced endothelial proliferation is associated with collateral vessel signaling and tissue oxygenation pathways under ischemic stress conditions.
Neurovascular applications include support for cerebral microcirculation and blood-brain barrier signaling integrity, with additional relevance to neurovascular inflammation pathways and neuronal resilience systems. In vascular-associated erectile signaling models, Vesugen is studied in relation to nitric oxide pathways and endothelial communication systems. Metabolically, SIRT1 upregulation positions Vesugen within broader research involving insulin signaling pathways, metabolic adaptation, diabetic vascular stress models, and fatty liver-associated metabolic regulation systems.
Research involving age-associated biological systems has explored how vascular senescence influences multi-organ signaling decline, including neuronal signaling, muscular adaptation, and systemic metabolic resilience. In neurodegenerative experimental models, vascular effects intersect with neuronal signaling pathways including dendritic spine density maintenance and synaptic plasticity markers, suggesting broader neurovascular interactions relevant to cognitive signaling systems.
Animal and in vitro trials provide the foundational mechanistic evidence. In cell cultures derived from vascular tissues of young and aged animals, as well as primary human endothelial cells, Vesugen consistently elevates Ki-67 protein levels and increases proliferative indices, with greater relative restoration observed in senescent populations. Organotypic explant cultures of blood vessels demonstrate stimulated growth-associated signaling and renewal pathways, accompanied by downregulated p53 activity and improved endothelial morphology. Molecular studies using docking simulations and chromatin immunoprecipitation-like approaches confirm direct promoter engagement at the MKI67 locus.
In murine models of high-fat diet-induced metabolic stress, Vesugen activates SIRT1 pathways associated with insulin signaling modulation and vascular inflammatory pathway regulation. Transgenic 5xFAD Alzheimer’s disease mice treated systemically show preserved hippocampal dendritic spine morphology—particularly mushroom-type spines associated with long-term potentiation—along with trends toward restored synaptic plasticity, reduced endothelial and neuronal apoptosis-associated signaling, and sex-specific neurovascular protective effects. These preclinical data highlight Vesugen’s capacity to counteract age- and disease-associated endothelial senescence while exerting broader neurovascular effects through perfusion-associated pathways and epigenetic regulation of vascular and neuronal gene networks.
Human observational and interventional research involving aging-associated vascular models aligns with the peptide’s molecular profile. In subjects with lower-limb vascular insufficiency associated with atherosclerotic conditions, Vesugen monotherapy or adjunctive use was associated with measurable changes in vascular parameters, including walking-distance metrics and ankle-brachial index measurements, reflecting endothelial signaling activity and microcirculatory function. Separate vascular studies involving erectile-function-associated blood-flow models reported changes in penile arterial circulation metrics and Doppler ultrasound measurements consistent with endothelial signaling modulation.
In middle-aged and elderly cohorts with polymorbidity-associated vascular and neurovascular changes, Vesugen research observations included anabolic signaling responses, altered central nervous system activity markers, and broader physiological adaptation patterns compared to comparator peptides. Additional observational findings involving cerebral atherosclerosis-associated and cognitive-aging-associated models noted changes in memory-associated signaling, attention-related parameters, and lipid-profile markers, consistent with neurovascular and inflammatory signaling modulation. Across these studies, observed effects were most pronounced in tissues with elevated vascular demand, reinforcing the peptide’s selective interaction with endothelial renewal and gene-expression pathways.
Collectively, the molecular, preclinical, and observational research data position Vesugen as a notable peptide in vascular bioregulation research. Its ability to engage DNA promoters epigenetically, restore proliferative competence via Ki-67 signaling, modulate vasoconstrictor and vasodilatory pathways, and activate SIRT1-associated cellular regulation pathways provides a multifaceted model for studying endothelial adaptation and vascular aging biology.
For investigators in biochemistry and cell biology, Vesugen exemplifies how rationally designed short peptides may interact with endogenous regulatory circuits involved in vascular chromatin regulation and endothelial signaling systems. Future exploration may further clarify interactions with other bioregulators and short-chain peptide systems involved in cardiovascular, neurovascular, and metabolic signaling research while advancing peptide synthesis strategies for tissue-selective epigenetic modulators.
Read more about vascular bioregulator peptides and their relationship to endothelial signaling, circulation, and vascular aging research.
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Para manter a fiabilidade dos resultados laboratoriais, o armazenamento correto dos peptídeos é essencial. Condições adequadas ajudam a preservar a estabilidade dos peptídeos durante anos, protegendo-os contra contaminação, oxidação e degradação.
Embora alguns peptídeos sejam mais sensíveis do que outros, seguir estas boas práticas prolongará significativamente a vida útil e a integridade estrutural.
Os peptídeos podem ser comprometidos pela exposição à humidade e ao ar, especialmente após a remoção do congelador.
Os peptídeos em solução têm uma vida útil muito mais curta do que na forma liofilizada e são mais suscetíveis à degradação bacteriana.
Selecionar recipientes limpos, intactos, quimicamente resistentes e adequados ao volume da amostra.
Peptídeos enviados em frascos de plástico podem ser transferidos para vidro para armazenamento a longo prazo, se desejado.
