FOXO4-DRI Peptide Reverses Endothelial Cell Aging Through P53 Pathway

Endothelial cells, which line our blood vessels, are crucial for cardiovascular health. Their senescence (cellular aging) contributes significantly to age-related diseases like atherosclerosis and hypertension. The P53 signaling pathway is a key regulator of this process, often promoting cell cycle arrest and senescence when activated. Despite its known role, the precise mechanisms by which novel therapeutic peptides like FOXO4-DRI interact with the P53 pathway to mitigate endothelial senescence remain underexplored.

The study revealed that FOXO4-DRI significantly reversed markers of senescence in both models. In senescent HUVECs, treatment with FOXO4-DRI led to a remarkable 58% reduction in SA-β-gal (senescence-associated beta-galactosidase) positive cells compared to untreated controls (p<0.001). Furthermore, expression of key senescence-associated genes, P16 and P21, decreased by 2.7-fold and 2.1-fold respectively (p<0.01). The most impactful finding was that FOXO4-DRI treatment significantly suppressed the P53 signaling pathway, evidenced by a 45% decrease in phosphorylated P53 levels and a 30% reduction in P53 target gene expression in aged mouse aortas (p<0.001). In vivo, aged mice treated with FOXO4-DRI showed a 43% decrease in aortic SA-β-gal staining and a 35% improvement in endothelium-dependent vasodilation, indicating enhanced vascular function compared to controls (p<0.05).