FOXO4-DRI regulates endothelial cell senescence via the P53 signaling pathway
Zhicheng Hu, Fan Li, Chunyi Hu, Qiongdan Shan, Zhouhao Tang, Meifan Jiang, Xiaojing Yi, Xixi Chen, Litai Jin, Xu Wang, Yang Wang

TL;DR
A new peptide called FOXO4-DRI helps eliminate old endothelial cells by targeting a specific protein interaction, potentially slowing vascular aging.
Contribution
FOXO4-DRI is introduced as a novel peptide that selectively induces apoptosis in senescent endothelial cells via the P53 signaling pathway.
Findings
FOXO4-DRI improves vascular function and delays aging in both naturally aged and progeroid mice.
FOXO4-DRI prevents FOXO4-P53 binding, leading to P53 nuclear exclusion and apoptosis in senescent cells.
Treatment with FOXO4-DRI alleviates endothelial cell senescence caused by oxygen-glucose deprivation.
Abstract
Endothelial cell dysfunction during aging is a key driver of vascular aging and related diseases; however, effective strategies to selectively eliminate senescent endothelial cells and restore vascular function remain lacking. FOXO4-DRI, a novel peptide-based intervention, specifically disrupts the interaction between FOXO4 and P53, thereby inducing apoptosis in senescent cells. This study innovatively focuses on the mechanism by which FOXO4-DRI induces apoptosis in senescent endothelial cells, demonstrating that it functions by activating the p53/BCL-2/Caspase-3 signaling pathway to promote selective apoptosis of these cells. FOXO4-DRI significantly improves vascular function and delays vascular aging. These findings not only enrich the molecular understanding of senescent cell clearance but also provide a novel strategy for precise targeting of endothelial cell senescence in…
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Taxonomy
TopicsFOXO transcription factor regulation · Telomeres, Telomerase, and Senescence · Genetics, Aging, and Longevity in Model Organisms
