Senolytic Peptide FOXO4-DRI Targets Disordered p53 to Combat Cellular Senescence

Cellular senescence, a state where cells stop dividing but remain metabolically active, is a fundamental process contributing to aging phenotypes and various age-related diseases, including cancers. Senescent cells accumulate in tissues and secrete inflammatory factors, driving pathology and tissue dysfunction. Previous research identified the FOXO4-p53 axis as pivotal in maintaining the viability of these persistent senescent cells, and the peptide FOXO4-DRI as a promising senolytic (senescent cell-killing) agent; however, the precise molecular mechanism by which FOXO4 and FOXO4-DRI interact with p53 to induce senolysis remained unclear, hindering targeted drug development.

The study revealed a striking finding: the intrinsically disordered FOXO4-DRI peptide binds directly to the disordered p53 transactivation domain 2 (p53TAD2), forming a transiently folded complex rather than a rigid structure. This interaction is crucial for its senolytic activity. > This transient complex formation is critical, as both the FOXO4-derived region and a cationic cell permeability peptide (a component designed to help the peptide enter cells) within FOXO4-DRI contribute synergistically to the interaction with p53. Furthermore, the researchers discovered that p53 phosphorylation (the addition of a phosphate group to p53) significantly enhances the binding affinity for both the natural FOXO4 protein and the FOXO4-DRI peptide, suggesting a key regulatory mechanism that could be exploited for therapeutic targeting. This enhanced affinity implies that phosphorylated p53 becomes a more receptive target for senolytic intervention.