Cell Death and Disease (Feb 2022)

Identification of Nanog as a novel inhibitor of Rad51

  • Ying Xin,
  • Juanjuan Wang,
  • Yahong Wu,
  • Qianqian Li,
  • Mingyang Dong,
  • Chang Liu,
  • Qijia He,
  • Ruifeng Wang,
  • Dian Wang,
  • Sen Jiang,
  • Wei Xiao,
  • Yang Tian,
  • Weiwei Zhang

DOI
https://doi.org/10.1038/s41419-022-04644-9
Journal volume & issue
Vol. 13, no. 2
pp. 1 – 13

Abstract

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Abstract To develop inhibitors targeting DNA damage repair pathways is important to improve the effectiveness of chemo- and radiotherapy for cancer patients. Rad51 mediates homologous recombination (HR) repair of DNA damages. It is widely overexpressed in human cancers and overwhelms chemo- and radiotherapy-generated DNA damages through enhancing HR repair signaling, preventing damage-caused cancer cell death. Therefore, to identify inhibitors of Rad51 is important to achieve effective treatment of cancers. Transcription factor Nanog is a core regulator of embryonic stem (ES) cells for its indispensable role in stemness maintenance. In this study, we identified Nanog as a novel inhibitor of Rad51. It interacts with Rad51 and inhibits Rad51-mediated HR repair of DNA damage through its C/CD2 domain. Moreover, Rad51 inhibition can be achieved by nanoscale material- or cell-penetrating peptide (CPP)-mediated direct delivery of Nanog-C/CD2 peptides into somatic cancer cells. Furthermore, we revealed that Nanog suppresses the binding of Rad51 to single-stranded DNAs to stall the HR repair signaling. This study provides explanation for the high γH2AX level in unperturbed ES cells and early embryos, and suggests Nanog-C/CD2 as a promising drug candidate applied to Rad51-related basic research and therapeutic application studies.