1. Academic Validation
  2. Tandem Deubiquitination and Acetylation of SPRTN Promotes DNA-Protein Crosslink Repair and Protects against Aging

Tandem Deubiquitination and Acetylation of SPRTN Promotes DNA-Protein Crosslink Repair and Protects against Aging

  • Mol Cell. 2020 Sep 3;79(5):824-835.e5. doi: 10.1016/j.molcel.2020.06.027.
Jinzhou Huang 1 Qin Zhou 1 Ming Gao 1 Somaira Nowsheen 1 Fei Zhao 1 Wootae Kim 1 Qian Zhu 1 Yusuke Kojima 1 Ping Yin 1 Yong Zhang 1 Guijie Guo 1 Xinyi Tu 1 Min Deng 1 Kuntian Luo 1 Bo Qin 1 Yuichi Machida 1 Zhenkun Lou 2
Affiliations

Affiliations

  • 1 Department of Oncology, Mayo Clinic, Rochester, MN 55905, USA.
  • 2 Department of Oncology, Mayo Clinic, Rochester, MN 55905, USA. Electronic address: lou.zhenkun@mayo.edu.
Abstract

DNA-protein crosslinks (DPCs) are highly toxic DNA lesions that threaten genomic integrity. Recent findings highlight that SPRTN, a specialized DNA-dependent metalloprotease, is a central player in proteolytic cleavage of DPCs. Previous studies suggest that SPRTN deubiquitination is important for its chromatin association and activation. However, the regulation and consequences of SPRTN deubiquitination remain unclear. Here we report that, in response to DPC induction, the Deubiquitinase VCPIP1/VCIP135 is phosphorylated and activated by ATM/ATR. VCPIP1, in turn, deubiquitinates SPRTN and promotes its chromatin relocalization. Deubiquitination of SPRTN is required for its subsequent acetylation, which promotes SPRTN relocation to the site of chromatin damage. Furthermore, Vcpip1 knockout mice are prone to genomic instability and premature aging. We propose a model where two sequential post-translational modifications (PTMs) regulate SPRTN chromatin accessibility to repair DPCs and maintain genomic stability and a healthy lifespan.

Keywords

DNA repair; DNA-protein crosslink; SPRTN; Top1cc; VCPIP1/VCIP135; acetylation; aging; genomic instability; metalloprotease; ubiquitination.

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