The BRD7-P53-SLC25A28 axis regulates ferroptosis in hepatic stellate cells

Zili Zhang; Mei Guo; Min Shen; Desong Kong; Feng Zhang; Jiangjuan Shao; Shanzhong Tan; Shijun Wang; Anping Chen; Peng Cao; Shizhong Zheng

doi:10.1016/j.redox.2020.101619

The BRD7-P53-SLC25A28 axis regulates ferroptosis in hepatic stellate cells

Redox Biol. 2020 Sep:36:101619. doi: 10.1016/j.redox.2020.101619. Epub 2020 Jun 24.

Authors

Zili Zhang¹, Mei Guo², Min Shen¹, Desong Kong¹, Feng Zhang¹, Jiangjuan Shao¹, Shanzhong Tan³, Shijun Wang⁴, Anping Chen⁵, Peng Cao⁶, Shizhong Zheng⁷

Affiliations

¹ Department of Pharmacology, School of Pharmacy, Nanjing University of Chinese Medicine, Nanjing, 210023, China.
² Department of Pathogenic Biology and Immunology, Medical School, Southeast University, Nanjing, 210009, China.
³ Nanjing Hospital Affiliated to Nanjing University of Chinese Medicine, Nanjing, 210003, China.
⁴ College of Traditional Chinese Medicine, Shandong University of Traditional Chinese Medicine, Jinan, 250035, China.
⁵ Department of Pathology, School of Medicine, Saint Louis University, St Louis, MO63104, USA.
⁶ Department of Pharmacology, School of Pharmacy, Nanjing University of Chinese Medicine, Nanjing, 210023, China; Affiliated Hospital of Integrated Traditional Chinese and Western Medicine, Nanjing University of Chinese Medicine, Nanjing, 210028, China. Electronic address: cao_peng@njucm.edu.cn.
⁷ Department of Pharmacology, School of Pharmacy, Nanjing University of Chinese Medicine, Nanjing, 210023, China. Electronic address: nytws@163.com.

Abstract

Ferroptosis is a recently discovered form of programmed cell death, but its regulatory mechanisms are not fully understood. In the current study, we reported that the BRD7-P53-SLC25A28 axis played a crucial role in regulating ferroptosis in hepatic stellate cells (HSCs). Upon exposure to ferroptosis inducers, bromodomain-containing protein 7 (BRD7) protein expression was remarkably increased through the inhibition of the ubiquitin-proteasome pathway. CRISPR/Cas9-mediated BRD7 knockout conferred resistance to HSC ferroptosis, whereas specific BRD7 plasmid-mediated BRD7 overexpression facilitated HSC ferroptosis. Interestingly, the elevated BRD7 expression exhibited to promote p53 mitochondrial translocation via direct binding with p53 N-terminal transactivation domain (TAD), which may be the underlying mechanisms for BRD7-enhanced HSC ferroptosis. Site-directed mutations of serine 392 completely blocked the binding of BRD7 to p53, and, in turn, prevented p53 mitochondrial translocation and HSC ferroptosis. Importantly, mitochondrial p53 interacted with solute carrier family 25 member 28 (SLC25A28) to form complex and enhanced the activity of SLC25A28, which could lead to the abnormal accumulation of redox-active iron and hyperfunction of electron transfer chain (ETC). SLC25A28 knockdown impaired BRD7-or p53-mediated ferroptotic events. In mice, erastin treatment ameliorated pathological damage of liver fibrosis through inducing HSC ferroptosis. HSC-specific blockade of BRD7-P53-SLC25A28 axis could abrogate erastin-induced HSC ferroptosis. Of note, we analyzed the effect of sorafenib on HSC ferroptosis in advanced fibrotic patients with hepatocellular carcinoma receiving sorafenib monotherapy. Attractively, BRD7 upregulation, p53 mitochondrial translocation, combination of SLC25A28 and p53, and ferroptosis induction occurred in primary human HSCs. Overall, these findings reveal novel signal transduction and regulatory mechanism of ferroptosis, and also suggest BRD7-P53-SLC25A28 axis as potential targets for liver fibrosis.

Keywords: BRD7; Ferroptosis; Hepatic stellate cell; P53; SLC25A28.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Carcinoma, Hepatocellular*
Cation Transport Proteins*
Chromosomal Proteins, Non-Histone
Ferroptosis*
Hepatic Stellate Cells
Humans
Liver Neoplasms*
Mice
Tumor Suppressor Protein p53 / genetics

Substances

BRD7 protein, human
Brd7 protein, mouse
Cation Transport Proteins
Chromosomal Proteins, Non-Histone
SLC25A28 protein, human
Tumor Suppressor Protein p53