HDAC3 aberration-incurred GPX4 suppression drives renal ferroptosis and AKI-CKD progression

Lijun Zhang; Fang Chen; Jian Dong; Rong Wang; Guangyu Bi; Daoliang Xu; Yingwei Zhang; Yijun Deng; Wenjun Lin; Zhongzhou Yang; Wangsen Cao

doi:10.1016/j.redox.2023.102939

HDAC3 aberration-incurred GPX4 suppression drives renal ferroptosis and AKI-CKD progression

Redox Biol. 2023 Dec:68:102939. doi: 10.1016/j.redox.2023.102939. Epub 2023 Oct 20.

Authors

Lijun Zhang¹, Fang Chen², Jian Dong³, Rong Wang⁴, Guangyu Bi⁴, Daoliang Xu⁴, Yingwei Zhang⁵, Yijun Deng², Wenjun Lin⁶, Zhongzhou Yang⁷, Wangsen Cao⁸

Affiliations

¹ Yancheng Medical Research Center of Nanjing University Medical School, Department of Central Laboratory, Yancheng First Hospital, Affiliated Hospital of Nanjing University Medical School, The First People's Hospital of Yancheng, Yancheng, China; Nanjing University Medical School, Jiangsu Key Lab of Molecular Medicine, Nanjing, China.
² Yancheng Medical Research Center of Nanjing University Medical School, Department of Central Laboratory, Yancheng First Hospital, Affiliated Hospital of Nanjing University Medical School, The First People's Hospital of Yancheng, Yancheng, China.
³ Nanjing University Medical School, Jiangsu Key Lab of Molecular Medicine, Nanjing, China.
⁴ Yangzhou Precision Research Institute of Kidney Disease, Department of Nephrology, Northern Jiangsu People's Hospital, Yangzhou, China.
⁵ Department of Respirology, Affiliated Drum Tower Hospital of Nanjing University Medical School, Nanjing, China.
⁶ Department of Nephrology, Shanghai Sixth People's Hospital Affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China. Electronic address: linwenjun5@126.com.
⁷ Nanjing University Medical School, Jiangsu Key Lab of Molecular Medicine, Nanjing, China. Electronic address: zhongzhouyang@nju.edu.cn.
⁸ Yancheng Medical Research Center of Nanjing University Medical School, Department of Central Laboratory, Yancheng First Hospital, Affiliated Hospital of Nanjing University Medical School, The First People's Hospital of Yancheng, Yancheng, China; Nanjing University Medical School, Jiangsu Key Lab of Molecular Medicine, Nanjing, China; Yangzhou Precision Research Institute of Kidney Disease, Department of Nephrology, Northern Jiangsu People's Hospital, Yangzhou, China. Electronic address: wangsencao@nju.edu.cn.

Abstract

Acute kidney injury (AKI) progression to chronic kidney disease (CKD) represents a unique renal disease setting characterized by early renal cellular injury and regulated cell death, and later renal fibrosis, of which the critical role and nature of ferroptosis are only partially understood. Here, we report that renal tubular epithelial ferroptosis caused by HDAC3 (histone deacetylase 3) aberration and the resultant GPX4 suppression drives AKI-CKD progression. In mouse models of AKI-CKD transition induced by nephrotoxic aristolochic acid (AA) and folic acid (FA), renal tubular epithelial ferroptosis occurred early that coincided with preferential HDAC3 elevation and marked suppression of a core anti-ferroptosis enzyme GPX4 (glutathione peroxidase 4). Intriguingly, genetic Hdac3 knockout or administration of a HDAC3-selective inhibitor RGFP966 effectively mitigated the GPX4 suppression, ferroptosis and the fibrosis-associated renal functional loss. In cultured tubular epithelial cells, HDAC3 over-expression or inhibition inversely affected GPX4 abundances. Further analysis revealed that Gpx4 promoter contains a typical binding motif of transcription factor KLF5 (Kruppel-like factor 5). HDAC3 and KLF5 inducibly associated and bound to Gpx4 promoter upon AA treatment, leading to local histone hypoacetylation and GPX4 transactivation inhibition, which was blocked by RGFP966 and a KLF5 inhibitor ML264, respectively, suggesting that KLF5 co-regulated the HDAC3-incurred Gpx4 transcription inhibition. More importantly, in AKI-CKD mice receiving a GPX4 inactivator RSL3, the anti-ferroptosis and renoprotective effects of RGFP966 were largely abrogated, indicating that GPX4 is an essential downstream mediator of the HDAC3 aberration and renal ferroptosis during AKI-CKD transition. Together, our study identified a critical epigenetic pathway of ferroptosis during AKI-CKD transition and suggested that the strategies preserving GPX4 by HDAC3 inhibition are potentially effective to reduce renal ferroptosis and slow AKI-CKD progression.

Keywords: AKI-CKD progression; Ferroptosis; GPX4; HDAC3; KLF5.

MeSH terms

Acute Kidney Injury* / etiology
Animals
Disease Progression
Ferroptosis* / genetics
Kidney / metabolism
Mice
Renal Insufficiency, Chronic* / complications
Renal Insufficiency, Chronic* / metabolism

Substances

RGFP966
histone deacetylase 3
glutathione peroxidase 4, mouse