1. Cisplatin-Mediated Upregulation of APE2 Binding to MYH9 Provokes Mitochondrial Fragmentation and Acute Kidney Injury
- Author
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Nikhil C. Munshi, Daisuke Tsuchimoto, Mei Yin, Allison J. Janocha, Yi Hu, Hua Fang, Shan Yan, Thomas LaFramboise, Li Xue, Alex Mejia-Garcia, Chen Li, Chun Yang, Jennifer S. Yu, Jianhong Lin, Kenneth C. Anderson, Chuanfeng Fang, Yusaku Nakabeppu, Qing Y. Zheng, Tania Amorim, Xin Qi, Leal Herlitz, Faiz Anwer, Jenny Lin, Jack Khouri, Mohsin Maqbool, Ariel Kwart, Xiaofeng Jiang, and Jianjun Zhao
- Subjects
0301 basic medicine ,Genetically modified mouse ,Cancer Research ,Mitochondrial Diseases ,DNA damage ,Hearing Loss, Sensorineural ,Transgene ,Antineoplastic Agents ,Mice, Transgenic ,Mitochondrion ,medicine.disease_cause ,DNA, Mitochondrial ,Article ,Carboplatin ,Kidney Tubules, Proximal ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Downregulation and upregulation ,DNA-(Apurinic or Apyrimidinic Site) Lyase ,Animals ,Humans ,Medicine ,Mice, Knockout ,Cisplatin ,Mutation ,Nephritis ,Myosin Heavy Chains ,business.industry ,Acute kidney injury ,Acute Kidney Injury ,Endonucleases ,medicine.disease ,Multifunctional Enzymes ,Thrombocytopenia ,Mitochondria ,Up-Regulation ,Mice, Inbred C57BL ,Oxaliplatin ,Phenotype ,030104 developmental biology ,Oncology ,030220 oncology & carcinogenesis ,Cancer research ,business ,DNA Damage ,medicine.drug - Abstract
Cisplatin chemotherapy is standard care for many cancers but is toxic to the kidneys. How this toxicity occurs is uncertain. In this study, we identified apurinic/apyrimidinic endonuclease 2 (APE2) as a critical molecule upregulated in the proximal tubule cells (PTC) following cisplatin-induced nuclear DNA and mitochondrial DNA damage in cisplatin-treated C57B6J mice. The APE2 transgenic mouse phenotype recapitulated the pathophysiological features of C-AKI (acute kidney injury, AKI) in the absence of cisplatin treatment. APE2 pulldown-MS analysis revealed that APE2 binds myosin heavy-Chain 9 (MYH9) protein in mitochondria after cisplatin treatment. Human MYH9-related disorder is caused by mutations in MYH9 that eventually lead to nephritis, macrothrombocytopenia, and deafness, a constellation of symptoms similar to the toxicity profile of cisplatin. Moreover, cisplatin-induced C-AKI was attenuated in APE2-knockout mice. Taken together, these findings suggest that cisplatin promotes AKI development by upregulating APE2, which leads to subsequent MYH9 dysfunction in PTC mitochondria due to an unrelated role of APE2 in DNA damage repair. This postulated mechanism and the availability of an engineered transgenic mouse model based on the mechanism of C-AKI provides an opportunity to identify novel targets for prophylactic treatment of this serious disease. Significance: These results reveal and highlight an unexpected role of APE2 via its interaction with MYH9 and suggest that APE2 has the potential to prevent acute kidney injury in patients with cisplatin-treated cancer.
- Published
- 2021
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