Farnesoid X receptor protects against cisplatin-induced acute kidney injury by regulating the transcription of ferroptosis-related genes

Dong-Hyun Kim; Hoon-In Choi; Jung Sun Park; Chang Seong Kim; Eun Hui Bae; Seong Kwon Ma; Soo Wan Kim

doi:10.1016/j.redox.2022.102382

Farnesoid X receptor protects against cisplatin-induced acute kidney injury by regulating the transcription of ferroptosis-related genes

Redox Biol. 2022 Aug:54:102382. doi: 10.1016/j.redox.2022.102382. Epub 2022 Jun 23.

Authors

Dong-Hyun Kim¹, Hoon-In Choi¹, Jung Sun Park¹, Chang Seong Kim¹, Eun Hui Bae¹, Seong Kwon Ma¹, Soo Wan Kim²

Affiliations

¹ Department of Internal Medicine, Chonnam National University Medical School, Gwangju, 61469, South Korea.
² Department of Internal Medicine, Chonnam National University Medical School, Gwangju, 61469, South Korea. Electronic address: skimw@chonnam.ac.kr.

Abstract

The side effects of cisplatin, a widely used chemotherapeutic agent, include nephrotoxicity. Previous studies have reported that cisplatin induces ferroptosis and lipid peroxide accumulation. Ferroptosis, a type of regulated cell death, is characterized by iron-dependent lipid peroxidation. Although previous studies have examined the regulation of ferroptosis in acute kidney injury (AKI), the regulatory mechanism of ferroptosis has not been elucidated. Here, the ability of activated farnesoid X receptor (FXR) to attenuate cisplatin-induced AKI through the regulation of ferroptosis was examined. FXR deficiency exhibited more ferroptosis responses, such as increase in lipid peroxidation, iron content and heme oxygenase 1 protein, and a decrease in glutathione/glutathione disulfide ratio and glutathione peroxidase 4 levels in HK2 cells and mice. Increased blood urea nitrogen, serum creatinine, and ferroptotic responses in the cisplatin-induced AKI mouse model were mitigated upon treatment with the FXR agonist GW4064 but were exacerbated in FXR knockout mice. RNA sequencing analysis revealed that ferroptosis-associated genes were novel targets of FXR. FXR agonist upregulated the expression of lipid and glutathione metabolism-related genes and downregulated cell death-related genes. Additionally, chromatin immunoprecipitation assays, using mice renal tissues, revealed that agonist-activated FXR could bind to its known target genes (Slc51a, Slc51b, Osgin1, and Mafg) and ferroptosis-related genes (Aifm2, Ggt6, and Gsta4). Furthermore, activated FXR-dependent MAFG, a transcriptional repressor, could bind to Hmox1, Nqo1, and Tf in the renal tissues of FXR agonist-treated mice. These findings indicate that activated FXR regulates the transcription of ferroptosis-related genes and protects against cisplatin-induced AKI.

Keywords: Acute kidney injury (AKI); Farnesoid X receptor (FXR); Ferroptosis; MAF bZIP transcription factor G (MAFG); Reactive oxidative stress (ROS).

MeSH terms

Acute Kidney Injury* / chemically induced
Acute Kidney Injury* / genetics
Acute Kidney Injury* / metabolism
Animals
Cisplatin / adverse effects
Ferroptosis* / genetics
Glutathione
Humans
Iron
Mice
Mice, Inbred C57BL
Receptors, Cytoplasmic and Nuclear* / genetics
Receptors, Cytoplasmic and Nuclear* / metabolism

Substances

Receptors, Cytoplasmic and Nuclear
farnesoid X-activated receptor
Iron
Glutathione
Cisplatin