| Literature DB >> 31735470 |
Sen Wei1, Tianming Qiu2, Xiaofeng Yao3, Ningning Wang4, Liping Jiang5, Xue Jia6, Ye Tao7, Zhidong Wang8, Pei Pei9, Jingyuan Zhang10, Yuhan Zhu11, Guang Yang12, Xiaofang Liu13, Shuang Liu14, Xiance Sun15.
Abstract
Chronic arsenic exposure is a significantly risk factor for pancreatic dysfunction and type 2 diabetes (T2D). Ferroptosis is a newly identified iron-dependent form of oxidative cell death that relies on lipid peroxidation. Previous data have indicated that ferroptosis is involved in various diseases, including cancers, neurodegenerative diseases, and T2D. However, the concrete effect and mechanism of ferroptosis on pancreatic dysfunction triggered by arsenic remains unknown. In this study, we verified that ferroptosis occurred in animal models of arsenic-induced pancreatic dysfunction through assessing proferroptotic markers and morphological changes in mitochondria. In vitro, arsenic caused execution of ferroptosis in a dose-dependent manner, which could be significantly reduced by ferrostatin-1. Additionally, arsenic damaged mitochondria manifested as diminishing of mitochondrial membrane potential, reduced cytochrome c level and production of mitochondrial reactive oxygen species (MtROS) in MIN6 cells. Using the Mito-TEMPO, we found the autophagy level and subsequent ferroptotic cell death induced by arsenic were both alleviated. With autophagy inhibitor chloroquine, we further revealed that ferritin regulated ferroptosis through the MtROS-autophagy pathway. Collectively, NaAsO2-induced ferroptotic cell death is relied on the MtROS-dependent autophagy by regulating the iron homeostasis. Ferroptosis is involved in pancreatic dysfunction triggered by arsenic, and arsenic-induced ferroptosis involves MtROS, autophagy, ferritin.Entities:
Keywords: Arsenic; Autophagy; Ferroptosis; Iron homeostasis; MtROS
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Year: 2019 PMID: 31735470 DOI: 10.1016/j.jhazmat.2019.121390
Source DB: PubMed Journal: J Hazard Mater ISSN: 0304-3894 Impact factor: 10.588