The interplay of oncogenic signaling, oxidative stress and ferroptosis in cancer

Author:

Zeng Wentao1,Long Xiaohang2,Liu Pu‐Ste3,Xie Xin1ORCID

Affiliation:

1. School of Life Science Shaoxing University Shaoxing Zhejiang China

2. School of Life Science The Chinese University of Hong Kong Hong Kong SAR China

3. Institute of Cellular and System Medicine National Health Research Institutes Miaoli County Taiwan

Abstract

AbstractOncogene‐induced hyper‐proliferation in cancer cells is accompanied by the onset of different stresses, including DNA‐replication stress, metabolic stress and oxidative stress. Excessive accumulation of reactive oxygen species (ROS) plays a pivotal and contradictory role in tumor progression. ROS dictates a multitude of cell signaling pathways to facilitate the malignant transformation of tumor cells. In the meantime, oxidative burden in tumor cells mandates reinforcing antioxidant capacity to mitigate detrimental damages. The addiction to oxidative stress and increased iron demands in cancer cells also impinges on the sensitivity of ferroptosis. Targeting redox homeostasis and ferroptosis to overcome drug resistance in cancer treatment has become an attractive research topic. However, the roles of oncogenic signaling in redox regulation and ferroptosis have not been comprehensively discussed. In this review, we summarize current knowledge regarding the interplay between redox regulation and ferroptosis in the context of cancer biology. We emphasize the implication of oncogenic signaling in redox homeostasis and ferroptosis regulation. We also provide an overview of strategies targeting oxidative stress and ferroptosis in cancer treatment.

Funder

Zhejiang Province Public Welfare Technology Application Research Project

Shaoxing University

Publisher

Wiley

Subject

Cancer Research,Oncology

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