The “Dark Side” of autophagy on the maintenance of genome stability: Does it really exist during excessive activation?

Siao Muk Cheng; Min Chieh Shieh; Tzu Yu Lin; Chun Hei Antonio Cheung

doi:10.1002/jcp.30555

The “Dark Side” of autophagy on the maintenance of genome stability: Does it really exist during excessive activation?

Siao Muk Cheng, Min Chieh Shieh, Tzu Yu Lin, Chun Hei Antonio Cheung

Department of Pharmacology

Research output: Contribution to journal › Review article › peer-review

3 Citations (Scopus)

Abstract

Dysregulation of DNA damage response/repair and genomic instability promote tumorigenesis and the development of various neurological diseases. Autophagy is a dynamic catabolic process used for removing unnecessary or dysfunctional proteins and organelles in cells. Despite the consensus in the field that upregulation of autophagy promotes the initiation of the DNA damage response and assists the process of homologous recombination upon genotoxic stress, a few studies showed that upregulation of autophagy (or excessive autophagy), under certain circumstances, triggers caspase/apoptosis-independent DNA damage and promotes genomic instability in cells. As the cytoprotective and the DNA repairing roles of autophagy have been discussed extensively in different reviews, here, we mainly focus on describing the latest studies which reported the “opposite” roles of autophagy (or excessive autophagy). We will discuss whether the “dark side” (i.e., the opposite/unconventional effect) of autophagy on the maintenance of DNA integrity and genomic stability really does exist in cells and if it does, will it be one of the yet-to-be-identified causes of cancer, in this review.

Original language	English
Pages (from-to)	178-188
Number of pages	11
Journal	Journal of Cellular Physiology
Volume	237
Issue number	1
DOIs	https://doi.org/10.1002/jcp.30555
Publication status	Published - 2022 Jan

All Science Journal Classification (ASJC) codes

Physiology
Clinical Biochemistry
Cell Biology

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10.1002/jcp.30555

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title = "The “Dark Side” of autophagy on the maintenance of genome stability: Does it really exist during excessive activation?",

abstract = "Dysregulation of DNA damage response/repair and genomic instability promote tumorigenesis and the development of various neurological diseases. Autophagy is a dynamic catabolic process used for removing unnecessary or dysfunctional proteins and organelles in cells. Despite the consensus in the field that upregulation of autophagy promotes the initiation of the DNA damage response and assists the process of homologous recombination upon genotoxic stress, a few studies showed that upregulation of autophagy (or excessive autophagy), under certain circumstances, triggers caspase/apoptosis-independent DNA damage and promotes genomic instability in cells. As the cytoprotective and the DNA repairing roles of autophagy have been discussed extensively in different reviews, here, we mainly focus on describing the latest studies which reported the “opposite” roles of autophagy (or excessive autophagy). We will discuss whether the “dark side” (i.e., the opposite/unconventional effect) of autophagy on the maintenance of DNA integrity and genomic stability really does exist in cells and if it does, will it be one of the yet-to-be-identified causes of cancer, in this review.",

author = "Cheng, {Siao Muk} and Shieh, {Min Chieh} and Lin, {Tzu Yu} and Cheung, {Chun Hei Antonio}",

note = "Funding Information: This work was supported by the Ministry of Science and Technology, Taiwan (MOST 109‐2320‐B‐006‐031) and Ditmanson Medical Foundation Chia‐Yi Christian Hospital, Taiwan (CYC109006). Funding Information: This work was supported by the Ministry of Science and Technology, Taiwan (MOST 109-2320-B-006-031) and Ditmanson Medical Foundation Chia-Yi Christian Hospital, Taiwan (CYC109006). Publisher Copyright: {\textcopyright} 2021 Wiley Periodicals LLC",

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N2 - Dysregulation of DNA damage response/repair and genomic instability promote tumorigenesis and the development of various neurological diseases. Autophagy is a dynamic catabolic process used for removing unnecessary or dysfunctional proteins and organelles in cells. Despite the consensus in the field that upregulation of autophagy promotes the initiation of the DNA damage response and assists the process of homologous recombination upon genotoxic stress, a few studies showed that upregulation of autophagy (or excessive autophagy), under certain circumstances, triggers caspase/apoptosis-independent DNA damage and promotes genomic instability in cells. As the cytoprotective and the DNA repairing roles of autophagy have been discussed extensively in different reviews, here, we mainly focus on describing the latest studies which reported the “opposite” roles of autophagy (or excessive autophagy). We will discuss whether the “dark side” (i.e., the opposite/unconventional effect) of autophagy on the maintenance of DNA integrity and genomic stability really does exist in cells and if it does, will it be one of the yet-to-be-identified causes of cancer, in this review.

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The “Dark Side” of autophagy on the maintenance of genome stability: Does it really exist during excessive activation?

Abstract

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