GAGE mediates radio resistance in cervical cancers via the regulation of chromatin accessibility
Nin, Dawn Sijin; Wujanto, Caryn; Tan, Tuan Zea; Lim, Diana; Damen, J Mirjam A; Wu, Kuan-Yi; Dai, Ziyu Melvin; Lee, Zheng-Wei; Idres, Shabana Binte; Leong, Yiat Horng; Jha, Sudhakar; Ng, Joseph Soon-Yau; Low, Jeffrey J H; Chang, Shih-Chung; Tan, David Shao Peng; Wu, Wei; Choo, Bok Ai; Deng, Lih-Wen
(2021) Cell Reports, volume 36, issue 9, pp. 1 - 26
(Article)
Abstract
Radiotherapy (RT) resistance is a major cause of treatment failure in cancers that use definitive RT as their primary treatment modality. This study identifies the cancer/testis (CT) antigen G antigen (GAGE) as a mediator of radio resistance in cervical cancers. Elevated GAGE expression positively associates with de novo RT resistance
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in clinical samples. GAGE, specifically the GAGE12 protein variant, confers RT resistance through synemin-dependent chromatin localization, promoting the association of histone deacetylase 1/2 (HDAC1/2) to its inhibitor actin. This cumulates to elevated histone 3 lysine 56 acetylation (H3K56Ac) levels, increased chromatin accessibility, and improved DNA repair efficiency. Molecular or pharmacological disruption of the GAGE-associated complex restores radiosensitivity. Molecularly, this study demonstrates the role of GAGE in the regulation of chromatin dynamics. Clinically, this study puts forward the utility of GAGE as a pre-screening biomarker to identify poor responders at initial diagnosis and the therapeutic potential of agents that target GAGE and its associated complex in combination with radiotherapy to improve outcomes.
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Keywords: CT antigens, DNA damage response, DNA repair, GAGE, GAGE12, cancer testis antigens, cervical cancer, chromatin dynamics, radioresistance, radiotherapy, General Biochemistry,Genetics and Molecular Biology
ISSN: 2211-1247
Publisher: Elsevier Saunders
Note: Funding Information: This work was supported by grants from the Terry Fox Foundation Singapore ( NF15TFR051 ) to B.A.C., National University Hospital, Singapore, Junior Pitch for Fund to C.W., National University Health System, Singapore ( R-183-000-461-733 ) to D.S.N., and the Ministry of Education, Taiwan ; ( MOE-AcRF-Tier 2 and R-183-000-459-112 ) and National University Cancer Institute, Singapore ( NR15NMR229 and NR18NMR119 ) to L.-W.D. Publisher Copyright: © 2021 The Author(s)
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