A potassium‐chloride co‐transporter with altered genome architecture functions as a suppressor in glioma

Author:

Liu Hongwei12,Pan Zhouyang12,Lin Xuelei12,Chen Long12,Yang Qi12,Zhang Wei12,Dai Luohuan12,Zhang Yihao12,Li Wang12,Chen Yinhua12,Peng Kang23,Wanggou Siyi12,Zeng Feiyue3,Li Xuejun12ORCID

Affiliation:

1. Department of Neurosurgery, Xiangya Hospital Central South University Changsha China

2. Hunan International Scientific and Technological Cooperation Base of Brain Tumor Research, Xiangya Hospital Central South University Changsha China

3. Department of Radiology, Xiangya Hospital Central South University Changsha China

Abstract

AbstractGliomas, the most lethal tumours in brain, have a poor prognosis despite accepting standard treatment. Limited benefits from current therapies can be attributed to genetic, epigenetic and microenvironmental cues that affect cell programming and drive tumour heterogeneity. Through the analysis of Hi‐C data, we identified a potassium‐chloride co‐transporter SLC12A5 associated with disrupted topologically associating domain which was downregulated in tumour tissues. Multiple independent glioma cohorts were included to analyse the characterization of SLC12A5 and found it was significantly associated with pathological features, prognostic value, genomic alterations, transcriptional landscape and drug response. We constructed two SLC12A5 overexpression cell lines to verify the function of SLC12A5 that suppressed tumour cell proliferation and migration in vitro. In addition, SLC12A5 was also positively associated with GABAA receptor activity and negatively associated with pro‐tumour immune signatures and immunotherapy response. Collectively, our study provides a comprehensive characterization of SLC12A5 in glioma and supports SLC12A5 as a potential suppressor of disease progression.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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