Comprehensive Characterization of Somatic Mutations Impacting LncRNA Expression for Pan-Cancer

Overview

Journal Mol Ther Nucleic Acids

Publisher Cell Press

Date 2019 Sep 17

PMID 31525663

Citations 20

Authors

Yue Gao

Xin Li

Hui Zhi

Yunpeng Zhang

Peng Wang

Yanxia Wang

Shipeng Shang

Ying Fang

Weitao Shen

Shangwei Ning

Steven Xi Chen

Xia Li

Affiliations

Soon will be listed here.

Abstract

Somatic mutations have long been recognized as an important feature of cancer. However, analysis of somatic mutations, to date, has focused almost entirely on the protein coding regions of the genome. The potential roles of somatic mutations in human long noncoding RNAs (lncRNAs) are therefore largely unknown, particularly their functional significance across different cancer types. In this study, we characterized some lncRNAs whose expression was affected by somatic mutations (defined as MutLncs) and constructed global MutLnc landscapes across 17 cancer types by systematically integrating multiple levels of data. MutLncs were commonly downregulated and carried low mutation frequencies and non-silent mutations in most cancer types. Co-occurrence analysis in pan-cancer highlighted combined patterns of specific MutLncs, suggesting that a number of MutLncs influence diverse cancer types through combination effects. Several conserved and cancer-specific functions of MutLncs were determined. We further explored the somatic mutations affecting lncRNA expression via mixed and unmixed effects, which led to specific functions in pan-cancer. Survival analysis indicated that MutLncs and co-occurrence pairs can potentially serve as cancer biomarkers. Clarification of the specific roles of MutLncs in human cancers could be beneficial for understanding the molecular pathogenesis of different cancer types and developing the appropriate treatments.

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