Comparative mRNA and microRNA Expression Profiling of Three Genitourinary Cancers Reveals Common Hallmarks and Cancer-Specific Molecular Events

Xianxin Li; Jiahao Chen; Xueda Hu; Yi Huang; Zhizhong Li; Liang Zhou; Zhijian Tian; Hongyu Ma; Zhiyun Wu; Maoshan Chen; Zujing Han; Zhiyu Peng; Xiaokun Zhao; Chang Yin Liang; Yong Wang; Liang Sun; Jing Chen; Jun Zhao; Bing‐Hua Jiang; Huanming Yang; Yaoting Gui; Zhiming Cai; Xiuqing Zhang

doi:10.1371/journal.pone.0022570

Comparative mRNA and microRNA Expression Profiling of Three Genitourinary Cancers Reveals Common Hallmarks and Cancer-Specific Molecular Events

Xianxin Li(Peking University Shenzhen Hospital), Jiahao Chen(South China University of Technology), Xueda Hu(Beijing Institute of Genomics), Yi Huang(Peking University Shenzhen Hospital), Zhizhong Li(South China University of Technology), Liang Zhou(Peking University Shenzhen Hospital), Zhijian Tian(BGI Group (China)), Hongyu Ma(BGI Group (China)), Zhiyun Wu(BGI Group (China)), Maoshan Chen(BGI Group (China)), Zujing Han(BGI Group (China)), Zhiyu Peng(BGI Group (China)), Xiaokun Zhao(Central South University), Chang Yin Liang(Anhui Medical University), Yong Wang(Peking University Shenzhen Hospital), Liang Sun(Peking University Shenzhen Hospital), Jing Chen(Peking University Shenzhen Hospital), Jun Zhao(Shantou University), Bing‐Hua Jiang(Shantou University Medical College), Huanming Yang(BGI Group (China)), Yaoting Gui(Peking University Shenzhen Hospital), Zhiming Cai(Shenzhen Second People's Hospital), Xiuqing Zhang(BGI Group (China))

PLoS ONE

July 25, 2011

10.1371/journal.pone.0022570

Cited by 80Open Access

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Abstract

BACKGROUND: Genome-wide gene expression profile using deep sequencing technologies can drive the discovery of cancer biomarkers and therapeutic targets. Such efforts are often limited to profiling the expression signature of either mRNA or microRNA (miRNA) in a single type of cancer. METHODOLOGY: Here we provided an integrated analysis of the genome-wide mRNA and miRNA expression profiles of three different genitourinary cancers: carcinomas of the bladder, kidney and testis. PRINCIPAL FINDINGS: Our results highlight the general or cancer-specific roles of several genes and miRNAs that may serve as candidate oncogenes or suppressors of tumor development. Further comparative analyses at the systems level revealed that significant aberrations of the cell adhesion process, p53 signaling, calcium signaling, the ECM-receptor and cell cycle pathways, the DNA repair and replication processes and the immune and inflammatory response processes were the common hallmarks of human cancers. Gene sets showing testicular cancer-specific deregulation patterns were mainly implicated in processes related to male reproductive function, and general disruptions of multiple metabolic pathways and processes related to cell migration were the characteristic molecular events for renal and bladder cancer, respectively. Furthermore, we also demonstrated that tumors with the same histological origins and genes with similar functions tended to group together in a clustering analysis. By assessing the correlation between the expression of each miRNA and its targets, we determined that deregulation of 'key' miRNAs may result in the global aberration of one or more pathways or processes as a whole. CONCLUSIONS: This systematic analysis deciphered the molecular phenotypes of three genitourinary cancers and investigated their variations at the miRNA level simultaneously. Our results provided a valuable source for future studies and highlighted some promising genes, miRNAs, pathways and processes that may be useful for diagnostic or therapeutic applications.

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