MicroRNA in colorectal cancer: from benchtop to bedside

William Ka Kei Wu(Chinese University of Hong Kong), Priscilla T. Y. Law, C. W. Lee, C. H. Cho(Chinese University of Hong Kong), D. Fan(Xijing Hospital), Kaichun Wu(Xijing Hospital), Jun Yu, Joseph J.�Y. Sung
Carcinogenesis
November 16, 2010
Cited by 138

Abstract

Colon carcinogenesis represents a stepwise progression from benign polyps to invasive adenocarcinomas and distant metastasis. It is believed that these pathologic changes are contributed by aberrant activation or inactivation of protein-coding proto-oncogenes and tumor suppressor genes. However, recent discoveries in microRNA (miRNA) research have reshaped our understanding of the role of non-protein-coding genes in carcinogenesis. In this regard, a remarkable number of miRNAs exhibit differential expression in colon cancer tissues. These miRNAs alter cell proliferation, apoptosis and metastasis through their interactions with intracellular signaling networks. From a clinical perspective, polymorphisms within miRNA-binding sites are associated with the risk for colon cancer, whereas miRNAs isolated from feces or blood may serve as biomarkers for early diagnosis. Altered expression of miRNA or polymorphisms in miRNA-related genes have also been shown to correlate with patient survival or treatment outcome. With further insights into miRNA dysregulation in colon cancer and the advancement of RNA delivery technology, it is anticipated that novel miRNA-based therapeutics will emerge.


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