Epigenetic regulation of microRNAs in cancer: An integrated review of literature

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• 作者：Tanja Kunej^a ;   ; ¹ ;   ; ^{tanja.kunej@bf.uni-lj.si} ; Irena Godnic^a ;   ; ¹ ;   ; ^{irena.godnic@gmail.com} ; Jana Ferdin^a ;   ; ^b ;   ; ¹ ;   ; ^{jana.ferdin@bf.uni-lj.si} ; Simon Horvat^a ;   ; ^{simon.horvat@bf.uni-lj.si} ; Peter Dovc^a ;   ; ^{peter.dovc@bf.uni-lj.si} ; George Adrian Calin^b ;   ; ^{gcalin@mdanderson.org}
• 关键词：Cancer ; DNA methylation ; Epigenetics ; microRNA ; oncomiRs
• 刊名：Mutation Research/Fundamental and Molecular Mechanisms of Mutagenesis
• 出版年：2011
• 出版时间：1 December 2011
• 年：2011
• 卷：717
• 期：1-2
• 页码：77-84
• 全文大小：1152 K

文摘

MicroRNAs (miRNAs) belong to the heterogeneous class of non-coding RNAs (ncRNAs) that regulate the translation and degradation of target mRNAs, and control approximately 30 % of human genes. MiRNA genes might be silenced in human tumors (oncomiRs) by aberrant hypermethylation of CpG islands that encompass or lie adjacent to miRNA genes and/or by histone modifications. We performed literature search for research articles describing epigenetically regulated miRNAs in cancer and identified 45 studies that were published between 2006 and 7/2010. The data from those papers are fragmented and methodologically heterogeneous and our work represents first systematic review towards to integration of diverse sets of information.

We reviewed the methods used for detection of miRNA epigenetic regulation, which comprise bisulfite genomic sequencing PCR (BSP), bisulfite pyrosequencing, methylation specific PCR (MSP), combined bisulfite restriction analysis (COBRA), methylation sensitive single nucleotide primer extension (Ms-SNuPE), MassARRAY technique and some modifications of those methods. This integrative study revealed 122 miRNAs that were reported to be epigenetically regulated in 23 cancer types. Compared to protein coding genes, human oncomiRs showed an order of magnitude higher methylation frequency (11.6 % ; 122/1048 known miRNAs). Nearly half, (45 % ; 55/122) epigenetically regulated miRNAs were associated with different cancer types, but other 55 % (67/122) miRNAs were present in only one cancer type and therefore representing cancer-specific biomarker potential. The data integration revealed miRNA epigenomic hot spots on the chromosomes 1q, 7q, 11q, 14q and 19q. CpG island analysis of corresponding miRNA precursors (pre-miRNAs) revealed that 20 % (26/133) of epigenetically regulated miRNAs had a CpG island within the range of 5 kb upstream, among them 14 % (19/133) of miRNAs resided within the CpG island. Our integrative survey and analyses revealed candidate cancer-specific miRNA epigenetic signatures which provide the basis for new therapeutic strategies in cancer by targeting the epigenetic regulation of miRNAs.