Sensitive and highly resolved identification of RNA-protein interaction sites in PAR-CLIP data

被引:0
作者
Federico Comoglio
Cem Sievers
Renato Paro
机构
[1] Swiss Federal Institute of Technology Zurich,Department of Biosystems Science and Engineering
[2] Massachusetts General Hospital and Harvard Medical School,Department of Pathology and Center for Cancer Research
[3] Broad Institute of MIT and Harvard,Faculty of Science
[4] University of Basel,undefined
来源
BMC Bioinformatics | / 16卷
关键词
PAR-CLIP; RNA; RNA binding proteins; Bayesian statistics;
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[1]  
van Kouwenhove M(2011)MicroRNA regulation by RNA-binding proteins and its implications for cancer Nat Rev Cancer 11 644-56
[2]  
Kedde M(2013)The long and short of microRNA Cell 153 516-9
[3]  
Agami R.(2008)RNA-binding proteins in human genetic disease Trends Genet 24 416-25
[4]  
Yates LA(2013)RNA-binding proteins in Mendelian disease Trends Genet 29 318-27
[5]  
Norbury CJ(2013)A compendium of RNA-binding motifs for decoding gene regulation Nature 499 172-177
[6]  
Gilbert RJ(2012)Protein-RNA interactions: new genomic technologies and perspectives Nat Rev Genet 13 77-83
[7]  
Lukong KE(2010)Transcriptome-wide identification of RNA-binding protein and microRNA target sites by PAR-CLIP Cell 141 129-41
[8]  
Chang KW(2012)Identification of RNA-protein interaction networks using PAR-CLIP Wiley Interdiscip Rev RNA 3 159-77
[9]  
Khandjian EW(2013)PRC2 binds active promoters and contacts nascent RNAs in embryonic stem cells Nat Struct Mol Biol 20 1258-64
[10]  
Richard S.(2009)MirZ: an integrated microRNA expression atlas and target prediction resource Nucleic Acids Res 37 W266-72
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