4.8 Article

Prediction of novel microRNA genes in cancer-associated genomic regionsa combined computational and experimental approach

Journal

NUCLEIC ACIDS RESEARCH
Volume 37, Issue 10, Pages 3276-3287

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/nar/gkp120

Keywords

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Funding

  1. Action 8.3.1 (Reinforcement Pro-gram of Human Research Manpower-'PENED 2003', [03EDelta842]) of the operational program 'competitiveness' of the Greek General Secretariat for Research and Technology
  2. EU [FP6-IST-2002-507585]
  3. European Commission [PIOF-GA-2008-219622]

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The majority of existing computational tools rely on sequence homology and/or structural similarity to identify novel microRNA (miRNA) genes. Recently supervised algorithms are utilized to address this problem, taking into account sequence, structure and comparative genomics information. In most of these studies miRNA gene predictions are rarely supported by experimental evidence and prediction accuracy remains uncertain. In this work we present a new computational tool (SSCprofiler) utilizing a probabilistic method based on Profile Hidden Markov Models to predict novel miRNA precursors. Via the simultaneous integration of biological features such as sequence, structure and conservation, SSCprofiler achieves a performance accuracy of 88.95% sensitivity and 84.16% specificity on a large set of human miRNA genes. The trained classifier is used to identify novel miRNA gene candidates located within cancer-associated genomic regions and rank the resulting predictions using expression information from a full genome tiling array. Finally, four of the top scoring predictions are verified experimentally using northern blot analysis. Our work combines both analytical and experimental techniques to show that SSCprofiler is a highly accurate tool which can be used to identify novel miRNA gene candidates in the human genome. SSCprofiler is freely available as a web service at http://www.imbb.forth.gr/SSCprofiler.html.

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