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- 2017-09-01 发布于上海
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dpore-mirna polymorphic regulation of microrna genesdpore-mirna多态调节微rna基因
dPORE-miRNA: Polymorphic Regulation of MicroRNA
Genes
Sebastian Schmeier, Ulf Schaefer, Cameron R. MacPherson, Vladimir B. Bajic*
Computational Bioscience Research Center (CBRC), King Abdullah University of Science and Technology (KAUST), Jeddah, Saudi Arabia
Abstract
Background: MicroRNAs (miRNAs) are short non-coding RNA molecules that act as post-transcriptional regulators and affect
the regulation of protein-coding genes. Mostly transcribed by PolII, miRNA genes are regulated at the transcriptional level
similarly to protein-coding genes. In this study we focus on human miRNAs. These miRNAs are involved in a variety of
pathways and can affect many diseases. Our interest is on possible deregulation of the transcription initiation of the miRNA
encoding genes, which is facilitated by variations in the genomic sequence of transcriptional control regions (promoters).
Methodology: Our aim is to provide an online resource to facilitate the investigation of the potential effects of single
nucleotide polymorphisms (SNPs) on miRNA gene regulation. We analyzed SNPs overlapped with predicted transcription
factor binding sites (TFBSs) in promoters of miRNA genes. We also accounted for the creation of novel TFBSs due to
polymorphisms not present in the reference genome. The resulting changes in the original TFBSs and potential creation of
new TFBSs were incorporated into the Dragon Database of Polymorphic Regulation of miRNA genes (dPORE-miRNA).
Conclusions: The dPORE-miRNA database enables researchers to explore potential effects of SNPs on the regulation of
miRNAs. dPORE-miRNA can be interrogated with regards to: a/miRNAs (their targets, or involvement in diseases, or
biological pathways), b/SNPs, or c/transcription factors. dPORE-miRNA can be accessed
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