Combinatorial microRNA target predictions

Azra Krek; Dominic Grün; Matthew N. Poy; Rachel Wolf; Lauren Rosenberg; Eric J. Epstein; Philip MacMenamin; Isabelle Da Piedade; Kristin C. Gunsalus; Markus Stoffel; Nikolaus Rajewsky

doi:10.1038/ng1536

Combinatorial microRNA target predictions

Azra Krek, Dominic Grün, Matthew N. Poy, Rachel Wolf, Lauren Rosenberg, Eric J. Epstein, Philip MacMenamin, Isabelle Da Piedade, Kristin C. Gunsalus, Markus Stoffel, Nikolaus Rajewsky

Research output: Contribution to journal › Article › peer-review

Abstract

MicroRNAs are small noncoding RNAs that recognize and bind to partially complementary sites in the 3′ untranslated regions of target genes in animals and, by unknown mechanisms, regulate protein production of the target transcript. Different combinations of microRNAs are expressed in different cell types and may coordinately regulate cell-specific target genes. Here, we present PicTar, a computational method for identifying common targets of microRNAs. Statistical tests using genome-wide alignments of eight vertebrate genomes, PicTar's ability to specifically recover published microRNA targets, and experimental validation of seven predicted targets suggest that PicTar has an excellent success rate in predicting targets for single microRNAs and for combinations of microRNAs. We find that vertebrate microRNAs target, on average, roughly 200 transcripts each. Furthermore, our results suggest widespread coordinate control executed by microRNAs. In particular, we experimentally validate common regulation of Mtpn by miR-375, miR-124 and let-7b and thus provide evidence for coordinate microRNA control in mammals.

Original language	English (US)
Pages (from-to)	495-500
Number of pages	6
Journal	Nature Genetics
Volume	37
Issue number	5
DOIs	https://doi.org/10.1038/ng1536
State	Published - May 2005

ASJC Scopus subject areas

Genetics

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10.1038/ng1536

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title = "Combinatorial microRNA target predictions",

abstract = "MicroRNAs are small noncoding RNAs that recognize and bind to partially complementary sites in the 3′ untranslated regions of target genes in animals and, by unknown mechanisms, regulate protein production of the target transcript. Different combinations of microRNAs are expressed in different cell types and may coordinately regulate cell-specific target genes. Here, we present PicTar, a computational method for identifying common targets of microRNAs. Statistical tests using genome-wide alignments of eight vertebrate genomes, PicTar's ability to specifically recover published microRNA targets, and experimental validation of seven predicted targets suggest that PicTar has an excellent success rate in predicting targets for single microRNAs and for combinations of microRNAs. We find that vertebrate microRNAs target, on average, roughly 200 transcripts each. Furthermore, our results suggest widespread coordinate control executed by microRNAs. In particular, we experimentally validate common regulation of Mtpn by miR-375, miR-124 and let-7b and thus provide evidence for coordinate microRNA control in mammals.",

author = "Azra Krek and Dominic Gr{\"u}n and Poy, {Matthew N.} and Rachel Wolf and Lauren Rosenberg and Epstein, {Eric J.} and Philip MacMenamin and {Da Piedade}, Isabelle and Gunsalus, {Kristin C.} and Markus Stoffel and Nikolaus Rajewsky",

note = "Funding Information: We thank V. Miljkovic and S. Pueblas for preparing figures for the manuscript. N. Rajewsky thanks T. Tuschl, P. Macino and F. Piano for discussions. This project was funded in part by a grant from the US National Institutes of Health Funding Information: (to M.S.). D.G. acknowledges a scholarship by the German Academic Exchange Service. K.C.G. and P.M. were supported by grants from the US National Institutes of Health (to F. P{\'i}aro) and the US National Science Foundation (to K.C.G.). This research was supported in part by the Howard Hughes Medical Institute grant through the Undergraduate Biological Sciences Education Program to New York University.",

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doi = "10.1038/ng1536",

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AU - Krek, Azra

AU - Grün, Dominic

AU - Poy, Matthew N.

AU - Wolf, Rachel

AU - Rosenberg, Lauren

AU - Epstein, Eric J.

AU - MacMenamin, Philip

AU - Da Piedade, Isabelle

AU - Gunsalus, Kristin C.

AU - Stoffel, Markus

AU - Rajewsky, Nikolaus

N1 - Funding Information: We thank V. Miljkovic and S. Pueblas for preparing figures for the manuscript. N. Rajewsky thanks T. Tuschl, P. Macino and F. Piano for discussions. This project was funded in part by a grant from the US National Institutes of Health Funding Information: (to M.S.). D.G. acknowledges a scholarship by the German Academic Exchange Service. K.C.G. and P.M. were supported by grants from the US National Institutes of Health (to F. Píaro) and the US National Science Foundation (to K.C.G.). This research was supported in part by the Howard Hughes Medical Institute grant through the Undergraduate Biological Sciences Education Program to New York University.

PY - 2005/5

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N2 - MicroRNAs are small noncoding RNAs that recognize and bind to partially complementary sites in the 3′ untranslated regions of target genes in animals and, by unknown mechanisms, regulate protein production of the target transcript. Different combinations of microRNAs are expressed in different cell types and may coordinately regulate cell-specific target genes. Here, we present PicTar, a computational method for identifying common targets of microRNAs. Statistical tests using genome-wide alignments of eight vertebrate genomes, PicTar's ability to specifically recover published microRNA targets, and experimental validation of seven predicted targets suggest that PicTar has an excellent success rate in predicting targets for single microRNAs and for combinations of microRNAs. We find that vertebrate microRNAs target, on average, roughly 200 transcripts each. Furthermore, our results suggest widespread coordinate control executed by microRNAs. In particular, we experimentally validate common regulation of Mtpn by miR-375, miR-124 and let-7b and thus provide evidence for coordinate microRNA control in mammals.

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Combinatorial microRNA target predictions

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