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SRX475870: GSM1334287: PAR-CLIP with T1, replicate 1; Homo sapiens; OTHER
2 ILLUMINA (Illumina HiSeq 2000) runs: 127.3M spots, 6.5G bases, 4.5Gb downloads

Submitted by: NCBI (GEO)
Study: Transcriptome wide identification of Dicer binding in human and C. elegans reveals a variety of substrates (HEK PAR-CLIP)
show Abstracthide Abstract
Dicer is a deeply conserved endoribonuclease with key functions in small RNA biogenesis. Here we employed PAR-CLIP/iPAR-CLIP to identify direct Dicer binding sites in the transcriptomes of human cells and human. We found hundreds of novel miRNAs and non-canonical Dicer substrates with high sensitivity. Small RNA production depended on structure of the binding site and is globally biased towards the 5'' arm of hairpins. Unexpectedly, in both species Dicer bound numerous hairpins inside mRNAs without observable small RNA production. Our data revealed ~100 mRNAs of protein coding genes to be targeted in both human and worm. These mRNAs significantly overlapped with the RNAi pathway. We also, unexpectedly, found that mitochondrial transcripts are Dicer targets in both species. We demonstrate functional consequences of Dicer binding by perturbation analysis. Taken together,we provide the first genome-wide catalog of direct Dicer targets. Our results suggest widespread function outside of miRNA biogenesis. Overall design: PAR-CLIP basically as described previously (Hafner et al. 2010).
Sample: PAR-CLIP with T1, replicate 1
SAMN02664656 • SRS561614 • All experiments • All runs
Organism: Homo sapiens
Library:
Instrument: Illumina HiSeq 2000
Strategy: OTHER
Source: TRANSCRIPTOMIC
Selection: other
Layout: SINGLE
Construction protocol: PAR-CLIP (Hafner et al. 2010) Illumina small RNA
Experiment attributes:
GEO Accession: GSM1334287
Links:
Runs: 2 runs, 127.3M spots, 6.5G bases, 4.5Gb
Run# of Spots# of BasesSizePublished
SRR117663812,712,587648.3M473.9Mb2014-11-21
SRR1176639114,584,0295.8G4Gb2014-11-21

ID:
664949

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