2016
DOI: 10.1261/rna.058115.116
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Quantifying RNA binding sites transcriptome-wide using DO-RIP-seq

Abstract: RNA-binding proteins (RBPs) and noncoding RNAs orchestrate post-transcriptional processes through the recognition of specific sites on targeted transcripts. Thus, understanding the connection between binding to specific sites and active regulation of the whole transcript is essential. Many immunoprecipitation techniques have been developed that identify either whole transcripts or binding sites of RBPs on each transcript using cell lysates. However, none of these methods simultaneously measures the strength of… Show more

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Cited by 49 publications
(57 citation statements)
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“…This step is followed by immunoprecipitations with antibodies against the RBP of interest, while using non-specific antibodies in parallel to measure background and account for overall transcript abundance. As described here, DO-RIP-seq was developed using the RBP ELAVL1/HuR as a test case, and the experiments yielded probabilistic measures (log of odds scores, LOD) for binding sites in HEK293 cells [25], and for XIST long non-coding RNA in mouse trophoblasts [26]. HuR binding site LOD scores correlated with binding strength and motif preference [25].…”
Section: Introductionmentioning
confidence: 99%
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“…This step is followed by immunoprecipitations with antibodies against the RBP of interest, while using non-specific antibodies in parallel to measure background and account for overall transcript abundance. As described here, DO-RIP-seq was developed using the RBP ELAVL1/HuR as a test case, and the experiments yielded probabilistic measures (log of odds scores, LOD) for binding sites in HEK293 cells [25], and for XIST long non-coding RNA in mouse trophoblasts [26]. HuR binding site LOD scores correlated with binding strength and motif preference [25].…”
Section: Introductionmentioning
confidence: 99%
“…As described here, DO-RIP-seq was developed using the RBP ELAVL1/HuR as a test case, and the experiments yielded probabilistic measures (log of odds scores, LOD) for binding sites in HEK293 cells [25], and for XIST long non-coding RNA in mouse trophoblasts [26]. HuR binding site LOD scores correlated with binding strength and motif preference [25]. Also DO-RIP-seq analysis of whole transcript association distinguished functional groups of messages and enriched gene sets [25].…”
Section: Introductionmentioning
confidence: 99%
See 3 more Smart Citations