Publication | Open Access
Transcriptome-wide discovery of coding and noncoding RNA-binding proteins
172
Citations
62
References
2018
Year
Systems BiologyBiochemistryUnknown RbpsNatural SciencesRna Binding ProteinsTranscriptome-wide DiscoveryClick ReactionRna BiologyMolecular BiologyMedicineRna-binding ProteinsTranscriptomicsGene ExpressionProteomicsFunctional GenomicsRna ProcessingTranscription RegulationNon-coding Rna
Transcriptome-wide identification of RNA-binding proteins (RBPs) is a prerequisite for understanding the posttranscriptional gene regulation networks. However, proteomic profiling of RBPs has been mostly limited to polyadenylated mRNA-binding proteins, leaving RBPs on nonpoly(A) RNAs, including most noncoding RNAs (ncRNAs) and pre-mRNAs, largely undiscovered. Here we present a click chemistry-assisted RNA interactome capture (CARIC) strategy, which enables unbiased identification of RBPs, independent of the polyadenylation state of RNAs. CARIC combines metabolic labeling of RNAs with an alkynyl uridine analog and in vivo RNA-protein photocross-linking, followed by click reaction with azide-biotin, affinity enrichment, and proteomic analysis. Applying CARIC, we identified 597 RBPs in HeLa cells, including 130 previously unknown RBPs. These newly discovered RBPs can likely bind ncRNAs, thus uncovering potential involvement of ncRNAs in processes previously unknown to be ncRNA-related, such as proteasome function and intermediary metabolism. The CARIC strategy should be broadly applicable across various organisms to complete the census of RBPs.
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