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Allele-specific binding of RNA-binding proteins reveals functional genetic variants in the RNA.

Nature communications · 2019 · Vol. 10 (1) · pp. 1338

Abstract

Allele-specific protein-RNA binding is an essential aspect that may reveal functional genetic variants (GVs) mediating post-transcriptional regulation. Recently, genome-wide detection of in vivo binding of RNA-binding proteins is greatly facilitated by the enhanced crosslinking and immunoprecipitation (eCLIP) method. We developed a new computational approach, called BEAPR, to identify allele-specific binding (ASB) events in eCLIP-Seq data. BEAPR takes into account crosslinking-induced sequence propensity and variations between replicated experiments. Using simulated and actual data, we show that BEAPR largely outperforms often-used count analysis methods. Importantly, BEAPR overcomes the inherent overdispersion problem of these methods. Complemented by experimental validations, we demonstrate that the application of BEAPR to ENCODE eCLIP-Seq data of 154 proteins helps to predict functional GVs that alter splicing or mRNA abundance. Moreover, many GVs with ASB patterns have known disease relevance. Overall, BEAPR is an effective method that helps to address the outstanding challenge of functional interpretation of GVs.

Publication Types

["Journal Article", "Research Support, N.I.H., Extramural", "Research Support, Non-U.S. Gov't"]

Keywords

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MeSH Terms

["3' Untranslated Regions", "Alleles", "Amino Acid Motifs", "Base Sequence", "Computational Biology", "Computer Simulation", "Disease", "Genetic Predisposition to Disease", "Genetic Variation", "Hep G2 Cells", "Humans", "K562 Cells", "Polymorphism, Single Nucleotide", "Protein Binding", "Quantitative Trait Loci", "RNA", "RNA Helicases", "RNA Splicing", "RNA, Messenger", "RNA-Binding Proteins", "Reproducibility of Results", "Trans-Activators"]

Funding

R00 HG009530 NHGRI NIH HHS (United States)
U01 HG009417 NHGRI NIH HHS (United States)
K99 HG009530 NHGRI NIH HHS (United States)
T32 GM087237 NIGMS NIH HHS (United States)
U54 HG007005 NHGRI NIH HHS (United States)
R01 AG056476 NIA NIH HHS (United States)
U54HG007005 NIH HHS (United States)
U01HG009417 NIH HHS (United States)
R01 HG006264 NHGRI NIH HHS (United States)
U01 CA204695 NCI NIH HHS (United States)
R01AG056476 NIH HHS (United States)
R01HG006264 NIH HHS (United States)