PT  - JOURNAL ARTICLE
AU  - Daniel Dominguez
AU  - Peter Freese
AU  - Maria Alexis
AU  - Amanda Su
AU  - Myles Hochman
AU  - Tsultrim Palden
AU  - Cassandra Bazile
AU  - Nicole J Lambert
AU  - Eric L Van Nostrand
AU  - Gabriel A. Pratt
AU  - Gene W. Yeo
AU  - Brenton R. Graveley
AU  - Christopher B. Burge
TI  - Sequence, Structure and Context Preferences of Human RNA Binding Proteins
AID  - 10.1101/201996
DP  - 2017 Jan 01
TA  - bioRxiv
PG  - 201996
4099  - http://biorxiv.org/content/early/2017/10/12/201996.short
4100  - http://biorxiv.org/content/early/2017/10/12/201996.full
AB  - Production of functional cellular RNAs involves multiple processing and regulatory steps principally mediated by RNA binding proteins (RBPs). Here we present the affinity landscapes of 78 human RBPs using an unbiased assay that determines the sequence, structure, and context preferences of an RBP in vitro from deep sequencing of bound RNAs. Analyses of these data revealed several interesting patterns, including unexpectedly low diversity of RNA motifs, implying frequent convergent evolution of binding specificity toward a relatively small set of RNA motifs, many with low compositional complexity. Offsetting this trend, we observed extensive preferences for contextual features outside of core RNA motifs, including spaced “bipartite” motifs, biased flanking nucleotide context, and bias away from or towards RNA structure. These contextual features are likely to enable targeting of distinct subsets of transcripts by different RBPs that recognize the same core motif. Our results enable construction of “RNA maps” of RBP activity without requiring crosslinking-based assays, and provide unprecedented depth of information on the interaction of RBPs with RNA.