Robust single-cell discovery of RNA targets of RNA binding proteins and ribosomes

Author:

Brannan Kristopher1,Chaim Isaac1,Yee Brian1,Marina Ryan1,Lorenz Daniel1,Dong Kevin1,Madrigal Assael1,Yeo Gene1ORCID

Affiliation:

1. University of California San Diego

Abstract

Abstract RNA binding proteins (RBPs) are critical regulators of gene expression and RNA processing that are required for gene function. Yet, the dynamics of RBP regulation in single cells is unknown. To address this gap in understanding, we developed STAMP (Surveying Targets by APOBEC Mediated Profiling), which efficiently detects RBP-RNA interactions. STAMP does not rely on UV-crosslinking or immunoprecipitation and, when coupled with single-cell capture, can identify RBP- and cell type-specific RNA-protein interactions for multiple RBPs and cell types in single-pooled experiments. Pairing STAMP with long-read sequencing also yields RBP target sites for full-length isoforms. Finally, conducting STAMP using small ribosomal subunits (Ribo-STAMP) allows analysis of transcriptome-wide ribosome association in single cells. STAMP enables the study of RBP-RNA interactomes and translational landscapes with unprecedented cellular resolution.

Publisher

Research Square Platform LLC

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