Novel molecular requirements for CRISPR RNA-guided transposition

Author:

Walker Matt W G1ORCID,Klompe Sanne E2ORCID,Zhang Dennis J1ORCID,Sternberg Samuel H2ORCID

Affiliation:

1. Department of Biological Sciences, Columbia University , New York , NY  10027, USA

2. Department of Biochemistry and Molecular Biophysics, Columbia University , New York , NY  10032, USA

Abstract

AbstractCRISPR-associated transposases (CASTs) direct DNA integration downstream of target sites using the RNA-guided DNA binding activity of nuclease-deficient CRISPR-Cas systems. Transposition relies on several key protein-protein and protein-DNA interactions, but little is known about the explicit sequence requirements governing efficient transposon DNA integration activity. Here, we exploit pooled library screening and high-throughput sequencing to reveal novel sequence determinants during transposition by the Type I-F Vibrio cholerae CAST system (VchCAST). On the donor DNA, large transposon end libraries revealed binding site nucleotide preferences for the TnsB transposase, as well as an additional conserved region that encoded a consensus binding site for integration host factor (IHF). Remarkably, we found that VchCAST requires IHF for efficient transposition, thus revealing a novel cellular factor involved in CRISPR-associated transpososome assembly. On the target DNA, we uncovered preferred sequence motifs at the integration site that explained previously observed heterogeneity with single-base pair resolution. Finally, we exploited our library data to design modified transposon variants that enable in-frame protein tagging. Collectively, our results provide new clues about the assembly and architecture of the paired-end complex formed between TnsB and the transposon DNA, and inform the design of custom payload sequences for genome engineering applications with CAST systems.

Funder

National Institutes of Health

Pew Biomedical Scholars Program

Alfred Sloan Foundation Research Fellowship

Irma T. Hirschl Career Scientist Award

National Science Foundation

Sternberg Lab, Columbia University

Publisher

Oxford University Press (OUP)

Subject

Genetics

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