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Real-time observation of DNA recognition and rejection by the RNA-guided endonuclease Cas9.


ABSTRACT: Binding specificity of Cas9-guide RNA complexes to DNA is important for genome-engineering applications; however, how mismatches influence target recognition/rejection kinetics is not well understood. Here we used single-molecule FRET to probe real-time interactions between Cas9-RNA and DNA targets. The bimolecular association rate is only weakly dependent on sequence; however, the dissociation rate greatly increases from <0.006?s(-1) to >2?s(-1) upon introduction of mismatches proximal to protospacer-adjacent motif (PAM), demonstrating that mismatches encountered early during heteroduplex formation induce rapid rejection of off-target DNA. In contrast, PAM-distal mismatches up to 11 base pairs in length, which prevent DNA cleavage, still allow formation of a stable complex (dissociation rate <0.006?s(-1)), suggesting that extremely slow rejection could sequester Cas9-RNA, increasing the Cas9 expression level necessary for genome-editing, thereby aggravating off-target effects. We also observed at least two different bound FRET states that may represent distinct steps in target search and proofreading.

SUBMITTER: Singh D 

PROVIDER: S-EPMC5027287 | biostudies-literature | 2016 Sep

REPOSITORIES: biostudies-literature

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Real-time observation of DNA recognition and rejection by the RNA-guided endonuclease Cas9.

Singh Digvijay D   Sternberg Samuel H SH   Fei Jingyi J   Doudna Jennifer A JA   Ha Taekjip T  

Nature communications 20160914


Binding specificity of Cas9-guide RNA complexes to DNA is important for genome-engineering applications; however, how mismatches influence target recognition/rejection kinetics is not well understood. Here we used single-molecule FRET to probe real-time interactions between Cas9-RNA and DNA targets. The bimolecular association rate is only weakly dependent on sequence; however, the dissociation rate greatly increases from <0.006 s(-1) to >2 s(-1) upon introduction of mismatches proximal to proto  ...[more]

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