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A positive, growth-based PAM screen identifies noncanonical motifs recognized by the S. pyogenes Cas9.


ABSTRACT: CRISPR technologies have overwhelmingly relied on the Streptococcus pyogenes Cas9 (SpyCas9), with its consensus NGG and less preferred NAG and NGA protospacer-adjacent motifs (PAMs). Here, we report that SpyCas9 also recognizes sequences within an N(A/C/T)GG motif. These sequences were identified on the basis of preferential enrichment in a growth-based screen in Escherichia coli. DNA binding, cleavage, and editing assays in bacteria and human cells validated recognition, with activities paralleling those for NAG(A/C/T) PAMs and dependent on the first two PAM positions. Molecular-dynamics simulations and plasmid-clearance assays with mismatch-intolerant variants supported induced-fit recognition of an extended PAM by SpyCas9 rather than recognition of NGG with a bulged R-loop. Last, the editing location for SpyCas9-derived base editors could be shifted by one nucleotide by selecting between (C/T)GG and adjacent N(C/T)GG PAMs. SpyCas9 and its enhanced variants thus recognize a larger repertoire of PAMs, with implications for precise editing, off-target predictions, and CRISPR-based immunity.

SUBMITTER: Collias D 

PROVIDER: S-EPMC7439565 | biostudies-literature | 2020 Jul

REPOSITORIES: biostudies-literature

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A positive, growth-based PAM screen identifies noncanonical motifs recognized by the <i>S. pyogenes</i> Cas9.

Collias D D   Leenay R T RT   Slotkowski R A RA   Zuo Z Z   Collins S P SP   McGirr B A BA   Liu J J   Beisel C L CL  

Science advances 20200715 29


CRISPR technologies have overwhelmingly relied on the <i>Streptococcus pyogenes</i> Cas9 (SpyCas9), with its consensus NGG and less preferred NAG and NGA protospacer-adjacent motifs (PAMs). Here, we report that SpyCas9 also recognizes sequences within an N(A/C/T)GG motif. These sequences were identified on the basis of preferential enrichment in a growth-based screen in <i>Escherichia coli</i>. DNA binding, cleavage, and editing assays in bacteria and human cells validated recognition, with acti  ...[more]

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