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Casposase structure and the mechanistic link between DNA transposition and spacer acquisition by CRISPR-Cas.


ABSTRACT: Key to CRISPR-Cas adaptive immunity is maintaining an ongoing record of invading nucleic acids, a process carried out by the Cas1-Cas2 complex that integrates short segments of foreign genetic material (spacers) into the CRISPR locus. It is hypothesized that Cas1 evolved from casposases, a novel class of transposases. We show here that the Methanosarcina mazei casposase can integrate varied forms of the casposon end in vitro, and recapitulates several properties of CRISPR-Cas integrases including site-specificity. The X-ray structure of the casposase bound to DNA representing the product of integration reveals a tetramer with target DNA bound snugly between two dimers in which single-stranded casposon end binding resembles that of spacer 3'-overhangs. The differences between transposase and CRISPR-Cas integrase are largely architectural, and it appears that evolutionary change involved changes in protein-protein interactions to favor Cas2 binding over tetramerization; this in turn led to preferred integration of single spacers over two transposon ends.

SUBMITTER: Hickman AB 

PROVIDER: S-EPMC6977970 | biostudies-literature | 2020 Jan

REPOSITORIES: biostudies-literature

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Casposase structure and the mechanistic link between DNA transposition and spacer acquisition by CRISPR-Cas.

Hickman Alison B AB   Kailasan Shweta S   Genzor Pavol P   Haase Astrid D AD   Dyda Fred F  

eLife 20200108


Key to CRISPR-Cas adaptive immunity is maintaining an ongoing record of invading nucleic acids, a process carried out by the Cas1-Cas2 complex that integrates short segments of foreign genetic material (spacers) into the CRISPR locus. It is hypothesized that Cas1 evolved from casposases, a novel class of transposases. We show here that the <i>Methanosarcina mazei</i> casposase can integrate varied forms of the casposon end in vitro, and recapitulates several properties of CRISPR-Cas integrases i  ...[more]

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