Inter-viral conflicts that exploit host CRISPR immune systems of Sulfolobus

Susanne Erdmann, Sven Le Moine Bauer, Roger Antony Garrett

57 Citations (Scopus)
1352 Downloads (Pure)

Abstract

Infection of Sulfolobus islandicusREY15A with mixtures of different Sulfolobus viruses, including STSV2, did not induce spacer acquisition by the host CRISPR immune system. However, coinfection with the tailed fusiform viruses SMV1 and STSV2 generated hyperactive spacer acquisition in both CRISPR loci, exclusively from STSV2, with the resultant loss of STSV2 but not SMV1. SMV1 was shown to activate adaptation while itself being resistant to CRISPR-mediated adaptation and DNA interference. Exceptionally, a single clone S-1 isolated from an SMV1+STSV2-infected culture, that carried STSV2-specific spacers and had lost STSV2 but not SMV1, acquired spacers from SMV1. This effect was also reproducible on reinfecting wild-type host cells with a variant SMV1 isolated from the S-1 culture. The SMV1 variant lacked a virion protein ORF114 that was shown to bind DNA. This study also provided evidence for: (i) limits on the maximum sizes of CRISPR loci; (ii) spacer uptake strongly retarding growth of infected cultures; (iii) protospacer selection being essentially random and non-directional, and (iv) the reversible uptake of spacers from STSV2 and SMV1. A hypothesis is presented to explain the interactive conflicts between SMV1 and the host CRISPR immune system.

Original languageEnglish
JournalMolecular Microbiology
Volume91
Issue number5
Pages (from-to)900-917
Number of pages18
ISSN1365-2958
DOIs
Publication statusPublished - Mar 2014

Fingerprint

Dive into the research topics of 'Inter-viral conflicts that exploit host CRISPR immune systems of Sulfolobus'. Together they form a unique fingerprint.

Cite this