Tomado de:
Multiple mechanisms for CRISPR–Cas inhibition by anti-CRISPR protein
- Nature
- doi:10.1038/nature15254
- Received
- Accepted
- Published online
jueves, 24 de septiembre de 2015
Los virus se defienden de nuevo
The battle for survival between bacteria and the viruses that infect
them (phages) has led to the evolution of many bacterial defence systems
and phage-encoded antagonists of these systems. Clustered regularly
interspaced short palindromic repeats (CRISPR) and the CRISPR-associated
(cas) genes comprise an adaptive immune system that is one of
the most widespread means by which bacteria defend themselves against
phages. We identified the first examples of proteins produced by phages that inhibit a CRISPR–Cas system. Here we performed biochemical and in vivo
investigations of three of these anti-CRISPR proteins, and show that
each inhibits CRISPR–Cas activity through a distinct mechanism. Two
block the DNA-binding activity of the CRISPR–Cas complex, yet do this by
interacting with different protein subunits, and using steric or
non-steric modes of inhibition. The third anti-CRISPR protein operates
by binding to the Cas3 helicase–nuclease and preventing its recruitment
to the DNA-bound CRISPR–Cas complex. In vivo, this anti-CRISPR
can convert the CRISPR–Cas system into a transcriptional repressor,
providing the first example—to our knowledge—of modulation of CRISPR–Cas
activity by a protein interactor. The diverse sequences and mechanisms
of action of these anti-CRISPR proteins imply an independent evolution,
and foreshadow the existence of other means by which proteins may alter
CRISPR–Cas function.
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