The recombination initiation functions DprA and RecFOR suppress microindel mutations in Acinetobacter baylyi ADP1
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https://hdl.handle.net/10037/34973Date
2024-05-17Type
Journal articleTidsskriftartikkel
Peer reviewed
Abstract
Short-Patch Double Illegitimate Recombination (SPDIR) has been recently identified
as a rare mutation mechanism. During SPDIR, ectopic DNA single-strands anneal with
genomic DNA at microhomologies and get integrated during DNA replication, presumably acting as primers for Okazaki fragments. The resulting microindel mutations
are highly variable in size and sequence. In the soil bacterium Acinetobacter baylyi,
SPDIR is tightly controlled by genome maintenance functions including RecA. It is
thought that RecA scavenges DNA single-strands and renders them unable to anneal.
To further elucidate the role of RecA in this process, we investigate the roles of the
upstream functions DprA, RecFOR, and RecBCD, all of which load DNA single-strands
with RecA. Here we show that all three functions suppress SPDIR mutations in the
wildtype to levels below the detection limit. While SPDIR mutations are slightly elevated in the absence of DprA, they are strongly increased in the absence of both DprA
and RecA. This SPDIR-avoiding function of DprA is not related to its role in natural
transformation. These results suggest a function for DprA in combination with RecA
to avoid potentially harmful microindel mutations, and offer an explanation for the
ubiquity of dprA in the genomes of naturally non-transformable bacteria.
Publisher
WileyCitation
Liljegren, Gama, Johnsen, Harms. The recombination initiation functions DprA and RecFOR suppress microindel mutations in Acinetobacter baylyi ADP1. Molecular Microbiology. 2024Metadata
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