RT Journal Article
SR Electronic
T1 SNP analysis implicates role of cytosine methylation in introducing consequential mutations in <em>Vibrio cholerae</em> genomes
JF bioRxiv
FD Cold Spring Harbor Laboratory
SP 070839
DO 10.1101/070839
A1 Mohak Sharda
A1 Aswin Sai Narain Seshasayee
A1 Supriya Khedkar
YR 2016
UL http://biorxiv.org/content/early/2016/08/22/070839.abstract
AB Epigenetic modifications play a key role in gene regulation and in recognition of self DNA in bacteria. In-spite of their positive role in cell survival, modifications like cytosine methylation incur a mutational cost. Cytosine methylation, specifically 5-methylcytosine, is prone to hydrolytic deamination which leads to C → T and G → A transitions. Here, we first study the abundance of mutagenic cytosine methylation target motifs and show that bacteria like Vibrio cholerae might use motif avoidance as a strategy to minimize the mutational effect of deamination of methylated cytosine. Second by performing SNP analysis on whole genome sequence data from Vibrio cholerae patient isolates we show a) high abundance of cytosine methylation-dependent mutations in the cytosine methylation target motif RCCGGY, b) 95% of these C → T and G → A transitions in the coding region lead to non-synonymous substitutions and c) many of these transitions are associated with membrane proteins and are implicated in virulence. Thus, our SNP analysis of V. cholerae genomes implicates the role of cytosine methylation in generating genotypic diversity with adaptive potential.