Deletion of One Nucleotide within the Homonucleotide Tract Present in the
            <i>hsdS</i>
            Gene Alters the DNA Sequence Specificity of Type I Restriction-Modification System NgoAV

Adamczyk-Popławska, Monika; Lower, Michal; Piekarowicz, Andrzej

doi:10.1128/jb.05672-11

Cited by 27 publications

(53 citation statements)

References 47 publications

(74 reference statements)

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“…We predict that variation in length of SSRs located in hsdM genes likely leads to ON-OFF switching, akin to that seen with Type III mod genes 9,17 ( Figure 5). SSR variation has been demonstrated to result in a switch between specificities due to expression of a full-length HsdS or truncated HsdS has been demonstrated in N. gonorrhoeae, 31 and full and extended versions of HsdS proteins are expressed by M. haemolytica commensurate with SSR tract variation (this work). For example, SSR tracts in hsdS genes invariably occur between two TRDs, which leads to expression of multiple HsdS variants, be they full length two TRD proteins, truncated HsdS subunits which then dimerise to form a functional HsdS protein, or an extended three TRD containing HsdS protein (Figure 1 and Figure 3).…”

Section: Hsds and Hsdm Genes Contain Ssr Tracts In Different Regionmentioning

confidence: 73%

“…Type I R-M systems that phase vary via changes in the length of SSRs are less well studied. The full-length and truncated HsdS proteins have differing methyltransferase specificities, 31 with two of these truncated HsdS subunits combining to participate in sequence recognition 32 (see Figure 1A). An hsdM gene containing a pentanucleotide SSR tract was identified in H. influenza, 30 and we previously noted changes in the length of this tract in multiple nontypeable H. influenzae (NTHi) isolates from paired samples taken from the human nasopharynx and middle ear during cases of otitis media.…”

Section: Introductionmentioning

confidence: 99%

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DNA sequence repeats identify numerous Type I restriction‐modification systems that are potential epigenetic regulators controlling phase‐variable regulons; phasevarions

et al. 2019

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Over recent years several examples of randomly switching methyltransferases, associated with Type III restriction-modification (R-M) systems, have been described in pathogenic bacteria. In every case examined, changes in simple DNA sequence repeats result in variable methyltransferase expression and result in global changes in gene expression, and differentiation of the bacterial cell into distinct phenotypes.These epigenetic regulatory systems are called phasevarions, phase-variable regulons, and are widespread in bacteria, with 17.4% of Type III R-M system containing simple DNA sequence repeats. A distinct, recombination-driven random switching system has also been described in Streptococci in Type I R-M systems that also regulate gene expression. Here, we interrogate the most extensive and well-curated database of R-M systems, REBASE, by searching for all possible simple DNA sequence repeats in the hsdRMS genes that encode Type I R-M systems. We report that 7.9% of hsdS, 2% of hsdM, and of 4.3% of hsdR genes contain simple sequence repeats that are capable of mediating phase variation. Phase variation of both hsdM and hsdS genes will lead to differential methyltransferase expression or specificity, and thereby the potential to control phasevarions. These data suggest that in addition to well characterized phasevarions controlled by Type III mod genes, and the previously described Streptococcal Type I R-M systems that switch via recombination, approximately 10% of all Type I R-M systems surveyed herein have independently evolved the ability to randomly switch expression via simple DNA sequence repeats. K E Y W O R D Sbacterial pathogenesis, epigenetics, phase variation, phasevarion, R-M systems | 1039 ATACK eT Al.

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Section: Hsds and Hsdm Genes Contain Ssr Tracts In Different Regionmentioning

confidence: 73%

Section: Introductionmentioning

confidence: 99%

DNA sequence repeats identify numerous Type I restriction‐modification systems that are potential epigenetic regulators controlling phase‐variable regulons; phasevarions

et al. 2019

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“…Analysis indicated the gene encoding the specificity subunit ( hsdS ) of the restriction-modification system contained a frameshift mutation. However, a truncated hsdS can still potentially translate and dimerize into a functional HsdS subunit, albeit with an altered DNA specificity [66]-[68]. Nevertheless, the presence of a DNA restriction-modification system in this genomic island may act as a ‘selfish’ genetic element to ensure its dissemination [69] and/or may function in bacteriophage defence and hindrance of lateral gene transfer [70].…”

Section: Resultsmentioning

confidence: 99%

The Complete Genome and Phenome of a Community-Acquired Acinetobacter baumannii

et al. 2013

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Many sequenced strains of Acinetobacter baumannii are established nosocomial pathogens capable of resistance to multiple antimicrobials. Community-acquired A. baumannii in contrast, comprise a minor proportion of all A. baumannii infections and are highly susceptible to antimicrobial treatment. However, these infections also present acute clinical manifestations associated with high reported rates of mortality. We report the complete 3.70 Mbp genome of A. baumannii D1279779, previously isolated from the bacteraemic infection of an Indigenous Australian; this strain represents the first community-acquired A. baumannii to be sequenced. Comparative analysis of currently published A. baumannii genomes identified twenty-four accessory gene clusters present in D1279779. These accessory elements were predicted to encode a range of functions including polysaccharide biosynthesis, type I DNA restriction-modification, and the metabolism of novel carbonaceous and nitrogenous compounds. Conversely, twenty genomic regions present in previously sequenced A. baumannii strains were absent in D1279779, including gene clusters involved in the catabolism of 4-hydroxybenzoate and glucarate, and the A. baumannii antibiotic resistance island, known to bestow resistance to multiple antimicrobials in nosocomial strains. Phenomic analysis utilising the Biolog Phenotype Microarray system indicated that A. baumannii D1279779 can utilise a broader range of carbon and nitrogen sources than international clone I and clone II nosocomial isolates. However, D1279779 was more sensitive to antimicrobial compounds, particularly beta-lactams, tetracyclines and sulphonamides. The combined genomic and phenomic analyses have provided insight into the features distinguishing A. baumannii isolated from community-acquired and nosocomial infections.

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“…Interestingly, a recent study uncovered a variable poly-G tract within the 3′ end of hsdS NgoAV1 in N. gonorrhoeae, and loss of a guanine in that tract restores the fusion of the hsdS NgoAV1 and hsdS NgoAV2 genes, resulting in the generation of a new HsdS NgoAVD protein, responsible for a novel NgoAV R-M system, termed 'NgoAVD'. The NgoAVD system has a modified DNA recognition specificity, thereby conferring an altered susceptibility to various phages (Adamczyk-Poplawska et al, 2011).…”

Section: Trs Within Genes Involved In Restrictionmodification Systemsmentioning

confidence: 99%

The role of variable DNA tandem repeats in bacterial adaptation

2014

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DNA tandem repeats (TRs), also designated as satellite DNA, are inter- or intragenic nucleotide sequences that are repeated two or more times in a head-to-tail manner. Because TR tracts are prone to strand-slippage replication and recombination events that cause the TR copy number to increase or decrease, loci containing TRs are hypermutable. An increasing number of examples illustrate that bacteria can exploit this instability of TRs to reversibly shut down or modulate the function of specific genes, allowing them to adapt to changing environments on short evolutionary time scales without an increased overall mutation rate. In this review, we discuss the prevalence and distribution of inter- and intragenic TRs in bacteria and the mechanisms of their instability. In addition, we review evidence demonstrating a role of TR variations in bacterial adaptation strategies, ranging from immune evasion and tissue tropism to the modulation of environmental stress tolerance. Nevertheless, while bioinformatic analysis reveals that most bacterial genomes contain a few up to several dozens of intra- and intergenic TRs, only a small fraction of these have been functionally studied to date.

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Deletion of One Nucleotide within the Homonucleotide Tract Present in the hsdS Gene Alters the DNA Sequence Specificity of Type I Restriction-Modification System NgoAV

Cited by 27 publications

References 47 publications

DNA sequence repeats identify numerous Type I restriction‐modification systems that are potential epigenetic regulators controlling phase‐variable regulons; phasevarions

DNA sequence repeats identify numerous Type I restriction‐modification systems that are potential epigenetic regulators controlling phase‐variable regulons; phasevarions

The Complete Genome and Phenome of a Community-Acquired Acinetobacter baumannii

The role of variable DNA tandem repeats in bacterial adaptation

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