Phase variation of a signal transduction system controls<i>Clostridioides difficile</i>colony morphology, motility, and virulence

Garrett, Elizabeth M.; Sekulović, Ognjen; Wetzel, Daniela; Jones, Joshua B.; Edwards, Adrianne N.; Vargas-Cuebas, Germán; McBride, Shonna M.; Tamayo, Rita

doi:10.1101/690230

Cited by 7 publications

(11 citation statements)

References 85 publications

(115 reference statements)

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“…Another c-di-GMP-responsive riboswitch, Cdi2_2, precedes the genes encoding the signal transduction system CmrRST in C. difficile , where CmrS is a putative histidine kinase, and CmrR and CmrT are two predicted response regulators [ 181 ]. Binding of c-di-GMP to Cdi2_2 positively affects cmrRST expression [ 182 ], most likely through anti-termination of transcription. Interestingly, cmrRST is also regulated by phase variation with an invertible DNA sequence, the cmr switch, located upstream of the corresponding genes [ 182 ].…”

Section: Srnas Regulating Host-pathogen Interactionsmentioning

confidence: 99%

“…Binding of c-di-GMP to Cdi2_2 positively affects cmrRST expression [ 182 ], most likely through anti-termination of transcription. Interestingly, cmrRST is also regulated by phase variation with an invertible DNA sequence, the cmr switch, located upstream of the corresponding genes [ 182 ]. CmrRST modulates colony morphology (rough or smooth) with the activation of cmrRST expression by c-di-GMP binding to Cdi2_2, promoting the development of rough colonies.…”

Section: Srnas Regulating Host-pathogen Interactionsmentioning

confidence: 99%

“…CmrRST also inversely regulates motility and surface migration and promotes bacterial chaining. Importantly, a cmrR deletion mutant is unable to colonize the intestinal tract and has a strong virulence defect in the hamster model of infection [ 182 ].…”

Section: Srnas Regulating Host-pathogen Interactionsmentioning

confidence: 99%

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Interplay between Regulatory RNAs and Signal Transduction Systems during Bacterial Infection

Piattelli

Peltier

Soutourina

2020

Genes

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The ability of pathogenic bacteria to stably infect the host depends on their capacity to respond and adapt to the host environment and on the efficiency of their defensive mechanisms. Bacterial envelope provides a physical barrier protecting against environmental threats. It also constitutes an important sensory interface where numerous sensing systems are located. Signal transduction systems include Two-Component Systems (TCSs) and alternative sigma factors. These systems are able to sense and respond to the ever-changing environment inside the host, altering the bacterial transcriptome to mitigate the impact of the stress. The regulatory networks associated with signal transduction systems comprise small regulatory RNAs (sRNAs) that can be directly involved in the expression of virulence factors. The aim of this review is to describe the importance of TCS- and alternative sigma factor-associated sRNAs in human pathogens during infection. The currently available genome-wide approaches for studies of TCS-regulated sRNAs will be discussed. The differences in the signal transduction mediated by TCSs between bacteria and higher eukaryotes and the specificity of regulatory RNAs for their targets make them appealing targets for discovery of new strategies to fight against multi-resistant bacteria.

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Section: Srnas Regulating Host-pathogen Interactionsmentioning

confidence: 99%

Section: Srnas Regulating Host-pathogen Interactionsmentioning

confidence: 99%

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Interplay between Regulatory RNAs and Signal Transduction Systems during Bacterial Infection

Piattelli

Peltier

Soutourina

2020

Genes

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“…difficile NAP1/B1/027 ribotype strain R20291, and an eighth in several 017 ribotype strains [ 43 , 44 ]. The identified sequences were shown to undergo inversion, and the sequence upstream of the cmrRST operon was confirmed to regulate expression of the downstream genes in a manner consistent with phase variation [ 44 , 45 ]. We subsequently showed that site-specific recombination also mediates phase variation of flagella and toxins by inversion of a genetic sequence called the “flagellar switch” [ 33 ].…”

Section: Introductionmentioning

confidence: 99%

“…difficile R20291 in broth culture consists of a heterogeneous population of flg ON and OFF bacteria. Notably, RecV is also required for inversion of the cwpV switch, as well as two of the other identified invertible sequences including one shown to impact multiple phenotypes including virulence [ 40 , 44 , 45 ].…”

Section: Introductionmentioning

confidence: 99%

Rho factor mediates flagellum and toxin phase variation and impacts virulence in Clostridioides difficile

et al. 2020

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The intestinal pathogen Clostridioides difficile exhibits heterogeneity in motility and toxin production. This phenotypic heterogeneity is achieved through phase variation by site-specific recombination via the DNA recombinase RecV, which reversibly inverts the "flagellar switch" upstream of the flgB operon. A recV mutation prevents flagellar switch inversion and results in phenotypically locked strains. The orientation of the flagellar switch influences expression of the flgB operon post-transcription initiation, but the specific molecular mechanism is unknown. Here, we report the isolation and characterization of spontaneous suppressor mutants in the non-motile, non-toxigenic recV flg OFF background that regained motility and toxin production. The restored phenotypes corresponded with increased expression of flagellum and toxin genes. The motile suppressor mutants contained singlenucleotide polymorphisms (SNPs) in rho, which encodes the bacterial transcription terminator Rho factor. Analyses using transcriptional reporters indicate that Rho contributes to heterogeneity in flagellar gene expression by preferentially terminating transcription of flg OFF mRNA within the 5' leader sequence. Additionally, Rho is important for initial colonization of the intestine in a mouse model of infection, which may in part be due to the sporulation and growth defects observed in the rho mutants. Together these data implicate Rho factor as a regulator of gene expression affecting phase variation of important virulence factors of C. difficile.

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Novel drivers of virulence inClostridioides difficileidentified via context-specific metabolic network analysis

Jenior

Leslie

Powers

et al. 2020

Preprint

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Clostridioides difficile is a Gram-positive, sporulating anaerobe that has become the leading cause of hospital-acquired infections. Over the previous decade, many studies have demonstrated the importance of metabolism in numerous aspects of C. difficile biology from initial colonization to regulation of virulence factors. Additionally, due to growing threats of antibiotic resistance and recurrent infection, targeting components of metabolism presents a novel possible approach to combat this infection. In the past, genome-scale metabolic network analysis of bacteria has enabled systematic investigation of the genetic and metabolic properties that potentially contribute to downstream phenotypes as well as prediction of outcome from perturbations to these pathways. These predictions ultimately create a platform for high-throughput identification and screening of metabolic targets prior to laboratory testing. To accomplish these goals in C. difficile, we constructed highly-curated genome-scale metabolic network reconstructions (GENREs) for a well-studied laboratory strain of the pathogen (str. 630) as well as a more recently characterized hyper-virulent isolate (str. R20291). These computational modeling platforms account for key components of C. difficile core metabolism and nutrient acquisition systems to recapitulate metabolic behaviors within the complex milieu of the gut. Simulating the impact of single-gene deletions resulted in accuracies of ~89.9% for both GENREs compared with transposon mutant libraries. Further analysis of both strains also revealed significant correlations between in silico and experimentally measured growth in carbon source utilization screens (p-values ≤ 0.002), with positive predictive values of ~95.0%. Subsequently, we generated context-specific models by integrating transcriptomic data from C. difficile grown in vitro or during in vivo infection. Simulations also predicted the consistent inverse patterns of carbohydrate and amino acid catabolism that corresponded with differential virulence factor expression measured experimentally. Collectively, our results indicate that GENRE-based analyses of C. difficile are an effective means for gaining novel insight into metabolism as it relates to pathogenesis and provides a platform for the identification of novel therapeutic targets.

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Phase variation of a signal transduction system controlsClostridioides difficilecolony morphology, motility, and virulence

Cited by 7 publications

References 85 publications

Interplay between Regulatory RNAs and Signal Transduction Systems during Bacterial Infection

Interplay between Regulatory RNAs and Signal Transduction Systems during Bacterial Infection

Rho factor mediates flagellum and toxin phase variation and impacts virulence in Clostridioides difficile

Novel drivers of virulence inClostridioides difficileidentified via context-specific metabolic network analysis

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