DNase Sda1 provides selection pressure for a switch to invasive group A streptococcal infection.

Walker, Mark J; Hollands, Andrew; Sanderson-Smith, Martina L; Cole, Jason N; Kirk, Joshua K; Henningham, Anna; McArthur, Jason D; Dinkla, Katrin; Aziz, Ramy K; Kansal, Rita G; Simpson, Amelia J; Buchanan, John T; Chhatwal, Gursharan S; Kotb, Malak; Nizet, Victor

dc.contributor.author	Walker, Mark J
dc.contributor.author	Hollands, Andrew
dc.contributor.author	Sanderson-Smith, Martina L
dc.contributor.author	Cole, Jason N
dc.contributor.author	Kirk, Joshua K
dc.contributor.author	Henningham, Anna
dc.contributor.author	McArthur, Jason D
dc.contributor.author	Dinkla, Katrin
dc.contributor.author	Aziz, Ramy K
dc.contributor.author	Kansal, Rita G
dc.contributor.author	Simpson, Amelia J
dc.contributor.author	Buchanan, John T
dc.contributor.author	Chhatwal, Gursharan S
dc.contributor.author	Kotb, Malak
dc.contributor.author	Nizet, Victor
dc.date.accessioned	2008-03-05T13:49:43Z
dc.date.available	2008-03-05T13:49:43Z
dc.date.issued	2007-08
dc.identifier.citation	DNase Sda1 provides selection pressure for a switch to invasive group A streptococcal infection. 2007, 13 (8):981-5 Nat. Med.	en
dc.identifier.issn	1078-8956
dc.identifier.pmid	17632528
dc.identifier.doi	10.1038/nm1612
dc.identifier.uri	http://hdl.handle.net/10033/19833
dc.description.abstract	Most invasive bacterial infections are caused by species that more commonly colonize the human host with minimal symptoms. Although phenotypic or genetic correlates underlying a bacterium's shift to enhanced virulence have been studied, the in vivo selection pressures governing such shifts are poorly understood. The globally disseminated M1T1 clone of group A Streptococcus (GAS) is linked with the rare but life-threatening syndromes of necrotizing fasciitis and toxic shock syndrome. Mutations in the GAS control of virulence regulatory sensor kinase (covRS) operon are associated with severe invasive disease, abolishing expression of a broad-spectrum cysteine protease (SpeB) and allowing the recruitment and activation of host plasminogen on the bacterial surface. Here we describe how bacteriophage-encoded GAS DNase (Sda1), which facilitates the pathogen's escape from neutrophil extracellular traps, serves as a selective force for covRS mutation. The results provide a paradigm whereby natural selection exerted by the innate immune system generates hypervirulent bacterial variants with increased risk of systemic dissemination.
dc.language.iso	en	en
dc.subject.mesh	Animals	en
dc.subject.mesh	Cell Survival	en
dc.subject.mesh	Deoxyribonuclease I	en
dc.subject.mesh	Humans	en
dc.subject.mesh	Immunity, Natural	en
dc.subject.mesh	Mice	en
dc.subject.mesh	Neutrophils	en
dc.subject.mesh	Phenotype	en
dc.subject.mesh	Selection (Genetics)	en
dc.subject.mesh	Streptococcal Infections	en
dc.subject.mesh	Streptococcus pyogenes	en
dc.subject.mesh	Virulence	en
dc.title	DNase Sda1 provides selection pressure for a switch to invasive group A streptococcal infection.	en
dc.type	Article	en
dc.contributor.department	School of Biological Sciences, University of Wollongong, Wollongong, New South Wales 2522, Australia.	en
dc.identifier.journal	Nature medicine	en
refterms.dateFOA	2018-06-13T16:59:32Z
html.description.abstract	Most invasive bacterial infections are caused by species that more commonly colonize the human host with minimal symptoms. Although phenotypic or genetic correlates underlying a bacterium's shift to enhanced virulence have been studied, the in vivo selection pressures governing such shifts are poorly understood. The globally disseminated M1T1 clone of group A Streptococcus (GAS) is linked with the rare but life-threatening syndromes of necrotizing fasciitis and toxic shock syndrome. Mutations in the GAS control of virulence regulatory sensor kinase (covRS) operon are associated with severe invasive disease, abolishing expression of a broad-spectrum cysteine protease (SpeB) and allowing the recruitment and activation of host plasminogen on the bacterial surface. Here we describe how bacteriophage-encoded GAS DNase (Sda1), which facilitates the pathogen's escape from neutrophil extracellular traps, serves as a selective force for covRS mutation. The results provide a paradigm whereby natural selection exerted by the innate immune system generates hypervirulent bacterial variants with increased risk of systemic dissemination.