Cytocidal Effect of<i>Streptococcus pyogenes</i>on Mouse Neutrophils In Vivo and the Critical Role of Streptolysin S

Miyoshi‐Akiyama, Tohru; Takamatsu, Daisuke; Koyanagi, Madoka; Zhao, Junlong; Imanishi, Ken’ichi; Uchiyama, Takehiko

doi:10.1086/430617

Cited by 78 publications

(84 citation statements)

References 33 publications

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“…17,59 In addition, high levels of expression of sagA (ranked 28th), which encodes the potent cytolysin SLS, was notable because SLS is thought to accelerate necrotic fascial injury through cytotoxic or apoptotic effects on many cell types including, but not limited to, neutrophils. 60 The untranslated mRNA of the pleiotropic effect locus (pel), which incidentally contains sagA, also acts as an antisense RNA transcriptional regulator, augmenting GAS virulence factor expression [SIC, M-protein, extracellular NAD-glycohydrolase (NADase encoded by nga/spn), plasminogen activator streptokinase encoded by ska, and SpeB] when pel RNA expression is induced. 61,62 We detected abundant sagA transcripts; thus pel-induced virulence gene expression may be predicted, as was observed in this study for all but nga (ranked 780th in WT extracts).…”

Section: Abundant Gas Transcripts In Soft Tissue Infectionmentioning

confidence: 99%

Analysis of the Transcriptome of Group A Streptococcus in Mouse Soft Tissue Infection

Graham

Virtaneva

Porcella

et al. 2006

The American Journal of Pathology

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Molecular mechanisms mediating group A Streptococcus (GAS)-host interactions remain poorly understood but are crucial for diagnostic, therapeutic, and vaccine development. An optimized high-density microarray was used to analyze the transcriptome of GAS during experimental mouse soft tissue infection. The transcriptome of a wild-type serotype M1 GAS strain and an isogenic transcriptional regulator knockout mutant (covR) also were compared. Array datasets were verified by quantitative real-time reverse transcriptase-polymerase chain reaction and in situ immunohistochemistry. The results unambiguously demonstrate that coordinated expression of proven and putative GAS virulence factors is directed toward overwhelming innate host defenses leading to severe cellular damage. We also identified adaptive metabolic responses triggered by nutrient signals and hypoxic/acidic conditions in the host, likely facilitating pathogen persistence and proliferation in soft tissues. Key discoveries included that oxidative stress genes, virulence genes, genes related to amino acid and maltodextrin utilization, and several two-component transcriptional regulators were highly expressed in vivo. This study is the first global analysis of the GAS transcriptome during invasive infection. Coupled with parallel analysis of the covR mutant strain, novel insights have been made into the regulation of GAS virulence in vivo, resulting in new avenues for targeted therapeutic and vaccine research.

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Section: Abundant Gas Transcripts In Soft Tissue Infectionmentioning

confidence: 99%

Analysis of the Transcriptome of Group A Streptococcus in Mouse Soft Tissue Infection

Graham

Virtaneva

Porcella

et al. 2006

The American Journal of Pathology

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“…Many bacterial pathogens actively secrete toxins and other soluble factors to aid in the destruction of host tissue, to initiate signaling changes in host cells or to manipulate immune system responses during the course of infection [1][2][3][4][5][6][7][8][9][10] . Though methods have been developed to successfully purify and produce many of these important virulence factors for study, some bacterial products have unique structures or extensive posttranslational modifications that make them recalcitrant candidates for purification methods and thus cannot be studied in isolation using in vitro systems.…”

Section: Introductionmentioning

confidence: 99%

Implementation of a Permeable Membrane Insert-based Infection System to Study the Effects of Secreted Bacterial Toxins on Mammalian Host Cells

Flaherty

Lee

2016

JoVE

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Many bacterial pathogens secrete potent toxins to aid in the destruction of host tissue, to initiate signaling changes in host cells or to manipulate immune system responses during the course of infection. Though methods have been developed to successfully purify and produce many of these important virulence factors, there are still many bacterial toxins whose unique structure or extensive post-translational modifications make them difficult to purify and study in in vitro systems. Furthermore, even when pure toxin can be obtained, there are many challenges associated with studying the specific effects of a toxin under relevant physiological conditions. Most in vitro cell culture models designed to assess the effects of secreted bacterial toxins on host cells involve incubating host cells with a one-time dose of toxin. Such methods poorly approximate what host cells actually experience during an infection, where toxin is continually produced by bacterial cells and allowed to accumulate gradually during the course of infection. This protocol describes the design of a permeable membrane insert-based bacterial infection system to study the effects of Streptolysin S, a potent toxin produced by Group A Streptococcus, on human epithelial keratinocytes. This system more closely mimics the natural physiological environment during an infection than methods where pure toxin or bacterial supernatants are directly applied to host cells. Importantly, this method also eliminates the bias of host responses that are due to direct contact between the bacteria and host cells. This system has been utilized to effectively assess the effects of Streptolysin S (SLS) on host membrane integrity, cellular viability, and cellular signaling responses. This technique can be readily applied to the study of other secreted virulence factors on a variety of mammalian host cell types to investigate the specific role of a secreted bacterial factor during the course of infection.

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“…By contrast, several genes associated with pro-and anti-apoptotic response were differentially expressed in the selected susceptible and resistant strains post-infection (Figure 3-5). Apoptosis in streptococcal pathogenesis is affected by interacting factors including, context of infection (Marriott and Dockrell, 2006), cells undergoing apoptosis (Kobayashi et al, 2003;Nakagawa et al, 2004;Miyoshi-Akiyama et al, 2005), for example, apoptosis aids in the clearing of infection if macrophages are undergoing apoptosis, while it would be harmful to the host if lymphocytes are undergoing apoptosis. Other factors include, whether the bacteria is internalized or extracellular (Cywes Bentley et al, 2005) and accordingly the type of apoptosis pathways activated (Klenk et al, 2005).…”

Section: Discussionmentioning

confidence: 99%

Systems Biology Approach to Identifying Host Interactive Pathways Modulating the Severity of Streptococcal Sepsis

Abdeltawab¹

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Cytocidal Effect ofStreptococcus pyogeneson Mouse Neutrophils In Vivo and the Critical Role of Streptolysin S

Cited by 78 publications

References 33 publications

Analysis of the Transcriptome of Group A Streptococcus in Mouse Soft Tissue Infection

Analysis of the Transcriptome of Group A Streptococcus in Mouse Soft Tissue Infection

Implementation of a Permeable Membrane Insert-based Infection System to Study the Effects of Secreted Bacterial Toxins on Mammalian Host Cells

Systems Biology Approach to Identifying Host Interactive Pathways Modulating the Severity of Streptococcal Sepsis

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