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M1T1 Variants Induce an Inflammatory Neutrophil Phenotype Including Activation of Inflammatory Caspases

Front Cell Infect Microbiol. 2021-01; 
Jonathan G Williams, Diane Ly, Nicholas J Geraghty, Jason D McArthur, Heema K N Vyas, Jody Gorman, James A Tsatsaronis, Ronald Sluyter, Martina L Sanderson-Smith
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Gene Synthesis … In brief, stable GFP expression by GAS was created by synthesizing the ribosomal binding site (RBS) and gfp gene from pDCerm-GFP (Ly et al., 2014) into the pUC57 plasmid (GenScript, Piscataway, NJ, USA), resulting in a pUC57-RBSGFP plasmid?… Get A Quote

摘要

Invasive infections due to group A (GAS) advance rapidly causing tissue degradation and unregulated inflammation. Neutrophils are the primary immune cells that respond to GAS. The neutrophil response to GAS was characterised in response to two M1T1 isolates; 5448 and animal passaged variant 5448AP. Co-incubation of neutrophils with 5448AP resulted in proliferation of GAS and lowered the production of reactive oxygen species when compared with 5448. Infection with both strains invoked neutrophil death, however apoptosis was reduced in response to 5448AP. Both strains induced neutrophil caspase-1 and caspase-4 expression , with inflammatory caspase activation detected and . GAS infections involving strains such... More

關鍵詞

CD16, CD31, Group A streptococcus, IL-1β, covS, inflammation, neutrophil, polymorphonuclear leukocyte
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