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首页> 外文期刊>Medical Microbiology and Immunology >Synergistic effects of streptolysin S and streptococcal pyrogenic exotoxin B on the mouse model of group A streptococcal infection
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Synergistic effects of streptolysin S and streptococcal pyrogenic exotoxin B on the mouse model of group A streptococcal infection

机译:链球菌溶血素S和链球菌热原性外毒素B对A组链球菌感染小鼠模型的协同作用

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摘要

Streptococcus pyogenes is a group A streptococcus (GAS) and an important human pathogen that causes a variety of diseases. Streptococcal pyrogenic exotoxin B (SPE B) and streptolysin S (SLS) are important virulence factors involved in GAS infection, but it is not clear which one is more virulent. Using an air pouch infection model, the wild-type strain NZ131, its isogenic mutants, and complementary mutants were used to examine the effects of SPE B and SLS on GAS infection. The results of the skin lesion and mouse mortality assays showed that although SPE B and SLS had a synergistic effect on GAS infection, SPE B played a more important role in local tissue damage while SLS had a more prominent effect on mouse mortality. Surveys of the exudates from the air pouch revealed that the expression of inflammatory cytokines was significantly inhibited in the sagB/ speB-double-mutant JM4-infected mice. Furthermore, in vivo and in vitro studies showed that the isogenic mutant strains were more susceptible to the immune cell killing than the wild-type strain and that the sagB/speB-doublemutant JM4 was the most sensitive among these strains. Moreover, infection with the sagB/speB-double-mutant JM4 strain caused the least amount of macrophage apoptosis compared to infection with the wild-type NZ131 and the other complementary strains, which express only SPE B or SLS or both. Taken together, these results indicate that both SPE B and SLS contributed to GAS evasion from immune cell killing, local tissue damage, and mouse mortality.
机译:化脓性链球菌是A组链球菌(GAS),是引起多种疾病的重要人类病原体。链球菌热原性外毒素B(SPE B)和链球菌溶血素S(SLS)是参与GAS感染的重要毒力因子,但尚不清楚哪种毒力更高。使用气袋感染模型,使用野生型菌株NZ131,其同基因突变体和互补突变体检查SPE B和SLS对GAS感染的影响。皮肤病变和小鼠死亡率测定的结果表明,尽管SPE B和SLS对GAS感染具有协同作用,但SPE B在局部组织损伤中起更重要的作用,而SLS对小鼠死亡率具有更显着的作用。对气囊渗出液的调查显示,在sagB / speB-双突变JM4感染的小鼠中,炎性细胞因子的表达被显着抑制。此外,体内和体外研究表明,同基因突变株比野生型株对免疫细胞的杀伤更敏感,并且在这些株中,sagB / speB-双突变JM4最敏感。此外,与仅表达SPE B或SLS或两者的野生型NZ131和其他互补菌株感染相比,sagB / speB双突变JM4菌株感染引起的巨噬细胞凋亡最少。两者合计,这些结果表明SPE B和SLS都有助于逃避免疫细胞杀伤,局部组织损伤和小鼠死亡率的GAS逃逸。

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