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The role of the twin-arginine translocation pathway in Escherichia coli K1 pathogenicity in the African migratory locust, Locusta migratoria

机译:双精氨酸易位途径在非洲游蝗蝗大肠埃希氏菌K1致病性中的作用

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摘要

Escherichia coli K1 infection is a major cause of neonatal meningitis, with high rates of mortality and disability. Despite years of research, only a small number of factors contributing to E. coli K1 virulence have been identified. The Tat (twin-arginine translocation) protein export system is found in the cytoplasmic membrane of E. coli and is involved in the transport of folded proteins. In vivo and ex vivo models using the African migratory locust, Locusta migratoria, were employed to explore the role of Tat pathway in E. coli K1 virulence using tat-deletion mutants. Groups of locusts were infected and mortality was recorded at 24-h intervals. The findings revealed that ΔtatA, ΔtatAC and Δtat produced levels of mortality similar to wild-type E. coli K1, with >78% mortality recorded within 72 h. Bacteraemia was determined from haemolymph obtained 3 and 24 h postinfection. Again, wild-type and ΔtatA produced similar levels of bacteraemia. In contrast, ΔtatAC and Δtat produced lower levels of bacteraemia. Following injection of bacteria into isolated head capsules ex vivo, all mutants invaded the CNS. Overall, these studies showed no evidence of involvement of the Tat pathway in locust mortality but suggest its possible role in bacteraemia.
机译:大肠杆菌K1感染是新生儿脑膜炎的主要原因,死亡率和致残率很高。尽管进行了多年的研究,但仅识别出少数导致大肠杆菌K1毒力的因素。 Tat(双精氨酸易位)蛋白输出系统存在于大肠杆菌的细胞质膜中,并参与折叠蛋白的运输。使用非洲迁移蝗Locusta migratoria的体内和离体模型,利用tat缺失突变体探讨Tat途径在大肠杆菌K1毒力中的作用。蝗虫被感染,每隔24小时记录一次死亡率。研究结果表明,ΔtatA,ΔtatAC和Δtat产生的死亡率与野生型大肠杆菌K1相似,在72小时内记录的死亡率> 78%。从感染后3和24小时获得的血淋巴确定细菌血症。同样,野生型和ΔtatA产生相似水平的菌血症。相反,ΔtatAC和Δtat产生较低的菌血症水平。在将细菌离体注射到离体的头部胶囊中后,所有突变体都侵入了CNS。总体而言,这些研究没有显示Tat途径参与蝗虫死亡率的证据,但表明其可能在菌血症中发挥作用。

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