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首页> 外文期刊>Diseases of Aquatic Organisms >Sortase inhibitor phenyl vinyl sulfone inhibits Renibacterium salmoninarum adherence and invasion of host cells
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Sortase inhibitor phenyl vinyl sulfone inhibits Renibacterium salmoninarum adherence and invasion of host cells

机译:分选酶抑制剂苯基乙烯基砜抑制沙门氏菌的粘附和侵袭宿主细胞

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ABSTRACT: Renibacterium salmoninarum, the causative agent of bacterial kidney disease in salmonid fishes, is a Gram-positive diplococcobacillus belonging to the family Micrococcaceae. Analysis of the genome sequence of the bacterium demonstrated the presence of a sortase homolog (srtD), a gene specifying an enzyme found in Gram-positive bacteria and required for covalent anchoring of cell surface proteins. Interference of sortase activity is being examined as a target for therapeutic prevention of infection by several pathogenic Gram-positive bacterial species. In silico analysis identified 8 open reading frames containing sortase recognition motifs, suggesting these proteins are translocated to the bacterial cell wall. The sortase and potential sortase substrate genes are transcribed in R. salmoninarum, suggesting they encode functional proteins. Treatment of R. salmoninarum with phenyl vinyl sulfone (PVS) significantly reduced bacterial adherence to Chinook salmon fibronectin. In addition, the ability of the PVS-treated bacteria to adhere to Chinook salmon embryo cells (CHSE-214) in vitro was dramatically reduced compared to that of untreated bacteria. More importantly, PVS-treated bacteria were unable to invade and replicate within CHSE-214 cells (demonstrated by an intracellular growth assay and by light microscopy). When treated with PVS, R. salmoninarum was not cytopathic to CHSE-214 cells, whereas untreated bacteria produced cytopathology within a few days. These findings clearly show that PVS, a small molecule drug and a known sortase inhibitor, can interfere with the ability of R. salmoninarum to adhere and colonize fish cells, with a corresponding decrease in virulence.
机译:摘要:鲑鱼肾单胞菌是鲑鱼鱼类细菌性肾脏疾病的病原体,是革兰氏阳性双球菌,属于微球菌科。对该细菌基因组序列的分析表明存在分选酶同系物 srtD ),该基因指定了革兰氏阳性细菌中发现的一种酶,并需要共价锚定细胞表面蛋白分选酶活性的干扰正在作为治疗性预防几种致病性革兰氏阳性细菌感染的目标。 计算机分析分析确定了8个包含分选酶识别基序的开放阅读框,表明这些蛋白易位至细菌细胞壁。分选酶和潜在的分选酶底物基因在中转录。鲑鱼,表明它们编码功能蛋白。 R的治疗。含苯基乙烯基砜(PVS)的沙门氏菌可显着降低细菌对奇努克鲑鱼纤连蛋白的粘附。此外,与未经处理的细菌相比,经PVS处理的细菌在体外粘附于奇努克鲑鱼胚胎细胞(CHSE-214)的能力大大降低。更重要的是,经PVS处理的细菌无法侵入CHSE-214细胞并在其中复制(通过细胞内生长试验和光学显微镜证实)。用PVS处理时, R。沙门氏菌对CHSE-214细胞没有细胞病变,而未经处理的细菌在几天内就产生了细胞病变。这些发现清楚地表明,PVS,一种小分子药物和一种已知的分选酶抑制剂,可能会干扰R的能力。沙门氏菌可以粘附并定居在鱼细胞上,并相应地降低了毒力。

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