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Phenomic and genomic approaches to studying the inhibition of multiresistant Salmonella enterica by microcin J25

机译:通过微核J25研究多人沙门氏菌肠苷的表情和基因组方法

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In livestock production, antibiotics are used to promote animal growth, control infections and thereby increase profitability. This practice has led to the emergence of multiresistant bacteria such as Salmonella, of which some serovars are disseminated in the environment. The objective of this study is to evaluate microcin J25 as an inhibitor of Salmonella enterica serovars of various origins including human, livestock and food. Among the 116 isolates tested, 37 (31.8%) were found resistant to at least one antibiotic, and 28 were multiresistant with 19 expressing the penta-resistant phenotype ACSSuT. Microcin J25 inhibited all isolates, with minimal inhibitory concentration values ranging from 0.06 mu g/ml (28.4 nM) to 400 mu g/ml (189 mu M). Interestingly, no cross-resistance was found between microcin J25 and antibiotics. Multiple sequence alignments of genes encoding for the different proteins involved in the recognition and transport of microcin J25 showed that only ferric-hydroxamate uptake is an essential determinant for susceptibility of S. enterica to microcin J25. Examination of Salmonella strains exposed to microcin J25 by transmission electronic microscopy showed for the first-time involvement of a pore formation mechanism. Microcin J25 was a strong inhibitor of several multiresistant isolates of Salmonella and may have a great potential as an alternative to antibiotics.
机译:在牲畜生产中,抗生素用于促进动物生长,对照感染,从而提高盈利能力。这种做法导致了多思科细菌的出现,如沙门氏菌,其中一些塞洛瓦斯在环境中传播。本研究的目的是评估微素J25作为肠道肠道肠道的抑制剂,包括人类,牲畜和食物等各种起源。在测试的116个分离物中,发现37个(31.8%)耐药于至少一种抗生素,28个是多过滤剂,其中19个表达抗抗抗体型Acssut。微素J25抑制所有分离物,最小抑制浓度值范围为0.06μg/ ml(28.4nm)至400μmg/ ml(189μm)。有趣的是,微外科J25和抗生素之间没有发现交叉抗性。涉及识别和传输中涉及的不同蛋白质的基因的多序列对准表明,只有铁 - 羟肟酸酯摄取是S.肠溶性至微癌J25的必要决定因素。通过透射电子显微镜检查暴露于微素J25的沙门氏菌菌株显示孔隙形成机制的第一次参与。微素J25是多人沙门氏菌的多态分离物的强烈抑制剂,并且可能具有抗生素替代品的潜力。

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