首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Antibiotic-based selection for bacterial genes that are specifically induced during infection of a host.
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Antibiotic-based selection for bacterial genes that are specifically induced during infection of a host.

机译:在宿主感染过程中特异性诱导的细菌基因的基于抗生素的选择。

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We have recently described a genetic system, termed in vivo expression technology (IVET), that uses an animal as a selective medium to identify genes that pathogenic bacteria specifically express when infecting host tissues. Here, the potential utility of the IVET approach has been expanded with the development of a transcriptional-fusion vector, pIVET8, which uses antibiotics resistance as the basis for selection in host tissues. pIVET8 contains promoterless chloramphenicol acetyltransferase (cat) and lacZY genes. A pool of Salmonella typhimurium clones carrying random cat-lac transcriptional fusions, produced with pIVET8, was used to infect BALB/c mice that were subsequently treated with intraperitoneal injections of chloramphenicol. Strains that survived the selection by expressing the cat gene in the animal were then screened for those that had low-level lacZY expression on laboratory medium. These strains carry operon fusions to genes that are specifically induced in vivo (ivi genes). One of the ivi genes identified (fadB) encodes an enzyme involved in fatty acid oxidation, suggesting that this enzyme might contribute to the metabolism of bactericidal or proinflammatory host fatty acids. The pIVET8-based selection system was also used to identify S. typhimurium genes that are induced in cultured macrophages. The nature of ivi gene products will provide a more complete understanding of the metabolic, physiological, and genetic factors that contribute to the virulence of microbial pathogens.
机译:我们最近描述了一种称为体内表达技术(IVET)的遗传系统,该系统使用动物作为选择性培养基来鉴定病原细菌感染宿主组织时特异性表达的基因。在这里,随着转录融合载体pIVET8的开发,扩大了IVET方法的潜在用途,该载体使用抗生素抗性作为在宿主组织中选择的基础。 pIVET8包含无启动子的氯霉素乙酰转移酶(cat)和lacZY基因。携带由pIVET8产生的携带随机cat-lac转录融合体的鼠伤寒沙门氏菌克隆库感染BALB / c小鼠,随后用腹膜内注射氯霉素对其进行治疗。然后筛选通过在动物中表达cat基因而在选择中幸存的菌株,寻找在实验室培养基中具有低水平lacZY表达的菌株。这些菌株将操纵子融合到体内特异性诱导的基因(ivi基因)上。鉴定出的ivi基因之一(fadB)编码一种参与脂肪酸氧化的酶,表明该酶可能有助于杀菌或促炎性宿主脂肪酸的代谢。基于pIVET8的选择系统还用于鉴定在培养的巨噬细胞中诱导的鼠伤寒沙门氏菌基因。 ivi基因产物的性质将提供对导致微生物病原体毒性的代谢,生理和遗传因素的更完整的理解。

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