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Isolation of Mycobacterium tuberculosis mutants defective in the arrest of phagosome maturation

机译:分离吞噬体成熟中有缺陷的结核分枝杆菌突变体

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Mycobacterium tuberculosis resides within the phagocytes of its host. It ensures its continued survival through arresting the normal maturation of its phagosome, which is retained within the early endosomal system of the macrophage. Although individual bacterial components have been shown to modulate phagosome biogenesis, the mechanism(s) active in live, intact bacteria remain elusive. We have developed a genetic screen that facilitates the isolation of mutants defective in arresting the maturation of their phagosomes. Macrophages were incubated with iron-dextran that was chased into lysosomes. The cells were subsequently infected with M. tuberculosis from a library of transposon-mutagenized bacteria. After four rounds of enrichment, the majority of mutants isolated were unable to prevent acidification of their phagosomes and were attenuated for intracellular survival. The genes affected range in function from those with no known homologues to putative transporters and lipid synthesis enzymes. Further characterization of these bacteria is needed. In addition to clarifying the processes active in modulation of phagosome biogenesis by M. tuberculosis, this screen may be applicable to other pathogens that restrict the maturation of their phagosome.
机译:结核分枝杆菌位于其宿主的吞噬细胞内。它通过阻止吞噬体的正常成熟来确保其继续生存,吞噬体保留在巨噬细胞的早期内体系统中。尽管已显示单个细菌成分可调节吞噬体的生物发生,但活的完整细菌中活跃的机制仍然难以捉摸。我们已经开发了一种遗传筛选技术,可帮助分离在阻止其吞噬体成熟方面存在缺陷的突变体。将巨噬细胞与葡聚糖铁一起孵育,将其加入溶酶体中。随后用转座子诱变细菌文库将细胞感染结核分枝杆菌。经过四轮富集后,分离出的大多数突变体无法阻止其吞噬体的酸化,并因细胞内存活而减弱。受影响的基因的功能范围从没有已知同源物的基因到推定的转运蛋白和脂质合成酶。需要进一步表征这些细菌。除了阐明结核分枝杆菌对吞噬体生物发生的调控具有积极作用的过程外,该筛选可能适用于其他限制其吞噬体成熟的病原体。

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