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Legionella pneumophilaRequires Polyamines for Optimal Intracellular Growth ▿

机译:嗜肺军团菌需要多胺才能获得最佳的细胞内生长 ▿

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摘要

The Gram-negative intracellular pathogen Legionella pneumophilareplicates in a membrane-bound compartment known as the Legionella-containing vacuole (LCV), into which it abundantly releases its chaperonin, HtpB. To determine whether HtpB remains within the LCV or reaches the host cell cytoplasm, we infected U937 human macrophages and CHO cells with L. pneumophilaexpressing a translocation reporter consisting of the Bordetella pertussisadenylate cyclase fused to HtpB. These infections led to increased cyclic AMP levels, suggesting that HtpB reaches the host cell cytoplasm. To identify potential functions of cytoplasmic HtpB, we expressed it in the yeast Saccharomyces cerevisiae, where HtpB induced pseudohyphal growth. A yeast-two-hybrid screen showed that HtpB interacted with S-adenosylmethionine decarboxylase (SAMDC), an essential yeast enzyme (encoded by SPE2) that is required for polyamine biosynthesis. Increasing the copy number of SPE2induced pseudohyphal growth in S. cerevisiae; thus, we speculated that (i) HtpB induces pseudohyphal growth by activating polyamine synthesis and (ii) L. pneumophilamay require exogenous polyamines for growth. A pharmacological inhibitor of SAMDC significantly reduced L. pneumophilareplication in L929 mouse cells and U937 macrophages, whereas exogenously added polyamines moderately favored intracellular growth, confirming that polyamines and host SAMDC activity promote L. pneumophilaproliferation. Bioinformatic analysis revealed that most known enzymes required for polyamine biosynthesis in bacteria (including SAMDC) are absent in L. pneumophila, further suggesting a need for exogenous polyamines. We hypothesize that HtpB may function to ensure a supply of polyamines in host cells, which are required for the optimal intracellular growth of L. pneumophila.
机译:革兰氏阴性细胞内病原体嗜肺军团菌在膜结合的隔室中复制,该隔室被称为含军团菌的液泡(LCV),在膜隔室中大量释放其伴侣蛋白HtpB。为了确定HtpB是否保留在LCV内或到达宿主细胞质,我们用嗜肺乳杆菌感染U937人巨噬细胞和CHO细胞,表达了由融合到HtpB的百日咳博德特氏腺苷酸环化酶组成的易位报道基因。这些感染导致循环AMP含量增加,表明HtpB到达了宿主细胞的细胞质。为了确定细胞质HtpB的潜在功能,我们在酵母Saccharomyces cerevisiae中表达了它,HtpB诱导了假菌丝的生长。酵母双杂交筛选显示HtpB与S-腺苷甲硫氨酸脱羧酶(SAMDC)相互作用,S-腺苷甲硫氨酸脱羧酶是多胺生物合成所需的必需酵母酶(由SPE2编码)。增加SPE2诱导的酿酒酵母假菌丝生长的拷贝数;因此,我们推测(i)HtpB通过激活多胺合成诱导假菌丝生长,并且(ii)嗜肺乳杆菌生长需要外源多胺。 SAMDC的药理抑制剂可显着降低L929小鼠细胞和U937巨噬细胞中的嗜肺乳杆菌的复制,而外源添加的多胺则适度促进细胞内的生长,证实多胺和宿主SAMDC的活性促进了嗜肺乳杆菌的增殖。生物信息学分析表明,细菌中多胺生物合成所需的大多数已知酶(包括SAMDC)在嗜肺乳杆菌中均不存在,这进一步表明需要外源多胺。我们假设HtpB可能起到确保宿主细胞中多胺供应的作用,而这正是肺炎嗜血杆菌的最佳细胞内生长所必需的。

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