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肺内蠕形哈特曼原虫:嗜肺军团菌在军团菌病小鼠模型中复制的潜在生态位。

Intrapulmonary Hartmannella vermiformis: a potential niche for Legionella pneumophila replication in a murine model of legionellosis.

作者信息

Brieland J, McClain M, LeGendre M, Engleberg C

机构信息

Unit for Laboratory Animal Medicine, University of Michigan Medical School, Ann Arbor 48109-0614, USA.

出版信息

Infect Immun. 1997 Nov;65(11):4892-6. doi: 10.1128/iai.65.11.4892-4896.1997.

Abstract

The potential role of inhaled protozoa as a niche for intrapulmonary replication of Legionella pneumophila was investigated in vivo with mutant strains of L. pneumophila which have reduced virulence for the amoeba Hartmannella vermiformis. L. pneumophila AA488 and AA502 were derived from wild-type strain AA100 after transposon mutagenesis. These mutants have reduced virulence for H. vermiformis but are fully virulent for mononuclear phagocytic cells. A/J mice, which are susceptible to replicative L. pneumophila lung infections, were inoculated intratracheally with L. pneumophila AA100, AA488, or AA502 (10[6] bacteria per mouse) or were coinoculated with one of the L. pneumophila strains (10[6] bacteria per mouse) and uninfected H. vermiformis (10[6] amoebae per mouse). The effect of coinoculation with H. vermiformis on intrapulmonary growth of each L. pneumophila strain was subsequently assessed. In agreement with our previous studies, coinoculation with H. vermiformis significantly enhanced intrapulmonary growth of the parent L. pneumophila strain (AA100). In contrast, intrapulmonary growth of L. pneumophila AA488 or AA502 was not significantly enhanced by coinoculation of mice with H. vermiformis. These studies demonstrate that L. pneumophila virulence for amoebae is required for maximal intrapulmonary growth of the bacteria in mice coinoculated with H. vermiformis and support the hypothesis that inhaled amoebae may potentiate intrapulmonary growth of L. pneumophila by providing a niche for bacterial replication.

摘要

利用对阿米巴虫嗜肺军团菌毒力降低的嗜肺军团菌突变株,在体内研究了吸入原生动物作为嗜肺军团菌肺内复制生态位的潜在作用。嗜肺军团菌AA488和AA502是转座子诱变后从野生型菌株AA100衍生而来的。这些突变体对蠕虫哈特曼氏变形虫的毒力降低,但对单核吞噬细胞具有完全毒力。对复制性嗜肺军团菌肺部感染易感的A/J小鼠经气管内接种嗜肺军团菌AA100、AA488或AA502(每只小鼠10[6]个细菌),或与其中一种嗜肺军团菌菌株(每只小鼠10[6]个细菌)和未感染的蠕虫哈特曼氏变形虫(每只小鼠10[6]个变形虫)共同接种。随后评估了与蠕虫哈特曼氏变形虫共同接种对每种嗜肺军团菌菌株肺内生长的影响。与我们之前的研究一致,与蠕虫哈特曼氏变形虫共同接种显著增强了亲本嗜肺军团菌菌株(AA100)的肺内生长。相比之下,小鼠与蠕虫哈特曼氏变形虫共同接种并未显著增强嗜肺军团菌AA488或AA502的肺内生长。这些研究表明,在与蠕虫哈特曼氏变形虫共同接种的小鼠中,嗜肺军团菌对变形虫的毒力是细菌在肺内最大程度生长所必需的,并支持了吸入变形虫可能通过为细菌复制提供生态位来增强嗜肺军团菌肺内生长的假说。

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