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首页> 外文期刊>Infection and immunity >Internalization and Trafficking of Nontypeable Haemophilus influenzae in Human Respiratory Epithelial Cells and Roles of IgA1 Proteases for Optimal Invasion and Persistence
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Internalization and Trafficking of Nontypeable Haemophilus influenzae in Human Respiratory Epithelial Cells and Roles of IgA1 Proteases for Optimal Invasion and Persistence

机译:人类呼吸道上皮细胞中不可分型流感嗜血杆菌的内化和贩运以及IgA1蛋白酶对最佳侵袭和持久性的作用

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Nontypeable Haemophilus influenzae (NTHI) is a leading cause of opportunistic infections of the respiratory tract in children and adults. Although considered an extracellular pathogen, NTHI has been observed repeatedly within and between cells of the human respiratory tract, and these observations have been correlated to symptomatic infection. These findings are intriguing in light of the knowledge that NTHI persists in the respiratory tract despite antibiotic therapy and the development of bactericidal antibodies. We hypothesized that intracellular NTHI avoids, escapes, or neutralizes the endolysosomal pathway and persists within human respiratory epithelial cells and that human IgA1 proteases are required for optimal internalization and persistence of NTHI. Virtually all strains encode a human IgA1 protease gene, igaA, and we previously characterized a novel human IgA1 protease gene, igaB, that is associated with disease-causing strains and is homologous to the IgA1 protease that is unique to pathogenic Neisseria spp. Here, we show that NTHI invades human bronchial epithelial cells in vitro in a lipid raft-independent manner, is subsequently trafficked via the endolysosomal pathway, and is killed in lysosomes after variable durations of persistence. IgaA is required for optimal invasion. IgaB appears to play little or no role in adherence or invasion but is required for optimal intracellular persistence of NTHI. IgaB cleaves lysosome-associated membrane protein 1 (LAMP1) at pHs characteristic of the plasma membrane, early endosome, late endosome, and lysosome. However, neither IgA1 protease inhibits acidification of intracellular vesicles containing NTHI. NTHI IgA1 proteases play important but different roles in NTHI invasion and trafficking in respiratory epithelial cells.
机译:不可归类的流感嗜血杆菌(NTHI)是儿童和成人呼吸道机会性感染的主要原因。尽管NTHI被认为是细胞外病原体,但已在人类呼吸道的细胞内和细胞之间反复观察到NTHI,并将这些观察结果与症状性感染相关。考虑到尽管抗生素疗法和杀菌抗体的发展,NTHI在呼吸道中仍然存在,但这些发现还是令人感兴趣的。我们假设细胞内NTHI避免,逃避或中和了溶酶体途径,并在人呼吸道上皮细胞内持续存在,而人IgA1蛋白酶是NTHI最佳内在化和持久性所必需的。几乎所有菌株都编码人IgA1蛋白酶基因igaA,并且我们以前鉴定了一种新型的人IgA1蛋白酶基因igaB,该基因与致病菌株相关,并且与致病性奈瑟氏菌属独特的IgA1蛋白酶同源。在这里,我们显示NTHI在体外以脂质筏非依赖性方式侵入人支气管上皮细胞,随后通过内溶酶体途径贩运,并在持续时间可变的持续时间后在溶酶体中被杀死。 IgaA是最佳入侵所必需的。 IgaB似乎在粘附或侵袭中几乎没有作用,但对于NTHI的最佳细胞内持久性是必需的。 IgaB在质膜,早期内体,晚期内体和溶酶体的pH值下裂解溶酶体相关膜蛋白1(LAMP1)。但是,两种IgA1蛋白酶均不能抑制含有NTHI的细胞内囊泡的酸化。 NTHI IgA1蛋白酶在呼吸道上皮细胞的NTHI侵袭和运输中发挥重要但不同的作用。

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