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CD4-T淋巴细胞与肺炎球菌溶血素及肺炎球菌的相互作用表明,其在宿主对肺炎球菌感染的反应中起着关键的保护作用。

CD4-T-lymphocyte interactions with pneumolysin and pneumococci suggest a crucial protective role in the host response to pneumococcal infection.

作者信息

Kadioglu Aras, Coward William, Colston M Joseph, Hewitt Colin R A, Andrew Peter W

机构信息

Department of Infection, Immunity & Inflammation, University of Leicester, Leicester LE1 9HN, United Kingdom.

出版信息

Infect Immun. 2004 May;72(5):2689-97. doi: 10.1128/IAI.72.5.2689-2697.2004.

Abstract

Previously, we had shown that T cells accumulated in peribronchiolar and perivascular areas of lungs soon after intranasal infection with Streptococcus pneumoniae. We have now presented new evidence, using major histocompatibility class II-deficient mice, that CD4 cells are important for early protective immunity. In addition, we have also shown that a population of human CD4 cells migrates towards pneumococci and that in vivo-passaged pneumococci are substantially more potent at inducing migration than in vitro-grown bacteria. This migratory process is unique to a specific population of CD4 cells, is highly reproducible, and is independent of prior CD4 cell activation, and yet the migratory process results in a significant proportion of CD4 cells becoming activated. The production of pneumolysin is a key facet in the induction of migration of CD4 cells by in vivo bacteria, as pneumolysin-deficient bacteria do not induce migration, but the data also show that pneumolysin alone is not sufficient to explain the enhanced migration. Increased CD25 expression occurs during migration, and a higher percentage of cells in the migrated population express gamma interferon or interleukin 4 (IL-4) than in the population that did not migrate. There is evidence that the activation of IL-4 expression occurs during migration.

摘要

此前,我们已经表明,鼻内感染肺炎链球菌后不久,T细胞会在肺的细支气管周围和血管周围区域积聚。现在,我们利用主要组织相容性复合体II类缺陷小鼠提供了新的证据,表明CD4细胞对早期保护性免疫很重要。此外,我们还表明,一群人类CD4细胞会向肺炎球菌迁移,并且体内传代的肺炎球菌在诱导迁移方面比体外培养的细菌效力要高得多。这种迁移过程是特定CD4细胞群体所特有的,具有高度可重复性,并且独立于先前的CD4细胞激活,然而迁移过程会导致相当一部分CD4细胞被激活。肺炎溶血素的产生是体内细菌诱导CD4细胞迁移的一个关键方面,因为缺乏肺炎溶血素的细菌不会诱导迁移,但数据也表明仅肺炎溶血素不足以解释增强的迁移。迁移过程中CD25表达增加,迁移群体中表达γ干扰素或白细胞介素4(IL-4)的细胞百分比高于未迁移群体。有证据表明IL-4表达的激活发生在迁移过程中。

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