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Activated Antigen-Specific CD8+ T Cells Persist in the Lungs Following Recovery from Respiratory Virus Infections

机译:从呼吸道病毒感染中恢复后,活化的抗原特异性CD8 + T细胞仍存在于肺中

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The poor correlation between cellular immunity to respiratory virus infections and the numbers of memory CD8+ T cells in the secondary lymphoid organs suggests that there may be additional reservoirs of T cell memory to this class of infection. Here we identify a substantial population of Ag-specific T cells in the lung that persist for several months after recovery from an influenza or Sendai virus infection. These cells are present in high numbers in both the airways and lung parenchyma and can be distinguished from memory cell populations in the spleen and peripheral lymph nodes in terms of the relative frequencies among CD8+ T cells, activation status, and kinetics of persistence. In addition, these cells are functional in terms of their ability to proliferate, express cytolytic activity, and secrete cytokines, although they do not express constitutive cytolytic activity. Adoptive transfer experiments demonstrated that the long-term establishment of activated T cells in the lung did not require infection in the lung by a pathogen carrying the inducing Ag. The kinetics of persistence of Ag-specific CD8+ T cells in the lung suggests that they play a key role in protective cellular immunity to respiratory virus infections.
机译:细胞对呼吸道病毒感染的免疫力与继发性淋巴器官中的记忆CD8 + T细胞数量之间的相关性较弱,这表明此类感染可能还有更多的T细胞记忆储集层。在这里,我们从肺炎或仙台病毒感染中恢复后,在肺中发现了大量的Ag特异性T细胞,并持续了几个月。这些细胞大量存在于气道和肺实质中,并且可以根据CD8 + T细胞之间的相对频率,激活状态和持久性动力学与脾脏和外周淋巴结中的记忆细胞群区分开。另外,尽管它们不表达组成型溶细胞活性,但就其增殖,表达溶细胞活性和分泌细胞因子的功能而言,它们是有功能的。过继转移实验表明,在肺中长期建立活化的T细胞并不需要在肺中被携带诱导性Ag的病原体感染。肺中Ag特异性CD8 + T细胞的持久动力学表明,它们在保护细胞抵抗呼吸道病毒感染中发挥了关键作用。

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