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感染流感病毒的小鼠肺部的细胞变化:细胞毒性反应的特征

Cellular changes in lungs of mice infected with influenza virus: characterization of the cytotoxic responses.

作者信息

Wyde P R, Cate T R

出版信息

Infect Immun. 1978 Nov;22(2):423-9. doi: 10.1128/iai.22.2.423-429.1978.

Abstract

Transpleural lavage of lungs from uninfected C3H mice yielded an average of 300,000 leukocytes per mouse. This number increased eightfold within 6 days after intranasal inoculation with virulent influenza A/Hong Kong/68 (H3N2) virus. Macrophages and lymphocytes in approximately equal numbers comprised 90% or more of the leukocytes both before and during infection. B, T, and null lymphocytes comprised, respectively, 9, 21, and 18% of the leukocytes before infection and 7, 26, and 5% by day 6. In absolute numbers, macrophages and T lymphocytes provided the major increments during infection. Cytotoxic activity of mononuclear cells from lung lavages was compared in a chromium release assay using syngeneic L929 target cells with the activity of mediastinal lymph nodes, spleens, and peripheral blood of uninfected and infected C3H mice. Nonspecific cytotoxicity for target cells infected with H3hkNeq1 or B/Lee influenza virus was found with mononuclear cells from uninfected mice. This activity tended to be highest with lavage leukocytes and was associated with adherent cells, presumably macrophages. Increased virus-specific cytotoxicity was detected with lavage cells by day 6 and persisted through day 9, the period of maximal pneumonia. Similar cytotoxic activity also appeared in cells from the nodes and spleen at this same time but was not detected in peripheral blood cells. The virus-specific cytotoxicity of lavage cells was due largely to a nonadherent cell possessing Fc receptors and theta antigen but lacking C3 receptors; these properties are compatible with actively cytotoxic T lymphocytes. The cytological characteristics of the infiltrating leukocytes and the cytotoxicity data suggest that the local T cell response to influenza virus infection in the lung is a major contributor to the pneumonia observed in this mouse model.

摘要

对未感染的C3H小鼠进行经胸膜肺灌洗,每只小鼠平均获得300,000个白细胞。在经鼻接种强毒甲型流感病毒A/香港/68(H3N2)后6天内,这个数字增加了八倍。在感染前和感染期间,巨噬细胞和淋巴细胞数量大致相等,占白细胞的90%或更多。B淋巴细胞、T淋巴细胞和裸淋巴细胞在感染前分别占白细胞的9%、21%和18%,到第6天时分别占7%、26%和5%。从绝对数量来看,巨噬细胞和T淋巴细胞在感染期间增加最多。在使用同基因L929靶细胞的铬释放试验中,比较了未感染和感染的C3H小鼠肺灌洗单核细胞与纵隔淋巴结、脾脏和外周血单核细胞的细胞毒性活性。发现未感染小鼠的单核细胞对感染H3hkNeq1或B/李株流感病毒的靶细胞具有非特异性细胞毒性。这种活性在灌洗白细胞中往往最高,并且与贴壁细胞(可能是巨噬细胞)有关。到第6天时,在灌洗细胞中检测到病毒特异性细胞毒性增加,并持续到第9天,即肺炎最严重的时期。同时,在淋巴结和脾脏的细胞中也出现了类似的细胞毒性活性,但在外周血细胞中未检测到。灌洗细胞的病毒特异性细胞毒性主要归因于一种非贴壁细胞,该细胞具有Fc受体和θ抗原,但缺乏C3受体;这些特性与活性细胞毒性T淋巴细胞相符。浸润白细胞 的细胞学特征和细胞毒性数据表明,肺中对流感病毒感染的局部T细胞反应是该小鼠模型中观察到的肺炎的主要原因。

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