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大鼠II型肺细胞和肺泡巨噬细胞中干扰素的产生。

Interferon production in rat type II pneumocytes and alveolar macrophages.

作者信息

Hahon N, Castranova V

机构信息

Division of Respiratory Disease Studies, National Institute for Occupational Safety and Health, Morgantown, WV 26505-2888.

出版信息

Exp Lung Res. 1989 May;15(3):429-45. doi: 10.3109/01902148909087869.

Abstract

The time course and magnitude of interferon production induced by influenza virus were determined in type II pneumocytes and alveolar macrophages isolated from rats (Sprague-Dawley). Although the peak of interferon production was approximately 20 h in both alveolar cell types, it was more than three- to fourfold higher in type II cells than in macrophages. Dose-response relationships were noted between the virus multiplicity of induction as well as population numbers of either alveolar cell type and interferon yields. The viral-induced cytokines produced by rat type II cells and alveolar macrophages exhibit physiochemical and biological properties characteristic of interferons and, with respect to type II pneumocytes, mark their heretofore unrecognized capability to produce interferon. The best cross-species antiviral protection afforded by these rat interferons to cells of different origin, expressed as percentage of homologous species (100%), was as follows: guinea pig 50, mouse 40%, and both human and monkey 0%. The heterologous antiviral activity by interferons from either rat alveolar macrophages or type II cells on alpha interferon-sensitive guinea pig cells suggests that these cytokines may be more appreciably related to the alpha-like interferon species. The growth of influenza and Sendai viruses was precluded in both rat alveolar macrophages and type II pneumocytes. The findings herein suggest that type II cells may be a major source of alveolar interferon for activating the antiviral state and modulating alveolar cell functions requisite for lung integrity.

摘要

在从大鼠(斯普拉格 - 道利大鼠)分离出的II型肺细胞和肺泡巨噬细胞中,测定了流感病毒诱导的干扰素产生的时间进程和幅度。尽管两种肺泡细胞类型中干扰素产生的峰值均约为20小时,但II型细胞中的干扰素产量比巨噬细胞中的高三到四倍以上。在诱导病毒的复数以及任何一种肺泡细胞类型的细胞数量与干扰素产量之间发现了剂量反应关系。大鼠II型细胞和肺泡巨噬细胞产生的病毒诱导细胞因子表现出干扰素特有的物理化学和生物学特性,就II型肺细胞而言,这标志着它们此前未被认识到的产生干扰素的能力。这些大鼠干扰素对不同来源细胞提供的最佳跨物种抗病毒保护,以同源物种的百分比(100%)表示如下:豚鼠50%,小鼠40%,人和猴均为0%。来自大鼠肺泡巨噬细胞或II型细胞的干扰素对α干扰素敏感的豚鼠细胞的异源抗病毒活性表明,这些细胞因子可能与α样干扰素种类更密切相关。流感病毒和仙台病毒在大鼠肺泡巨噬细胞和II型肺细胞中的生长均受到抑制。本文的研究结果表明,II型细胞可能是肺泡干扰素的主要来源,用于激活抗病毒状态并调节维持肺完整性所需的肺泡细胞功能。

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