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肺炎支原体感染后大鼠气道中表达MHC II类分子的细胞在形状和数量上的快速变化。

Rapid changes in shape and number of MHC class II expressing cells in rat airways after Mycoplasma pulmonis infection.

作者信息

Umemoto Eric Y, Brokaw James J, Dupuis Marc, McDonald Donald M

机构信息

Cardiovascular Research Institute, Department of Anatomy, and Comprehensive Cancer Center, University of California, San Francisco, CA 94143, USA.

出版信息

Cell Immunol. 2002 Dec;220(2):107-15. doi: 10.1016/s0008-8749(03)00026-1.

Abstract

Mycoplasma pulmonis infection in rodents causes a chronic inflammatory airway disease with a strong immunological component, leading to mucosal remodeling and angiogenesis. We sought to determine the effect of this infection on the shape and number of dendritic cells and other major histocompatibility complex (MHC) class II expressing cells in the airway mucosa of Wistar rats. Changes in the shape of subepithelial OX6 (anti-MHC class II)-immunoreactive cells were evident in the tracheal mucosa 2 days after intranasal inoculation with M. pulmonis. By 1 week, the shape of the cells had changed from stellate to rounded (mean shape index increased from 0.42 to 0.77). The number of OX6-positive cells was increased 6-fold at 1 week and 16-fold at 4 weeks. Coincident with these changes, many columnar epithelial cells developed OX6 immunoreactivity, which was still present at 4 weeks. We conclude that M. pulmonis infection creates a potent immunologic stimulus that augments and transforms the OX6-immunoreactive cell population in the airways by changing the functional state of airway dendritic cells, initiating an influx of MHC class II expressing cells, and activating expression of MHC class II molecules by airway epithelial cells.

摘要

啮齿动物肺部支原体感染会引发一种具有强烈免疫成分的慢性炎症性气道疾病,导致黏膜重塑和血管生成。我们试图确定这种感染对Wistar大鼠气道黏膜中树突状细胞以及其他主要组织相容性复合体(MHC)II类表达细胞的形态和数量的影响。鼻内接种肺部支原体2天后,气管黏膜上皮下OX6(抗MHC II类)免疫反应性细胞的形态变化明显。到第1周时,细胞形态从星状变为圆形(平均形态指数从0.42增加到0.77)。OX6阳性细胞数量在第1周增加了6倍,在第4周增加了16倍。与这些变化同时发生的是,许多柱状上皮细胞出现了OX6免疫反应性,在第4周时仍然存在。我们得出结论,肺部支原体感染产生了一种强大的免疫刺激,通过改变气道树突状细胞的功能状态、引发MHC II类表达细胞的流入以及激活气道上皮细胞中MHC II类分子的表达,增强并改变了气道中OX6免疫反应性细胞群体。

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