Gereke Marcus, Gröbe Lothar, Prettin Silvia, Kasper Michael, Deppenmeier Stefanie, Gruber Achim D, Enelow Richard I, Buer Jan, Bruder Dunja
Immune Regulation Group, Helmholtz Centre for Infection Research, Braunschweig, Germany.
Respir Res. 2007 Jul 4;8(1):47. doi: 10.1186/1465-9921-8-47.
Although the contribution of alveolar type II epithelial cell (AEC II) activities in various aspects of respiratory immune regulation has become increasingly appreciated, our understanding of the contribution of AEC II transcriptosome in immunopathologic lung injury remains poorly understood. We have previously established a mouse model for chronic T cell-mediated pulmonary inflammation in which influenza hemagglutinin (HA) is expressed as a transgene in AEC II, in mice expressing a transgenic T cell receptor specific for a class II-restricted epitope of HA. Pulmonary inflammation in these mice occurs as a result of CD4+ T cell recognition of alveolar antigen. This model was utilized to assess the profile of inflammatory mediators expressed by alveolar epithelial target cells triggered by antigen-specific recognition in CD4+ T cell-mediated lung inflammation.
We established a method that allows the flow cytometric negative selection and isolation of primary AEC II of high viability and purity. Genome wide transcriptional profiling was performed on mRNA isolated from AEC II isolated from healthy mice and from mice with acute and chronic CD4+ T cell-mediated pulmonary inflammation.
T cell-mediated inflammation was associated with expression of a broad array of cytokine and chemokine genes by AEC II cell, indicating a potential contribution of epithelial-derived chemoattractants to the inflammatory cell parenchymal infiltration. Morphologically, there was an increase in the size of activated epithelial cells, and on the molecular level, comparative transcriptome analyses of AEC II from inflamed versus normal lungs provide a detailed characterization of the specific inflammatory genes expressed in AEC II induced in the context of CD4+ T cell-mediated pneumonitis.
An important contribution of AEC II gene expression to the orchestration and regulation of interstitial pneumonitis is suggested by the panoply of inflammatory genes expressed by this cell population, and this may provide insight into the molecular pathogenesis of pulmonary inflammatory states. CD4+ T cell recognition of antigen presented by AEC II cells appears to be a potent trigger for activation of the alveolar cell inflammatory transcriptosome.
尽管肺泡II型上皮细胞(AEC II)活性在呼吸免疫调节各个方面的作用已得到越来越多的认识,但我们对AEC II转录组在免疫病理性肺损伤中的作用仍知之甚少。我们之前建立了一种慢性T细胞介导的肺部炎症小鼠模型,在表达针对HA II类限制性表位的转基因T细胞受体的小鼠中,流感血凝素(HA)作为转基因在AEC II中表达。这些小鼠的肺部炎症是由于CD4 + T细胞识别肺泡抗原所致。该模型用于评估在CD4 + T细胞介导的肺部炎症中,由抗原特异性识别触发的肺泡上皮靶细胞所表达的炎症介质谱。
我们建立了一种方法,可通过流式细胞术阴性选择并分离出高活力和高纯度的原代AEC II。对从健康小鼠以及患有急性和慢性CD4 + T细胞介导的肺部炎症的小鼠分离出的AEC II中提取的mRNA进行全基因组转录谱分析。
T细胞介导的炎症与AEC II细胞表达多种细胞因子和趋化因子基因有关,表明上皮来源的趋化因子对炎症细胞实质浸润有潜在作用。形态学上,活化的上皮细胞大小增加,在分子水平上,对发炎肺与正常肺的AEC II进行比较转录组分析,详细表征了在CD4 + T细胞介导的肺炎背景下AEC II中表达的特定炎症基因。
该细胞群体表达的大量炎症基因表明AEC II基因表达对间质性肺炎的协调和调节有重要作用,这可能为肺部炎症状态的分子发病机制提供见解。CD4 + T细胞识别AEC II细胞呈递的抗原似乎是激活肺泡细胞炎症转录组的有效触发因素。
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