首页> 外文期刊>Virchows Archiv: an international journal of pathology >Expression of vascular adhesion protein-1 in normal and inflamed mice lungs and normal human lungs.
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Expression of vascular adhesion protein-1 in normal and inflamed mice lungs and normal human lungs.

机译:正常和发炎的小鼠肺和正常人肺中血管粘附蛋白-1的表达。

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摘要

Recently, vascular adhesion protein-1 (VAP-1) was implicated in adhesion and transmigration of lymphocytes across endothelial cells in liver and other organs. There is very little information on VAP-1 expression in normal and inflamed lungs. Therefore, we conducted a study to localize VAP-1 in normal mice and human lungs and in two distinct murine models of lung inflammation. Normal mice and human lungs revealed VAP-1 expression in the endothelium of large and mid-sized pulmonary vessels but not in alveolar septae, airway epithelium or blood cells. Mice that lack the lpr(-/-) gene and develop extensive lymphocytic infiltration in their lungs showed VAP-1 expression similar to the normal mice lungs. Mice subjected to cecal ligation and puncture developed acute lung inflammation and showed VAP-1 not only in endothelial cells but also in inflammatory cells in perivascular areas at 72 h after the procedure. We concluded that VAP-1 expression may contribute to the functional heterogeneity of endothelial cells within the lung to create distinct sites for the recruitment of inflammatory cells. Furthermore, since VAP-1 is expressed over a longer period of time in inflamed lungs, it may even be a suitable target for drug delivery and therapeutic manipulations.
机译:最近,血管粘附蛋白-1(VAP-1)参与了淋巴细胞在肝脏和其他器官中跨内皮细胞的粘附和迁移。在正常和发炎的肺中,关于VAP-1表达的信息很少。因此,我们进行了一项研究,以将VAP-1定位在正常小鼠和人的肺部以及两种不同的小鼠肺炎症模型中。正常小鼠和人肺在大中型肺血管的内皮中显示VAP-1表达,但在肺泡隔,气道上皮或血细胞中则未显示。缺少lpr(-/-)基因并在其肺部形成广泛的淋巴细胞浸润的小鼠,其VAP-1表达与正常小鼠的肺相似。盲肠结扎和穿刺的小鼠在手术后72小时出现急性肺部炎症,不仅在内皮细胞中而且在血管周围区域的炎症细胞中显示VAP-1。我们得出的结论是,VAP-1表达可能有助于肺内内皮细胞的功能异质性,从而创造出炎症细胞募集的独特位点。此外,由于VAP-1在发炎的肺中会在更长的时间内表达,它甚至可能成为药物输送和治疗操作的合适靶标。

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