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首页> 外文期刊>American Journal of Physiology >Expression and functional implications of CCR2 expression on murine alveolar epithelial cells.
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Expression and functional implications of CCR2 expression on murine alveolar epithelial cells.

机译:CCR2表达在鼠肺泡上皮细胞上的表达及其功能意义。

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Acute lung injury results in damage to the alveolar epithelium, leading to leak of proteins into the alveolar space and impaired gas exchange. Lung function can be restored only if the epithelial layer is restored. The process of reepithelialization requires migration of lung epithelial cells to cover denuded basement membranes. The factors that control the migration of lung epithelial cells are incompletely understood. We examined isolated murine type II alveolar epithelial cells (AECs) for expression of CC chemokine receptor 2 (CCR2) and functional consequences of the binding of the main CCR2 ligand monocyte chemoattractant protein-1 (MCP-1). We found that primary AECs bound MCP-1 and expressed CCR2 mRNA. These cells demonstrated functional consequences of CCR2 expression with migration in response to MCP-1 in chemotaxis/haptotaxis assays. Primary AECs cultured from mice lacking CCR2 did not respond to MCP-1. Monolayers of AECs lacking CCR2 demonstrated delayed closure of mechanical wounds compared with AEC monolayers expressing CCR2. Delayed closure of mechanical wounds of wild-type AECs was also demonstrated in the presence of anti-MCP-1 antibody. These data demonstrate for the first time that AECs express CCR2 and are capable of using this receptor for chemotaxis and healing of wounds. CCR2-MCP-1 interactions may be important in the process of reepithelialization after lung injury.
机译:急性肺损伤导致肺泡上皮受损,导致蛋白质渗入肺泡腔并损害气体交换。仅在上皮层恢复后才能恢复肺功能。再上皮化的过程需要肺上皮细胞迁移以覆盖裸露的基底膜。控制肺上皮细胞迁移的因素尚不完全清楚。我们检查了分离的鼠类II型肺泡上皮细胞(AEC)的CC趋化因子受体2(CCR2)的表达以及主要CCR2配体单核细胞趋化蛋白1(MCP-1)结合的功能后果。我们发现初级AEC绑定MCP-1,并表达CCR2 mRNA。这些细胞在趋化/触觉测定中显示出响应MCP-1迁移而迁移的CCR2表达的功能后果。从缺乏CCR2的小鼠培养的原代AEC对MCP-1无反应。与表达CCR2的AEC单层相比,缺少CCR2的AEC的单层表现出机械伤口闭合延迟。在抗MCP-1抗体的存在下,野生型AEC的机械伤口的延迟闭合也被证实。这些数据首次证明AEC表达CCR2,并且能够使用该受体进行趋化性和伤口愈合。 CCR2-MCP-1相互作用在肺损伤后再上皮形成过程中可能很重要。

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