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肺上皮细胞对纤维蛋白原的极化分泌。

Polarized secretion of fibrinogen by lung epithelial cells.

作者信息

Guadiz G, Sporn L A, Goss R A, Lawrence S O, Marder V J, Simpson-Haidaris P J

机构信息

Department of Medicine-Vascular Medicine Unit, University of Rochester School of Medicine and Dentistry, New York.

出版信息

Am J Respir Cell Mol Biol. 1997 Jul;17(1):60-9. doi: 10.1165/ajrcmb.17.1.2730.

Abstract

The lung epithelium has recently been identified as a novel site of fibrinogen (FBG) biosynthesis. A coordinated upregulation of A alpha, B beta, and gamma chain FBG gene transcription occurs upon stimulation of A549 lung epithelial cells with dexamethasone (DEX) and the proinflammatory mediator interleukin-6 (IL-6). Subsequently, the cells synthesize and secrete fully assembled FBG. This study addresses the polarity of such FBG secretion by A549 cells cultured on polycarbonate membrane filters. After induction with IL-6 and DEX, cells were metabolically labeled, and FBG was immunopurified from the apical and basolateral chambers. Analysis by gel electrophoresis revealed that A549 cells secreted newly synthesized FBG in a polarized manner, with the majority (80%) of FBG secreted basolaterally. Consistent with this observation, immunoelectron microscopy using Protein A-gold labeling showed FBG within secretory vesicles in close proximity to the basolateral aspect of the A549 cell membrane. Polarized secretion was microtubule-dependent since depolymerization using colchicine significantly reduced the basolateral component of secretion, causing intracellular retention of FBG. These data provide evidence that FBG is secreted by lung alveolar epithelial cells vectorially toward the basement membrane, which may reflect in vivo processes associated with local injury, inflammation, and repair mechanisms.

摘要

肺上皮细胞最近被确定为纤维蛋白原(FBG)生物合成的新位点。用地塞米松(DEX)和促炎介质白细胞介素-6(IL-6)刺激A549肺上皮细胞后,Aα、Bβ和γ链FBG基因转录会协同上调。随后,细胞合成并分泌完全组装好的FBG。本研究探讨了在聚碳酸酯膜滤器上培养的A549细胞分泌FBG的极性。用IL-6和DEX诱导后,对细胞进行代谢标记,并从顶侧和基底外侧腔室免疫纯化FBG。凝胶电泳分析显示,A549细胞以极化方式分泌新合成的FBG,大部分(80%)FBG从基底外侧分泌。与此观察结果一致,使用蛋白A-金标记的免疫电子显微镜显示,分泌小泡内的FBG靠近A549细胞膜的基底外侧。极化分泌依赖于微管,因为用秋水仙碱解聚微管会显著降低分泌的基底外侧成分,导致FBG在细胞内滞留。这些数据证明,FBG由肺泡上皮细胞向基底膜定向分泌,这可能反映了与局部损伤、炎症和修复机制相关的体内过程。

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