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质膜和小窝中的水通道蛋白-1提供了跨肺内皮的汞敏感水通道。

Aquaporin-1 in plasma membrane and caveolae provides mercury-sensitive water channels across lung endothelium.

作者信息

Schnitzer J E, Oh P

机构信息

Department of Pathology, Harvard Medical School, Beth Israel Hospital, Boston, Massachusetts 02215, USA.

出版信息

Am J Physiol. 1996 Jan;270(1 Pt 2):H416-22. doi: 10.1152/ajpheart.1996.270.1.H416.

Abstract

Classically, water transport across endothelium of the continuous type found in the microvessels of many organs such as lung was thought to occur almost completely via the paracellular pathway through intercellular junctions. Direct transmembrane and transcellular transport was considered to be minimal. In this study, we focused on the critical transport interface in direct contact with the circulating blood by purifying luminal endothelial cell plasma membranes directly from rat lungs and then isolating the noncoated plasmalemmal vesicles or caveolae from these membranes. Immunoblotting of these fractions showed that the transmembrane water channel protein aquaporin-1 was amply expressed on the endothelial cell surface at levels comparable to rat erythrocyte plasma membranes. It was found concentrated, but not exclusively, in caveolae. The functional role of these water channels in transport was examined in rat lungs perfused in situ with tritiated water by testing known inhibitors of aquaporin-1-mediated transmembrane water transport. Mercurial sulfhydryl reagents such as HgCl2 reversibly reduced tritiated water uptake without affecting small solute transport. Just like certain epithelia, endothelia might express physiologically relevant amounts of aquaporin-1 on their cell surface to permit direct, mercurial-sensitive, transcellular transport of water.

摘要

传统上,人们认为在许多器官(如肺)的微血管中发现的连续型内皮细胞的水运输几乎完全通过细胞间连接的细胞旁途径进行。直接的跨膜和跨细胞运输被认为是极少的。在本研究中,我们通过直接从大鼠肺中纯化管腔内内皮细胞质膜,然后从这些膜中分离出无包被的质膜囊泡或小窝,聚焦于与循环血液直接接触的关键运输界面。对这些组分的免疫印迹显示,跨膜水通道蛋白水通道蛋白-1在内皮细胞表面大量表达,其水平与大鼠红细胞质膜相当。发现它集中,但并非仅集中在小窝中。通过测试水通道蛋白-1介导的跨膜水运输的已知抑制剂,在原位灌注氚标记水的大鼠肺中研究了这些水通道在运输中的功能作用。汞巯基试剂如HgCl2可逆地减少了氚标记水的摄取,而不影响小分子溶质的运输。就像某些上皮细胞一样,内皮细胞可能在其细胞表面表达生理相关量的水通道蛋白-1,以允许水进行直接的、对汞敏感的跨细胞运输。

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