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水通道蛋白水通道在肾脏和肺中的作用。

Role of aquaporin water channels in kidney and lung.

作者信息

Verkman A S

机构信息

Department of Medicine, Cardiovascular Research Institute, University of California, San Francisco 94143-0521, USA.

出版信息

Am J Med Sci. 1998 Nov;316(5):310-20. doi: 10.1097/00000441-199811000-00004.

Abstract

Several aquaporin-type water channels are expressed in mammalian kidney and lung: AQP1 in lung microvessels and kidney proximal tubule, thin descending limb of Henle, and vasa recta; AQP2 in apical membrane of collecting duct epithelium; AQP3 and AQP4 in basolateral membranes of airway and collecting duct epithelium; and AQP5 in alveolar epithelium. Novel quantitative fluorescence methods demonstrated very high water permeabilities of the alveolar epithelial and endothelial barriers, and moderately high water permeability across distal airways. In the kidney, water permeability is high in proximal tubule and thin descending limb of Henle, and regulated by vasopressin in collecting duct. The author's laboratory has studied the role of aquaporins in organ physiology using transgenic knockout mice lacking specific aquaporins. AQP1 null mice are mildly growth-retarded, manifest a severe urinary concentrating defect, and have reduced water permeability between airspace and capillary compartments. AQP4 null mice appear normal grossly except for a mild defect in maximum urinary concentrating ability. AQP2-deficient humans have hereditary non-X-linked nephrogenic diabetes insipidus (NDI). In transfected mammalian cells, many NDI-causing AQP2 mutants are retained in the endoplasmic reticulum. The author's laboratory has found that "chemical chaperones," that is, small compounds that promote protein folding in vitro, are able to correct defective AQP2 trafficking in cell culture models. The transgenic mouse and mammalian cell models are thus beginning to provide clues about the role of aquaporins in normal physiology and disease.

摘要

几种水通道蛋白类型的水通道在哺乳动物的肾脏和肺中表达

肺微血管、肾近端小管、髓袢细降支和直小血管中表达水通道蛋白1(AQP1);集合管上皮细胞顶端膜中表达水通道蛋白2(AQP2);气道和集合管上皮细胞基底外侧膜中表达水通道蛋白3(AQP3)和水通道蛋白4(AQP4);肺泡上皮细胞中表达水通道蛋白5(AQP5)。新的定量荧光方法显示,肺泡上皮和内皮屏障具有非常高的水通透性,远端气道的水通透性也较高。在肾脏中,近端小管和髓袢细降支的水通透性较高,集合管中的水通透性受血管加压素调节。作者所在的实验室利用缺乏特定水通道蛋白的转基因敲除小鼠研究了水通道蛋白在器官生理学中的作用。水通道蛋白1基因敲除小鼠生长轻度迟缓,表现出严重的尿液浓缩缺陷,气腔与毛细血管腔之间的水通透性降低。水通道蛋白4基因敲除小鼠除最大尿液浓缩能力有轻度缺陷外,大体外观正常。水通道蛋白2缺陷的人类患有遗传性非X连锁肾性尿崩症(NDI)。在转染的哺乳动物细胞中,许多导致NDI的水通道蛋白2突变体保留在内质网中。作者所在的实验室发现,“化学伴侣”,即体外促进蛋白质折叠的小分子化合物,能够纠正细胞培养模型中缺陷性水通道蛋白2的转运。因此,转基因小鼠和哺乳动物细胞模型开始为水通道蛋白在正常生理学和疾病中的作用提供线索。

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