Disordered water channel expression and distribution in acquired nephrogenic diabetes insipidus.

D Marples, J Frøkiaer, M A Knepper, S Nielsen
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Abstract

A series of recent studies have demonstrated that expression of aquaporin-2 (AQP2), the vasopressin-regulated water channel of the kidney collecting duct, is greatly reduced in acquired forms of nephrogenic diabetes insipidus (NDI). In some forms of NDI, there is also impaired delivery of these channels to the apical plasma membrane, where they permit water reabsorption from the urine. The combination of these factors is likely to underlie the urinary concentrating defect that defines these conditions. Direct infusion of vasopressin causes an increase in AQP2 expression, probably via a rise in cytosolic adenosine 3:5-cyclic phosphate, which also acts as the second messenger, triggering the delivery of AQP2 to the plasma membrane. However, it is clear from the studies described that there are also vasopressin-independent pathways that regulate the expression of AQP2, some of which appear to reflect intranephric changes, whereas others involve systemic signals. These studies also show that recovery of AQP2 expression, even after correction of the underlying condition, can be slow, consistent with the clinical observation that recovery of urinary-concentrating ability often takes weeks or months. An understanding of the cellular signals and mechanisms responsible for the decrease in AQP2 expression may make it possible to develop treatments for this common clinical problem.

获得性肾源性尿崩症水通道表达与分布紊乱。
最近的一系列研究表明,在获得性肾源性尿囊症(NDI)中,水通道蛋白-2 (AQP2)的表达大大降低,AQP2是肾收集管中抗利尿激素调节的水通道。在某些形式的NDI中,这些通道向顶质膜的输送也受到损害,在那里它们允许尿液中的水分重新吸收。这些因素的结合可能是定义这些条件的尿浓缩缺陷的基础。直接输注抗利尿激素导致AQP2表达增加,可能是通过胞质腺苷3:5-环磷酸的增加,而胞质腺苷3:5-环磷酸也是第二信使,触发AQP2向质膜的传递。然而,从所描述的研究中可以清楚地看出,也有不依赖于抗利尿激素的途径调节AQP2的表达,其中一些似乎反映了肾内的变化,而另一些则涉及全身信号。这些研究还表明,即使在基础条件得到纠正后,AQP2表达的恢复也可能是缓慢的,这与临床观察一致,即尿浓缩能力的恢复往往需要数周或数月。了解导致AQP2表达减少的细胞信号和机制可能使开发治疗这一常见临床问题成为可能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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