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首页> 外文期刊>American Journal of Physiology >Vasopressin regulation of sodium transport in the distal nephron and collecting duct
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Vasopressin regulation of sodium transport in the distal nephron and collecting duct

机译:血管加压素调节远端肾脏和收集管道中的钠输送

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摘要

Arginine vasopressin (AVP) is released from the posterior pituitary gland during states of hyperosmolality or hypovolemia. AVP is a peptide hormone, with antidiuretic and antinatriuretic properties. It allows the kidneys to increase body water retention predominantly by increasing the cell surface expression of aquaporin water channels in the collecting duct alongside increasing the osmotic driving forces for water reabsorption. The antinatriuretic effects of AVP are mediated by the regulation of sodium transport throughout the distal nephron, from the thick ascending limb through to the collecting duct, which in turn partially facilitates osmotic movement of water. In this review, we will discuss the regulatory role of AVP in sodium transport and summarize the effects of AVP on various molecular targets, including the sodium-potassium-chloride cotransporter NKCC2, the thiazide-sensitive sodium-Chloride cotransporter NCC, and the epithelial sodium channel ENaC.
机译:在高渗或缓解血症的状态期间,精氨酸血管加压素(AVP)从后脑后腺释放。 AVP是一种肽激素,具有抗性和抗湿性性质。 它允许肾脏主要通过增加收集管道中的水上蛋白水道的细胞表面表达,增加了水上的渗透驱动力用于水再吸收的渗透驱动力来增加体液水。 AVP的抗肾炎效应由整个远端肾的钠运输的调节介导,从厚的上升肢体到收集管道,这又促进了水的渗透运动。 在本综述中,我们将讨论AVP在钠运输中的调节作用,并总结AVP对各种分子靶标的作用,包括氯化钠COTRANSPORTER NKCC2,噻嗪敏感性氯化钠COT转运者NCC和上皮钠 频道ENAC。

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