噻唑烷二酮类药物引起的液体潴留与集合管α-上皮钠通道活性无关。

Thiazolidinedione-induced fluid retention is independent of collecting duct alphaENaC activity.

作者信息

Vallon Volker, Hummler Edith, Rieg Timo, Pochynyuk Oleh, Bugaj Vladislav, Schroth Jana, Dechenes Georges, Rossier Bernard, Cunard Robyn, Stockand James

机构信息

Nephrology and Hypertension, Department of Medicine, University of California, San Diego, and Veterans Affairs San Diego Healthcare System, 3350 La Jolla Village Drive (9151), San Diego, California 92161, USA.

出版信息

J Am Soc Nephrol. 2009 Apr;20(4):721-9. doi: 10.1681/ASN.2008040415. Epub 2009 Jan 21.

DOI:10.1681/ASN.2008040415

PMID:19158355

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2663822/

Abstract

Thiazolidinediones are agonists of peroxisome proliferator-activated receptor gamma (PPARgamma) that can induce fluid retention and weight gain through unclear mechanisms. To test a proposed role for the epithelial sodium channel ENaC in thiazolidinedione-induced fluid retention, we used mice with conditionally inactivated alphaENaC in the collecting duct (Scnn1a(loxloxCre) mice). In control mice, rosiglitazone did not alter plasma aldosterone levels or protein expression of ENaC subunits in the kidney, but did increase body weight, plasma volume, and the fluid content of abdominal fat pads, and decreased hematocrit. Scnn1a(loxloxCre) mice provided functional evidence for blunted Na+ uptake in the collecting duct, but still exhibited rosiglitazone-induced fluid retention. Moreover, treatment with rosiglitazone or pioglitazone did not significantly alter the open probability or number of ENaC channels per patch in isolated, split-open cortical collecting ducts of wild-type mice. Finally, patch-clamp studies in primary mouse inner medullary collecting duct cells did not detect ENaC activity but did detect a nonselective cation channel upregulated by pioglitazone. These data argue against a primary and critical role of ENaC in thiazolidinedione-induced fluid retention.

摘要

噻唑烷二酮类药物是过氧化物酶体增殖物激活受体γ（PPARγ）的激动剂，可通过不明机制导致液体潴留和体重增加。为了验证上皮钠通道ENaC在噻唑烷二酮类药物诱导的液体潴留中的作用，我们使用了集合管中αENaC条件性失活的小鼠（Scnn1a(loxloxCre)小鼠）。在对照小鼠中，罗格列酮不改变血浆醛固酮水平或肾脏中ENaC亚基的蛋白表达，但确实增加了体重、血浆容量和腹部脂肪垫的液体含量，并降低了血细胞比容。Scnn1a(loxloxCre)小鼠为集合管中Na+摄取减弱提供了功能证据，但仍表现出罗格列酮诱导的液体潴留。此外，用罗格列酮或吡格列酮治疗并未显著改变野生型小鼠分离的、劈开的皮质集合管中每个膜片上ENaC通道的开放概率或数量。最后，对原代小鼠内髓集合管细胞的膜片钳研究未检测到ENaC活性，但检测到一种由吡格列酮上调的非选择性阳离子通道。这些数据表明ENaC在噻唑烷二酮类药物诱导的液体潴留中不发挥主要和关键作用。

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