Clinical and molecular features of type 1 pseudohypoaldosteronism.

Hormone research Pub Date : 2009-01-01 Epub Date: 2009-06-30 DOI:10.1159/000224334
Felix G Riepe
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引用次数: 108

Abstract

Pseudohypoaldosteronism (PHA) is a rare heterogeneous syndrome of mineralocorticoid resistance causing insufficient potassium and hydrogen secretion. PHA type 1 (PHA1) causes neonatal salt loss, failure to thrive, dehydration and circulatory shock. Two different forms of PHA1 can be distinguished on the clinical and genetic level, showing either a systemic or a renal form of mineralocorticoid resistance. This review provides an overview on transepithelial sodium reabsorption and on clinical features and the underlying molecular pathology of systemic and renal PHA1 caused by mutations in the subunit genes (SCNN1A, SCNN1B, SCNN1G) of the epithelial sodium channel (ENaC) and the mineralocorticoid receptor coding gene NR3C2. The in vitro investigation of several mutants has resulted in important progress in the understanding of the physiology of ENaC and the mineralocorticoid receptor. Some mutations are discussed in more detail to demonstrate some of these findings. A better clinical work-up of the patients suffering from PHA1 may delineate additional associations between the genotype and phenotype in the future.

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1型假性醛固酮减少症的临床和分子特征。
假性醛固酮减少症(PHA)是一种罕见的矿物皮质激素抵抗的异质性综合征,引起钾和氢分泌不足。PHA1型(PHA1)导致新生儿盐分流失,发育失败,脱水和循环性休克。在临床和遗传水平上可以区分两种不同形式的PHA1,显示矿皮质激素抵抗的系统性或肾性形式。本文综述了上皮钠离子通道(ENaC)亚基基因(SCNN1A、SCNN1B、SCNN1G)和矿化皮质激素受体编码基因NR3C2突变引起的全身和肾脏PHA1的临床特征和潜在分子病理。几个突变体的体外研究在ENaC和矿皮质激素受体的生理学理解方面取得了重要进展。对一些突变进行了更详细的讨论,以证明其中的一些发现。对患有PHA1的患者进行更好的临床检查可能会在未来描述基因型和表型之间的其他关联。
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Hormone research
Hormone research 医学-内分泌学与代谢
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