Mutations in subunits of the epithelial sodium channel cause salt wasting with hyperkalaemic acidosis, pseudohypoaldosteronism type 1

被引：627

作者：

Chang, SS

Grunder, S

Hanukoglu, A

Rosler, A

Mathew, PM

Hanukoglu, I

Schild, L

Lu, Y

Shimkets, RA

NelsonWilliams, C

Rossier, BC

Lifton, RP

机构：

[1] YALE UNIV, SCH MED,HOWARD HUGHES MED INST,DEPT GENET, BOYER CTR MOLEC MED, NEW HAVEN, CT 06510 USA

[2] YALE UNIV, SCH MED, DEPT MED, NEPHROL SECT, NEW HAVEN, CT 06510 USA

[3] UNIV LAUSANNE, INST PHARMACOL & TOXICOL, CH-1005 LAUSANNE, SWITZERLAND

[4] E WOLFSON HOSP, DEPT PEDIAT, HOLON, ISRAEL

[5] TEL AVIV UNIV, SACKLER SCH MED, IL-69978 TEL AVIV, ISRAEL

[6] HEBREW UNIV JERUSALEM, HADASSAH MED CTR, DEPT ENDOCRINOL & METAB, JERUSALEM, ISRAEL

[7] DHAHRAN HLTH CTR, DEPT PEDIAT, DHAHRAN, SAUDI ARABIA

[8] COLL JUDEA & SAMARIA, RES INST, ARIEL, ISRAEL

[9] SOURASKY MED CTR, INST ENDOCRINOL, TEL AVIV, ISRAEL

来源：

NATURE GENETICS | 1996年 / 12卷 / 03期

关键词：

D O I：

10.1038/ng0396-248

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Autosomal recessive pseudohypoaldosteronism type I is a rave life-threatening disease characterized by severe neonatal salt wasting, hyperkalaemia, metabolic acidosis, and unresponsiveness to mineralocorticoid hormones. Investigation of affected offspring of consanguineous union reveals mutations in either the alpha or beta subunits of the amiloride-sensitive epithelial sodium channel in five kindreds. These mutations are homozygous in affected subjects, co-segregate with the disease, and introduce frameshift, premature termination or missense mutations that result in loss of channel activity. These findings demonstrate the molecular basis and explain the pathophysiology of this disease.

引用

页码：248 / 253

页数：6

共 40 条

[1] ALDOSTERONE-RECEPTOR DEFICIENCY IN PSEUDOHYPOALDOSTERONISM [J].