Diagnosis of Liddle syndrome by genetic analysis of β and γ subunits of epithelial sodium channel -: a report of five affected family members

被引：23

作者：

Gao, PJ

Zhang, KX

Zhu, DL

He, X

Han, ZY

Zhan, YM

Yang, LW

机构：

[1] Shanghai Second Med Univ, Ruijin Hosp, Shanghai Inst Hypertens, Shanghai 200025, Peoples R China

[2] Sanmenxia Hosp, Sanmenxia, Henan Province, Peoples R China

来源：

JOURNAL OF HYPERTENSION | 2001年 / 19卷 / 05期

关键词：

Liddle syndrome; hypertension; epithelial sodium channel; genetics;

D O I：

10.1097/00004872-200105000-00008

中图分类号：

R6 [外科学];

学科分类号：

1002 ; 100210 ;

摘要：

Objective To screen the gene mutation in beta and gamma subunits of the epithelial sodium channel (ENaC) of a Chinese family, some of whose members are clinically diagnosed as suffering from Liddle syndrome. Methods Twelve family members were recruited to the study, Among them, two brothers had been clinically diagnosed as suffering from Liddle syndrome. Peripheral blood samples were collected from all members of the family and total genomic DNA was prepared for genetic analysis. Polymerase chain reaction (PCR) was used for amplifying the last exon of beta (codon 513-673) and gamma (codon 503-632) subunits of the ENaC gene. PCR products were purified and subjected to a direct DNA sequence analysis, Results Genetic analysis of the beta ENaC gene revealed a missense mutation of CCC to CTC at codon 616 in four middle-aged men of the second generation and one young woman of the third generation. There was no mutation of the gamma ENaC gene in any of the individuals examined, Conclusion Through direct DNA sequencing analysis, we diagnosed the disease present in five members of a Chinese family as Liddle syndrome, and excluded it in some other young offspring suffering from the monogenic disease, Our results provide further evidence that Pro(816) is a critical amino acid that has a key role in the inhibition of sodium channel activity. J Hypertens 19:885-889 (C) 2001 Lippincott Williams & Wilkins.

引用

页码：885 / 889

页数：5

共 17 条

[1] LIDDLES SYNDROME REVISITED - A DISORDER OF SODIUM-REABSORPTION IN THE DISTAL TUBULE
BOTEROVELEZ, M
CURTIS, JJ
WARNOCK, DG
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1994, 330 (03) : 178 - 181
[2] AMILORIDE-SENSITIVE EPITHELIAL NA+ CHANNEL IS MADE OF 3 HOMOLOGOUS SUBUNITS
CANESSA, CM
SCHILD, L
BUELL, G
THORENS, B
GAUTSCHI, I
HORISBERGER, JD
ROSSIER, BC
[J]. NATURE, 1994, 367 (6462) : 463 - 467
[3] EPITHELIAL SODIUM-CHANNEL RELATED TO PROTEINS INVOLVED IN NEURODEGENERATION
CANESSA, CM
HORISBERGER, JD
ROSSIER, BC
[J]. NATURE, 1993, 361 (6411) : 467 - 470
[4] CHEN QR, 1987, CHIN J NEPHROL, V3, P226
[5] Epithelial sodium channels and hypertension
Fuller, PJ
[J]. JOURNAL OF HYPERTENSION, 1996, 14 (12) : 1383 - 1386
[6] Inhibition of the epithelial Na+ channel by interaction of Nedd4 with a PY motif deleted in Liddle's syndrome
Goulet, CC
Volk, KA
Adams, CM
Prince, LS
Stokes, JB
Snyder, PM
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1998, 273 (45) : 30012 - 30017
[7] GUSTINCICH S, 1991, BIOTECHNIQUES, V11, P298
[8] A DE-NOVO MISSENSE MUTATION OF THE BETA-SUBUNIT OF THE EPITHELIAL SODIUM-CHANNEL CAUSES HYPERTENSION AND LIDDLE SYNDROME, IDENTIFYING A PROLINE-RICH SEGMENT CRITICAL FOR REGULATION OF CHANNEL ACTIVITY
HANSSON, JH
SCHILD, L
LU, Y
WILSON, TA
GAUTSCHI, I
SHIMKETS, R
NELSONWILLIAMS, C
ROSSIER, BC
LIFTON, RP
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (25) : 11495 - 11499
[9] HYPERTENSION CAUSED BY A TRUNCATED EPITHELIAL SODIUM-CHANNEL GAMMA-SUBUNIT - GENETIC-HETEROGENEITY OF LIDDLE SYNDROME
HANSSON, JH
NELSONWILLIAMS, C
SUZUKI, H
SCHILD, L
SHIMKETS, R
LU, Y
CANESSA, C
IWASAKI, T
ROSSIER, B
LIFTON, RP
[J]. NATURE GENETICS, 1995, 11 (01) : 76 - 82
[10] Genotype-phenotype analysis of a newly discovered family with Liddle's syndrome
Jeunemaitre, X
Bassilana, F
Persu, A
Dumont, C
Champigny, G
Lazdunski, M
Corvol, P
Barbry, P
[J]. JOURNAL OF HYPERTENSION, 1997, 15 (10) : 1091 - 1100

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