SCN5A MUTATIONS ASSOCIATED WITH AN INHERITED CARDIAC-ARRHYTHMIA, LONG QT SYNDROME

被引：1302

作者：

WANG, Q

SHEN, JX

SPLAWSKI, I

ATKINSON, D

LI, ZZ

ROBINSON, JL

MOSS, AJ

TOWBIN, JA

KEATING, MT

机构：

[1] UNIV UTAH, HLTH SCI CTR, DEPT HUMAN GENET, SALT LAKE CITY, UT 84112 USA

[2] UNIV UTAH, HLTH SCI CTR, ECCLES PROGRAM HUMAN MOLEC BIOL & GENET, SALT LAKE CITY, UT 84112 USA

[3] UNIV UTAH, HLTH SCI CTR, DIV CARDIOL, SALT LAKE CITY, UT 84112 USA

[4] UNIV ROCHESTER, MED CTR, DEPT COMMUNITY & PREVENT MED, ROCHESTER, NY 14627 USA

[5] UNIV ROCHESTER, MED CTR, DEPT MED, ROCHESTER, NY 14627 USA

[6] BAYLOR COLL MED, DEPT PEDIAT, HOUSTON, TX 77030 USA

[7] BAYLOR COLL MED, DEPT MOLEC & HUMAN GENET, HOUSTON, TX 77030 USA

来源：

CELL | 1995年 / 80卷 / 05期

关键词：

D O I：

10.1016/0092-8674(95)90359-3

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Long QT syndrome (LQT) is an inherited disorder that causes sudden death from cardiac arrhythmias, specifically torsade de pointes and ventricular fibrillation. We previously mapped three LQT loci: LQT1 on chromosome 11p15.5, LQT2 on 7q35-36, and LQT3 on 3p21-24. Here we report genetic linkage between LQT3 and polymorphisms within SCN5A, the cardiac sodium channel gene. Single strand conformation polymorphism and DNA sequence analyses reveal identical intragenic deletions of SCN5A in affected members of two unrelated LQT families. The deleted sequences reside in a region that is important for channel inactivation. These data suggest that mutations in SCN5A cause chromosome 3-linked LQT and indicate a likely cellular mechanism for this disorder.

引用

页码：805 / 811

页数：7

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