The congenital long QT syndromes from genotype to phenotype: clinical implications

被引:161
作者
Schwartz, PJ
机构
[1] IRCCS Policlin S Matteo, Dept Cardiol, I-27100 Pavia, Italy
[2] Univ Pavia, I-27100 Pavia, Italy
来源
JOURNAL OF INTERNAL MEDICINE | 2006年 / 259卷 / 01期
关键词
genetics; ion channels; left cardiac sympathetic denervation; long QT syndrome; modifier genes; sudden death;
D O I
10.1111/j.1365-2796.2005.01583.x
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The long QT syndrome (LQTS) is a genetic disorder responsible for many sudden deaths before age 20. The identification of several LQTS genes. all encoding cardiac ion channels, has had a major impact on the management strategy for both patients and family members. Genotype-guided therapy allows more effective individually tailored therapy. Therapeutic options, including beta-blockers. left cardiac sympathetic denervation. and implantable defibrillators are discussed for patients of known and of unknown genotype. The recent identification of modifier genes which amplify the effect of an LOTS mutation may change the approach to risk stratification.
引用
收藏
页码:39 / 47
页数:9
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[1]   Swimming, a gene-specific arrhythmogenic trigger for inherited long QT syndrome [J].
Ackerman, MJ ;
Tester, DJ ;
Porter, CJ .
MAYO CLINIC PROCEEDINGS, 1999, 74 (11) :1088-1094
[2]   K(v)LQT1 and IsK (minK) proteins associate to form the I-Ks cardiac potassium current [J].
Barhanin, J ;
Lesage, F ;
Guillemare, E ;
Fink, M ;
Lazdunski, M ;
Romey, G .
NATURE, 1996, 384 (6604) :78-80
[3]   MOLECULAR MECHANISM FOR AN INHERITED CARDIAC-ARRHYTHMIA [J].
BENNETT, PB ;
YAZAWA, K ;
MAKITA, N ;
GEORGE, AL .
NATURE, 1995, 376 (6542) :683-685
[4]   KCNH2-K897T is a genetic modifier of latent congenital long-QT syndrome [J].
Crotti, L ;
Lundquist, AL ;
Insolia, R ;
Pedrazzini, M ;
Ferrandi, C ;
De Ferrari, GM ;
Vicentini, A ;
Yang, P ;
Roden, DM ;
George, AL ;
Schwartz, PJ .
CIRCULATION, 2005, 112 (09) :1251-1258
[5]   A MOLECULAR-BASIS FOR CARDIAC-ARRHYTHMIA - HERG MUTATIONS CAUSE LONG QT SYNDROME [J].
CURRAN, ME ;
SPLAWSKI, I ;
TIMOTHY, KW ;
VINCENT, GM ;
GREEN, ED ;
KEATING, MT .
CELL, 1995, 80 (05) :795-803
[6]   MAPPING OF BODY-SURFACE POTENTIALS IN PATIENTS WITH THE IDIOPATHIC LONG QT SYNDROME [J].
DEAMBROGGI, L ;
BERTONI, T ;
LOCATI, E ;
STRAMBABADIALE, M ;
SCHWARTZ, PJ .
CIRCULATION, 1986, 74 (06) :1334-1345
[7]   EFFECT OF CALCIUM-CHANNEL BLOCK ON THE WALL-MOTION ABNORMALITY OF THE IDIOPATHIC LONG QT SYNDROME [J].
DEFERRARI, GM ;
NADOR, F ;
BERIA, G ;
SALA, S ;
LOTTO, A ;
SCHWARTZ, PJ .
CIRCULATION, 1994, 89 (05) :2126-2132
[8]   Multiple mechanisms of Na+ channel-linked long-QT syndrome [J].
Dumaine, R ;
Wang, Q ;
Keating, MT ;
Hartmann, HA ;
Schwartz, PJ ;
Brown, AM ;
Kirsch, GE .
CIRCULATION RESEARCH, 1996, 78 (05) :916-924
[9]   CONGENITAL DEAF-MUTISM, FUNCTIONAL HEART DISEASE WITH PROLONGATION OF THE Q-T INTERVAL, AND SUDDEN DEATH [J].
JERVELL, A ;
LANGENIELSEN, F .
AMERICAN HEART JOURNAL, 1957, 54 (01) :59-68
[10]   Identification of a common genetic substrate underlying postpartum cardiac events in congenital long QT syndrome [J].
Khositseth, A ;
Tester, DJ ;
Will, ML ;
Bell, CM ;
Ackerman, MJ .
HEART RHYTHM, 2004, 1 (01) :60-64
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