FAMILIAL HYPERTROPHIC CARDIOMYOPATHY IS A GENETICALLY HETEROGENEOUS DISEASE

被引:139
作者
SOLOMON, SD
JARCHO, JA
MCKENNA, W
GEISTERFERLOWRANCE, A
GERMAIN, R
SALERNI, R
SEIDMAN, JG
SEIDMAN, CE
机构
[1] BRIGHAM & WOMENS HOSP,DIV CARDIOVASC,BOSTON,MA 02115
[2] ST GEORGE HOSP,SCH MED,DEPT CARDIOL,LONDON,ENGLAND
[3] CLIN FAMILIALE COATICOOK,COATICOOK,QUEBEC,CANADA
[4] PRESBYTERIAN UNIV HOSP,DIV CARDIOL,PITTSBURGH,PA 15213
[5] HARVARD UNIV,SCH MED,HOWARD HUGHES MED INST,BOSTON,MA 02115
[6] HARVARD UNIV,SCH MED,DEPT GENET,BOSTON,MA 02115
来源
JOURNAL OF CLINICAL INVESTIGATION | 1990年 / 86卷 / 03期
关键词
Familial hypertrophic cardiomyopathy; Heterogeneity; Linkage;
D O I
10.1172/JCI114802
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
We demonstrate that familial hypertrophic cardiomyopathy (FHC), an autosomal dominant disorder of heart muscle, is a genetically heterogeneous disease. The locus responsible for FHC in members of one large kindred was recently mapped to chromosome 14q11-12 (FHC-1). We have characterized three additional unrelated families in which the gene for FHC segregates as an autosomal dominant trait to determine if these disease loci also map to FHC-1. All family members were clinically studied by physical examination, electrocardiogram, and two-dimensional echocardiography. Genetic studies were performed using DNA probes which are derived from loci that are closely linked to FHC-1. In one family the genetic defect maps to the previously identified FHC-1 locus. However, the loci responsible for FHC in two other families were not linked to FHC-1. We conclude that FHC can be caused by defects in at least two loci and is a genetically heterogeneous disorder.
引用
收藏
页码:993 / 999
页数:7
相关论文
共 22 条
[1]  
COX DW, 1989, CYTOGENET CELL GENET, V51, pA2694
[2]   A GENETIC-LINKAGE MAP OF THE HUMAN GENOME [J].
DONISKELLER, H ;
GREEN, P ;
HELMS, C ;
CARTINHOUR, S ;
WEIFFENBACH, B ;
STEPHENS, K ;
KEITH, TP ;
BOWDEN, DW ;
SMITH, DR ;
LANDER, ES ;
BOTSTEIN, D ;
AKOTS, G ;
REDIKER, KS ;
GRAVIUS, T ;
BROWN, VA ;
RISING, MB ;
PARKER, C ;
POWERS, JA ;
WATT, DE ;
KAUFFMAN, ER ;
BRICKER, A ;
PHIPPS, P ;
MULLERKAHLE, H ;
FULTON, TR ;
NG, S ;
SCHUMM, JW ;
BRAMAN, JC ;
KNOWLTON, RG ;
BARKER, DF ;
CROOKS, SM ;
LINCOLN, SE ;
DALY, MJ ;
ABRAHAMSON, J .
CELL, 1987, 51 (02) :319-337
[3]  
HOLCOMBE R F, 1987, Genomics, V1, P287, DOI 10.1016/0888-7543(87)90058-9
[4]   MAPPING A GENE FOR FAMILIAL HYPERTROPHIC CARDIOMYOPATHY TO CHROMOSOME-14Q1 [J].
JARCHO, JA ;
MCKENNA, W ;
PARE, JAP ;
SOLOMON, SD ;
HOLCOMBE, RF ;
DICKIE, S ;
LEVI, T ;
DONISKELLER, H ;
SEIDMAN, JG ;
SEIDMAN, CE .
NEW ENGLAND JOURNAL OF MEDICINE, 1989, 321 (20) :1372-1378
[5]   LINKAGE HETEROGENEITY OF AUTOSOMAL DOMINANT POLYCYSTIC KIDNEY-DISEASE [J].
KIMBERLING, WJ ;
FAIN, PR ;
KENYON, JB ;
GOLDGAR, D ;
SUJANSKY, E ;
GABOW, PA .
NEW ENGLAND JOURNAL OF MEDICINE, 1988, 319 (14) :913-918
[6]   STRATEGIES FOR MULTILOCUS LINKAGE ANALYSIS IN HUMANS [J].
LATHROP, GM ;
LALOUEL, JM ;
JULIER, C ;
OTT, J .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (11) :3443-3446
[7]   PARTIAL CHARACTERIZATION OF THE HUMAN BETA-MYOSIN HEAVY-CHAIN GENE WHICH IS EXPRESSED IN HEART AND SKELETAL-MUSCLE [J].
LICHTER, P ;
UMEDA, PK ;
LEVIN, JE ;
VOSBERG, HP .
EUROPEAN JOURNAL OF BIOCHEMISTRY, 1986, 160 (02) :419-426
[8]   THE GENETICS OF HYPERTROPHIC CARDIOMYOPATHY [J].
MARON, BJ ;
MULVIHILL, JJ .
ANNALS OF INTERNAL MEDICINE, 1986, 105 (04) :610-613
[9]   PATTERNS AND SIGNIFICANCE OF DISTRIBUTION OF LEFT-VENTRICULAR HYPERTROPHY IN HYPERTROPHIC CARDIOMYOPATHY - A WIDE ANGLE, 2 DIMENSIONAL ECHOCARDIOGRAPHIC STUDY OF 125 PATIENTS [J].
MARON, BJ ;
GOTTDIENER, JS ;
EPSTEIN, SE .
AMERICAN JOURNAL OF CARDIOLOGY, 1981, 48 (03) :418-428
[10]   HYPERTROPHIC CARDIOMYOPATHY - INTERRELATIONS OF CLINICAL MANIFESTATIONS, PATHOPHYSIOLOGY, AND THERAPY .1. [J].
MARON, BJ ;
BONOW, RO ;
CANNON, RO ;
LEON, MB ;
EPSTEIN, SE .
NEW ENGLAND JOURNAL OF MEDICINE, 1987, 316 (13) :780-789
123