Recessive Schwartz-Jampel syndrome (SJS']JS): Confirmation of linkage to chromosome 1p, evidence of genetic homogeneity and reduction of the SJS']JS locus to a 3-cM interval

被引:21
作者
Fontaine, B
Nicole, S
Topaloglu, H
BenHamida, C
Beighton, P
Spaans, F
Cantu, JMA
Bakouri, S
Romero, N
Ricker, K
BarrosNunez, P
Ponsot, G
BenHamida, M
Weissenbach, J
Hentati, F
LehmannHorn, F
机构
[1] HOP LA PITIE SALPETRIERE,INSERM U134,F-75651 PARIS 13,FRANCE
[2] HACETTEPE UNIV,FAC MED,TR-06100 ANKARA,TURKEY
[3] INST NATL NEUROL,TUNIS,TUNISIA
[4] UNIV CAPE TOWN,DEPT HUMAN GENET,ZA-7925 CAPE TOWN,SOUTH AFRICA
[5] UNIV LIMBURG,DEPT CLIN NEUROPHYSIOL,NL-6200 MD MAASTRICHT,NETHERLANDS
[6] CTR INVEST BIOMED DE OCCIDENTE,GUADALAJARA,JALISCO,MEXICO
[7] CHU BENI MESSOUS,DIV PEDIAT,ALGIERS,ALGERIA
[8] HOP PARIS,PARIS,FRANCE
[9] UNIV ULM,D-7900 ULM,GERMANY
[10] GENETHON,EVRY,FRANCE
来源
HUMAN GENETICS | 1996年 / 98卷 / 03期
关键词
D O I
10.1007/s004390050225
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Schwartz-Jampel syndrome (SJS), or chondrodystrophic myotonia, is a rare autosomal recessive disorder characterized by generalized myotonia resulting in a particular, recognizable facies and osteoarticular abnormalities, Some of us have recently shown genetic linkage of SJS to a locus on lp34-p36.1 in five families, Here, we show by homozygosity mapping and segregation analysis that eight new families are most likely linked to the SJS locus on chromosome 1, confirming the localization of SJS to chromosome Ip and suggesting genetic homogeneity. Recombination events reduced the SJS locus from a generic interval of 8 to 3 cM, which should facilitate the identification of the SJS gene, Low clinical variability was observed between the studied families, except for osteoarticular abnormalities, Since the severity and the location of osteoarticular abnormalities varied from one individual to another, even in the same Families, other factors than the SJS gene itself, genetic or epigenetic, might contribute to the phenotype.
引用
收藏
页码:380 / 385
页数:6
相关论文
共 34 条
[1]  
BEIGHTON P, 1973, CLIN GENET, V4, P548
[2]  
BENHAMIDA M, 1991, REV NEUROL, V147, P279
[3]  
BENOTHMANE K, 1995, AM J HUM GENET, V57, P732
[4]  
BROWN SB, 1975, NEUROLOGY, V25, P365
[5]   GENETIC-MAPPING OF CHRONIC CHILDHOOD-ONSET SPINAL MUSCULAR-ATROPHY TO CHROMOSOME-5Q11.2-13.3 [J].
BRZUSTOWICZ, LM ;
LEHNER, T ;
CASTILLA, LH ;
PENCHASZADEH, GK ;
WILHELMSEN, KC ;
DANIELS, R ;
DAVIES, KE ;
LEPPERT, M ;
ZITER, F ;
WOOD, D ;
DUBOWITZ, V ;
ZERRES, K ;
HAUSMANOWAPETRUSEWICZ, I ;
OTT, J ;
MUNSAT, TL ;
GILLIAM, TC .
NATURE, 1990, 344 (6266) :540-541
[6]   DETECTION OF AN UNSTABLE FRAGMENT OF DNA SPECIFIC TO INDIVIDUALS WITH MYOTONIC-DYSTROPHY [J].
BUXTON, J ;
SHELBOURNE, P ;
DAVIES, J ;
JONES, C ;
VANTONGEREN, T ;
ASLANIDIS, C ;
DEJONG, P ;
JANSEN, G ;
ANVRET, M ;
RILEY, B ;
WILLIAMSON, R ;
JOHNSON, K .
NATURE, 1992, 355 (6360) :547-548
[7]   SCHWARTZ-JAMPEL SYNDROME - CLINICAL, ELECTROPHYSIOLOGICAL AND HISTOPATHOLOGICAL STUDY OF A SEVERE VARIANT [J].
CAO, A ;
CIANCHETTI, C ;
CALISTI, L ;
DEVIRGILIIS, S ;
FERRELI, A ;
TANGHERONI, W .
JOURNAL OF THE NEUROLOGICAL SCIENCES, 1978, 35 (2-3) :175-187
[8]  
Desbois J C, 1977, Ann Pediatr (Paris), V24, P563
[9]  
DOERFLINGER N, 1995, AM J HUM GENET, V56, P1116
[10]   TOWARD A MOLECULAR UNDERSTANDING OF SKELETAL DEVELOPMENT [J].
ERLEBACHER, A ;
FILVAROFF, EH ;
GITELMAN, SE ;
DERYNCK, R .
CELL, 1995, 80 (03) :371-378
1234