Clinical and genetic analysis of a large pedigree with juvenile myoclonic epilepsy

被引：53

作者：

Serratosa, JM

DelgadoEscueta, AV

Medina, MT

Zhang, QW

Iranmanesh, R

Sparkes, RS

机构：

[1] W LOS ANGELES VET AFFAIRS MED CTR, COMPREHENS EPILEPSY PROGRAM 127B, SW REG EPILEPSY CTR, LOS ANGELES, CA 90073 USA

[2] W LOS ANGELES VET AFFAIRS MED CTR, RES SERV, SW REG EPILEPSY CTR, LOS ANGELES, CA 90073 USA

[3] UNIV CALIF LOS ANGELES, CALIF COMPREHENS EPILEPSY PROGRAM, LOS ANGELES, CA USA

[4] UNIV CALIF LOS ANGELES, DEPT NEUROL, LOS ANGELES, CA 90024 USA

[5] UNIV CALIF LOS ANGELES, DEPT MED, DIV MED GENET, LOS ANGELES, CA 90024 USA

[6] UNIV NACL AUTONOMA HONDURAS, DIRECC INVEST CIENT, TEGUCIGALPA, HONDURAS

来源：

ANNALS OF NEUROLOGY | 1996年 / 39卷 / 02期

关键词：

D O I：

10.1002/ana.410390208

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Juvenile myoclonic epilepsy is a common type of idiopathic generalized epilepsy characterized by myoclonic, generalized tonic-clonic, and in 30% of patients, absence seizures. We studied a three-generation pedigree of 33 members, 10 of whom were clinically affected with juvenile myoclonic epilepsy or presented with subclinical electroencephalographic (EEG) 3.5- to 6.0-Hz diffuse polyspike-wave or spike-wave complexes. Juvenile myoclonic epilepsy and the EEG trait segregated as an autosomal dominant trait with 70% penetrance. Linkage analysis using this model showed significant linkage to four microsatellite markers centromeric to human leukocyte antigen (HLA) in chromosome Gp. Maximum lod scores of 3.43 at theta(m=f) = 0.00 for D6S272, D6S466, D6S257, and D6S402 were obtained. Recombinant events in 2 affected members defined the gene region to a 43-cM interval Banked by D6S258 (HLA region) and D6S313 (centro-mere). Our results in this large family provide evidence that a gene responsible for juvenile myoclonic epilepsy and the subclinical, 3.5- to 6.0-Hz, polyspike-wave or spike-wave EEG pattern is located in chromosome 6p.

引用

页码：187 / 195

页数：9

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