Baulac S, Picard F, Herman A, Feingold J, Genin E, Hirsch E, Prud'homme J F, Baulac M, Brice A, LeGuern E
INSERM U289, Hĵpital de la Pitié-Salpêtrière, Paris, France.
Ann Neurol. 2001 Jun;49(6):786-92. doi: 10.1002/ana.1014.
We report a clinical and genetic study of a French family among whom febrile convulsions (FC) are associated with subsequent temporal lobe epilepsy (TLE) in the same individual, without magnetic resonance imaging-identifiable hippocampal abnormalities. Linkage analyses excluded the loci FEB1 and FEB2, previously implicated in FC; the GEFS+1 locus responsible for generalized epilepsy with febrile seizures plus; and the locus implicated in lateral temporal lobe epilepsy. After scanning the entire genome, significant lod scores (>3) for markers on 18qter and suggestive lod scores (>2) for markers on 1q25-q31 were obtained. An analysis of the haplotypes at these two loci supported the hypothesis that two genes segregated with the phenotype. All patients shared common haplotypes for both 1q25-q31 and 18qter chromosomes. All but one unaffected at-risk individuals carried only one, or none, of the disease haplotypes. Under the assumption of digenic inheritance, haplotype reconstruction defined a 26 cM interval on chromosome 1 and a 10 cM interval on chromosome 18. This family suggests that the association between FC and TLE may be observed in the absence of hippocampal structural abnormalities and that they may have, in some cases, a common genetic basis.
我们报告了一个法国家庭的临床和遗传学研究,在这个家庭中,发热惊厥(FC)与同一个体随后发生的颞叶癫痫(TLE)相关,且磁共振成像未发现海马异常。连锁分析排除了先前与FC相关的FEB1和FEB2基因座;排除了与伴有热性惊厥附加症的全身性癫痫相关的GEFS +1基因座;以及与外侧颞叶癫痫相关的基因座。在扫描整个基因组后,获得了18qter上标记的显著对数优势分数(>3)和1q25 - q31上标记的提示性对数优势分数(>2)。对这两个基因座的单倍型分析支持了两个基因与该表型分离的假设。所有患者在1q25 - q31和18qter染色体上都有共同的单倍型。除一名未受影响的高危个体外,所有其他个体仅携带一种或不携带疾病单倍型。在双基因遗传的假设下,单倍型重建在1号染色体上定义了一个26厘摩的区间,并在18号染色体上定义了一个10厘摩的区间。这个家庭表明,在没有海马结构异常的情况下,可能会观察到FC与TLE之间的关联,并且在某些情况下,它们可能有共同的遗传基础。