Combi Romina, Dalprà Leda, Malcovati Massimo, Oldani Alessandro, Tenchini Maria Luisa, Ferini-Strambi Luigi
Department of Biology and Genetics for Medical Sciences, University of Milan, Via Viotti 3/5, 20133 Milan, Italy.
Brain Res Bull. 2004 Jun 30;63(5):353-9. doi: 10.1016/j.brainresbull.2003.12.007.
Mutations responsible for autosomal dominant nocturnal frontal lobe epilepsy have been identified in two members of the neuronal nicotinic acetylcholine receptor gene family: CHRNA4(ENFL1 locus) and CHRNB2 (ENFL3 locus) coding for alpha4 and beta2 subunit, respectively. However, mutations in these genes account for only a minority (less than 10%) of cases. For a third ADNFLE locus (ENFL2) on chromosome 15q24 the gene was not identified. The involvement of the three loci in the pathogenesis of ADNFLE was investigated in 12 unrelated Italian families, selected on the basis of anamnestic and video-polysomnographic data. Compliant family members were typed for polymorphic markers spanning the analyzed chromosome regions. Linkage analyses excluded association of all chromosome regions with ADNFLE in 72% of cases. In two, four and one families it was impossible to ascertain or exclude association with ENFL1, ENFL2, or ENFL3, respectively, however, no mutations have been detected in the nicotinic receptor genes located in these regions. These data strongly suggest that ENFL1, ENFL2 and ENFL3 are minor loci for the disease and point to the existence of at least a fourth locus for ADNFLE.
分别编码α4和β2亚基的CHRNA4(ENFL1位点)和CHRNB2(ENFL3位点)。然而,这些基因中的突变仅占病例的少数(不到10%)。对于位于15q24染色体上的第三个ADNFLE位点(ENFL2),该基因尚未被鉴定。基于病史和视频多导睡眠图数据,在12个无亲缘关系的意大利家族中研究了这三个位点在ADNFLE发病机制中的作用。对符合条件的家庭成员进行了跨越分析染色体区域的多态性标记分型。连锁分析在72%的病例中排除了所有染色体区域与ADNFLE的关联。在两个、四个和一个家族中,分别无法确定或排除与ENFL1、ENFL2或ENFL3的关联,然而,在这些区域的烟碱型受体基因中未检测到突变。这些数据强烈表明,ENFL1、ENFL2和ENFL3是该疾病的次要位点,并指出至少存在第四个ADNFLE位点。