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首页> 外文期刊>Journal of child neurology >The first genome-wide scan in a tunisian family with generalized epilepsy with febrile seizure plus (GEFS+).
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The first genome-wide scan in a tunisian family with generalized epilepsy with febrile seizure plus (GEFS+).

机译:突尼斯家庭伴高热性癫痫发作(GEFS +)的全身性癫痫病的首次全基因组扫描。

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摘要

Generalized epilepsy with febrile seizure plus (GEFS+) is an autosomal dominant disorder. In the literature, 5 responsible genes were identified and 2 novel susceptibility loci for GEFS+ at 2p24 and 8p23-p21 were reported, indicating the genetic heterogeneity of this disorder. The aim of this report is to identify the responsible loci in a large affected Tunisian family by performing a 10cM density genome-wide scan. The highest multipoint logarithm of odds (LOD) score (1.04) was found for D5S407 in the absence of recombination. Two other interesting regions were found around marker D19S210 (LOD=0.799) and D7S484 (LOD=0.61) markers. To fine map these loci, additional markers in 2 regions on 5q13.3 and 7p14.2 were analyzed and positive LOD scores for both loci were obtained. Sequencing of the Sodium channel subunit beta-1 gene (SCN1B) (19q13.1) showed the absence of any causal mutation. Our findings emphasized the genetic heterogeneity of febrile seizures.
机译:伴有高热惊厥(GEFS +)的全身性癫痫是常染色体显性遗传疾病。在文献中,鉴定了5个负责任的基因,并报道了2个在2p24和8p23-p21的GEFS +的新易感基因座,表明该疾病的遗传异质性。本报告的目的是通过进行10cM密度的全基因组扫描来确定受影响的突尼斯大家庭中的负责基因座。在没有重组的情况下,D5S407的最高多点对数对数(LOD)分数(1.04)被发现。在标记D19S210(LOD = 0.799)和D7S484(LOD = 0.61)标记附近发现了另外两个有趣的区域。为了精确定位这些基因座,分析了5q13.3和7p14.2上2个区域中的其他标记,并获得了两个基因座的阳性LOD分数。钠通道亚基β-1基因(SCN1B)(19q13.1)的测序显示没有任何因果突变。我们的发现强调了高热惊厥的遗传异质性。

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