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首页> 外文期刊>Epilepsia: Journal of the International League against Epilepsy >No evidence of a major locus for benign familial infantile convulsions on chromosome 19q12-q13.1.
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No evidence of a major locus for benign familial infantile convulsions on chromosome 19q12-q13.1.

机译:没有证据表明染色体19q12-q13.1上有良性家族性婴儿惊厥的主要病因。

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摘要

PURPOSE: A locus for benign familial convulsions (BFICs) has been recently mapped on chromosome 19q12-13.1 by studying five families of Italian descent. The main goal of this study was to investigate the role of this locus in a set of seven newly identified families with at least three affected cases. METHODS: Five polymorphic microsatellite markers covering the BFIC locus on chromosome 19q have been typed, and parametric linkage analysis has been performed to analyze the segregation of the BFIC locus within our families. RESULTS: Cumulative 2-point lod scores and multipoint analysis showed no evidence of linkage between chromosome 19 markers and the BFIC phenotype. The analysis of family-specific 2-point lod scores and haplotypes, however, indicated the presence of linkage to chromosome 19q in a single family, suggesting genetic heterogeneity within our family sample. CONCLUSIONS: Our study demonstrates that the previously reported BFIC locus on chromosome 19q12-13.1 is not a major locus for BFICs. We suggest that genetic heterogeneity may have generated our discordant linkage findings, as it was reported in benign familial neonatal convulsions, a related idiopathic mendelian syndrome.
机译:目的:通过研究五个意大利血统家族,最近在染色体19q12-13.1上绘制了一个良性家族性惊厥(BFICs)的位点。这项研究的主要目的是调查这个基因座在一组七个新发现的家庭中的作用,其中至少三个受影响的病例。方法:已经确定了覆盖19q染色体BFIC基因座的5个多态微卫星标记,并进行了参数连锁分析以分析我们家庭中BFIC基因座的分离。结果:累积的2点lod得分和多点分析显示19号染色体标记与BFIC表型之间没有联系的证据。但是,对家庭特定的2点lod得分和单倍型的分析表明,单个家庭中存在与19q染色体的连锁,这表明我们家庭样本中的遗传异质性。结论:我们的研究表明,先前报道的19q12-13.1染色体上的BFIC基因座不是BFICs的主要基因座。我们建议遗传异质性可能已经产生了我们不一致的连锁发现,正如在良性家族性新生儿惊厥(一种相关的特发性孟德尔综合征)中报道的那样。

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