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Computer simulation of linkage and heterogeneity in tuberous sclerosis: a critical evaluation of the collaborative family data.

机译:结节性硬化中连锁和异质性的计算机模拟:对协作家庭数据的重要评估。

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摘要

The existence of locus heterogeneity for a genetic disease may complicate linkage studies considerably, especially when very few large families with the disease are available. In this situation a modest collection of families is unlikely to be sufficient for successful localisation of one or more disease genes. Recently, eight research groups working on tuberous sclerosis (TSC) brought together linkage data pertaining to the candidate chromosomes 9, 11, and 12 for a large group of families. In a series of simulation studies we determined the probability of detecting linkage and linkage heterogeneity in this set of families. On average TSC families are very small; in most cases there are fewer than two informative meioses. The size distribution of chromosome 9 linked families was similar to that of non-linked families. This indicates that a dramatic difference in the clinical severity of major genetic forms of TSC is unlikely. The results of our simulation studies show that this set of families can generate highly significant evidence for linkage and heterogeneity. When two TSC genes are equally common, the strongest evidence for linkage and heterogeneity could be obtained using a method based on the incorporation of multiple candidate regions in a single analysis, with an average lod score of 24.27.
机译:遗传疾病的基因座异质性的存在可能使连锁研究大大复杂化,尤其是在很少有这种疾病的大家庭中。在这种情况下,少量的家庭收集不足以成功定位一个或多个疾病基因。最近,从事结节性硬化症(TSC)的八个研究小组将与一大群家庭的候选染色体9、11和12有关的连锁数据汇总在一起。在一系列模拟研究中,我们确定了在这套家族中检测连锁和连锁异质性的可能性。平均而言,TSC家庭很小。在大多数情况下,信息通报会少于两个。 9号染色体连锁家庭的大小分布与非连锁家庭相似。这表明,TSC主要遗传形式的临床严重性差异不大。我们的模拟研究结果表明,这组家庭可以为联系和异质性提供非常重要的证据。当两个TSC基因同等普遍时,可以使用基于在单个分析中并入多个候选区域的方法获得连锁和异质性的最有力证据,平均lod得分为24.27。

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