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A Second Locus for Very-Late-Onset Alzheimer Disease: A Genome Scan Reveals Linkage to 20p and Epistasis between 20p and the Amyloid Precursor Protein Region

机译:阿尔茨海默病极晚发作的第二个位点:基因组扫描揭示了与20p的联系以及20p与淀粉样前体蛋白区域之间的上位性

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摘要

We used a covariate-based linkage method to reanalyze genome scan data from affected sibships collected by the Alzheimer Disease (AD) Genetics Initiative of the National Institute of Mental Health. As reported in an earlier article, the amyloid-β precursor protein (APP) region is strongly linked to affected sib pairs of the oldest current age (i.e., age either at last exam or at death) who lack E4 alleles at the apolipoprotein E (ApoE) locus. We now report that a region on 20p shows the same pattern. A model that includes current age and the number of E2 alleles as covariates gives a LOD score of 4.1. The signal on 20p is near the location of the gene coding for cystatin-C, previously shown to be associated with late-onset AD and to codeposit with APP in the brains of patients with AD. Two-locus analysis provides evidence of strong epistasis between 20p and the APP region, limited to the oldest age group and to those lacking ApoE4 alleles. We speculate that high-risk polymorphisms in both regions produce a biological interaction between these two proteins that increases susceptibility to a very-late-onset form of AD.
机译:我们使用了基于协变量的链接方法来重新分析来自由美国国家心理健康研究所的阿尔茨海默氏病(AD)遗传倡议收集的患病同胞的基因组扫描数据。如较早的文章所报道,淀粉样蛋白-β前体蛋白(APP)区域与当前年龄最大(即上次检查或死亡时的年龄)受影响的同胞对紧密相关,这些同胞对在载脂蛋白E上缺乏E4等位基因( ApoE)基因座。现在我们报告20p上的区域显示了相同的模式。包含当前年龄和E2等位基因数量作为协变量的模型的LOD得分为4.1。 20p处的信号位于编码半胱氨酸蛋白酶抑制剂C的基因的位置附近,先前已证明该基因与迟发性AD相关并与APP共存于AD患者的大脑中。两基因座分析提供了在20p和APP区域之间强烈上皮性的证据,仅限于年龄最大的人群和缺乏ApoE4等位基因的人群。我们推测这两个区域中的高风险多态性会在这两种蛋白质之间产生生物学相互作用,从而增加对非常迟发性AD的易感性。

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