摘要
背景:阿尔茨海默氏病的发病率在世界范围内呈上升趋势。但是,在病因和发病机制研究上仍没有重大突破。 目的:筛选阿尔茨海默氏病的致病基因,可能有助于阐明阿尔茨海默氏病的致病机理,并通过各种计算机软件预测其致病性。 方法:先证者进行临床和神经影像学检查,全外显子组测序和桑格测序。在158位受试者中验证了突变位点。 结果:我们报道了一个先证者携带可能是新的致病突变,在临床上表现为进行性记忆丧失,视觉空间障碍,失用症,心理行为障碍以及气质和性格改变。全外显子组测序检测到一个新的222位密码子错义突变(Q222L),这是早老素1外显子5中665位(c.665A> T)的杂合A到T点突变,导致谷氨酰胺-亮氨酸取代。还通过一个家庭成员的Sanger测序鉴定了该突变。但是,在其他7个未受影响的家庭成员,50例散发的阿尔茨海默氏病患者和100例对照受试者中未检测到。 结论:早发性阿尔茨海默氏病中国家庭中早老素1基因外显子5(Gln222Leu)发生了新的突变,据报道,该错义突变可能是一种新的致病突变。第一次在中国家庭中患早发性阿尔茨海默氏病。
关键词: 早发性阿尔茨海默病,家族性,突变,PSEN 1 Gln222Leu突变,痴呆,记忆丧失。
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