Deng Bo, Lian Yan, Wang Xin, Zeng Fan, Jiao Bin, Wang Ye-Ran, Liang Chun-Rong, Liu Yu-Hui, Bu Xian-Le, Yao Xiu-Qing, Zhu Chi, Shen Lu, Zhou Hua-Dong, Zhang Tao, Wang Yan-Jiang
Department of Neurology and Centre for Clinical Neuroscience, Daping Hospital, Third Military Medical University, Chongqing, China.
Neurotox Res. 2014 Oct;26(3):211-5. doi: 10.1007/s12640-014-9462-3. Epub 2014 Apr 16.
This study has identified a gene mutation in a Chinese family with Alzheimer's disease (AD). Family members were screened by a set of medical examinations and neuropsychological tests. Their DNA was extracted from blood cells and sequenced for gene mutation in the amyloid precursor protein (APP), the presenilin 1 (PS1) and the presenilin 2 (PS2) genes. Genetic analysis showed that the AD patients in the family harbored a T to G missense mutation at the position 314 in exon 4 of the PS1 gene, resulting in a change of F105C in amino acid sequence. Clinical manifestation of these patients included memory loss, counting difficulty, personality change, disorientation, dyscalculia, agnosia, aphasia, and apraxia, which was similar to that of the familial AD (FAD) patients harboring other PS1 mutations. We intend to add a novel mutation F105C of the PS1 gene to the pool of FAD mutations. With the current available genetic data, mutations of the PS1 gene account for the majority of gene mutations in Chinese FAD.
本研究在一个患有阿尔茨海默病(AD)的中国家庭中发现了一种基因突变。通过一系列医学检查和神经心理学测试对家庭成员进行了筛查。从血细胞中提取他们的DNA,并对淀粉样前体蛋白(APP)、早老素1(PS1)和早老素2(PS2)基因进行基因突变测序。遗传分析表明,该家族中的AD患者在PS1基因第4外显子的314位存在一个从T到G的错义突变,导致氨基酸序列中F105C的改变。这些患者的临床表现包括记忆力减退、计数困难、性格改变、定向障碍、失算症、失认症、失语症和失用症,这与携带其他PS1突变的家族性AD(FAD)患者相似。我们打算将PS1基因的一种新突变F105C添加到FAD突变库中。根据目前可用的遗传数据,PS1基因的突变在中国FAD基因突变中占大多数。
