Association Between Alzheimer’s Disease and the NOS3 gene Glu298Asp Polymorphism in Chinese
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  • 作者:Binbin Wang (1) (4)
    Sainan Tan (1) (4)
    Ze Yang (2)
    Yan-Chen Xie (3)
    Jing Wang (1) (4)
    Sirui Zhou (1) (4)
    Shu Li (2)
    Chenguang Zheng (5)
    Xu Ma (1) (4) (6)
  • 关键词:Late ; onset Alzheimer’s disease ; Endothelial nitric oxide synthase ; NOS3 ; Apolipoprotein E ; Polymorphism ; Chinese
  • 刊名:Journal of Molecular Neuroscience
  • 出版年:2008
  • 出版时间:February 2008
  • 年:2008
  • 卷:34
  • 期:2
  • 页码:173-176
  • 全文大小:93KB
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    11. Monastero, R., Cefalù, A. B., Camarda, C., Buglino, C. M., Mannino, M., Barbagallo, C. M., et al. (2003). No association between Glu298Asp endothelial nitric oxide synthase polymorphism and Italian sporadic Alzheimer’s disease. / Neurosci Letters, / 341, 229-32. CrossRef
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  • 作者单位:Binbin Wang (1) (4)
    Sainan Tan (1) (4)
    Ze Yang (2)
    Yan-Chen Xie (3)
    Jing Wang (1) (4)
    Sirui Zhou (1) (4)
    Shu Li (2)
    Chenguang Zheng (5)
    Xu Ma (1) (4) (6)

    1. Center for Genetics, National Research Institute for Family Planning, 12, Dahuisi Road, Haidian, Beijing, 100081, China
    4. Peking Union Medical College, Beijing, China
    2. Laboratory for Medical Genetics, Institute of Geriatrics, Beijing Hospital, Ministry of Health, Beijing, 100730, China
    3. Department of Neurology, Beijing Friendship Hospital, Affiliate of Capital University of Medical Sciences, Beijing, 100050, China
    5. Jiangbin Hospital, Nanning, Guangxi, 530021, China
    6. World Health Organization Collaborating Centre for Research in Human Reproduction, Beijing, China
文摘
The oxidative stress caused by nitric oxide (NO) in the brain has been proposed as a pathogenic mechanism in Alzheimer’s disease. Endothelial NO synthase (ecNOS) produces the majority of circulating NO. The biological functional and genetic association studies suggested that the Glu298Asp polymorphism of the ecNOS gene (NOS3) may be a genetic risk factor for late-onset Alzheimer’s disease (LOAD). To investigate an association between the NOS31 Glu298Asp polymorphism and sporadic LOAD in Chinese, we examined 338 LOAD patients and 378 healthy controls. The associations of the Glu/Glu genotype and Glu allele with LOAD (χ 2--.12, df--, P--.003 by genotype; χ 2--.37, df--, P--.038 by allele) were found. After stratifying by apolipoprotein E allele 4 (APOE ?4) status, increased LOAD risks associated with the Glu/Glu genotype and Glu allele only in the APOE ?4 noncarriers (χ 2--.28, df--, P--.012 by genotype; χ 2--.62, df--, P--.018 by allele) were seen. These results suggest that the NOS3 gene Glu298Asp polymorphism might be a risk factor for LOAD and dependent on APOE ?4 status in Chinese.

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