Genetic association of the cytochrome c oxidase-related genes with Alzheimer’s disease in Han Chinese

被引:0
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作者
Rui Bi
Wen Zhang
Deng-Feng Zhang
Min Xu
Yu Fan
Qiu-Xiang Hu
Hong-Yan Jiang
Liwen Tan
Tao Li
Yiru Fang
Chen Zhang
Yong-Gang Yao
机构
[1] Chinese Academy of Sciences,Key Laboratory of Animal Models and Human Disease Mechanisms of the Chinese Academy of Sciences and Yunnan Province, Kunming Institute of Zoology
[2] Chinese Academy of Sciences,Center for Excellence in Animal Evolution and Genetics
[3] Hainan Medical College,Department of Biochemistry and Molecular Biology and Key Laboratory of Molecular Biology, School of Basic Medicine and Life Sciences
[4] University of Chinese Academy of Sciences,Kunming College of Life Science
[5] the First Affiliated Hospital of Kunming Medical University,Department of Psychiatry
[6] Central South University,Mental Health Institute of the Second Xiangya Hospital
[7] Sichuan University,The Mental Health Center and Psychiatric Laboratory, West China Hospital
[8] Shanghai Jiao Tong University School of Medicine,Division of Mood Disorders, Shanghai Mental Health Center
[9] Chinese Academy of Sciences,Center for Excellence in Brain Science and Intelligence Technology
[10] KIZ/CUHK Joint Laboratory of Bioresources and Molecular Research in Common Diseases,undefined
来源
Neuropsychopharmacology | 2018年 / 43卷
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摘要
Alzheimer’s disease (AD) is the most common cause of dementia. Mitochondrial dysfunction has been widely reported in AD due to its important role in cellular metabolism and energy production. Complex IV (cytochrome c oxidase, COX) of mitochondrial electron transport chain, is particularly vulnerable in AD. Defects of COX in AD have been well documented, but there is little evidence to support the genetic association of the COX-related genes with AD. In this study, we investigated the genetic association between 17 nuclear-encoded COX-related genes and AD in 1572 Han Chinese. The whole exons of these genes were also screened in 107 unrelated AD patients with a high probability of hereditarily transmitted AD. Variants in COX6B1, NDUFA4, SURF1, and COX10 were identified to be associated with AD. An integrative analysis with data of eQTL, expression and pathology revealed that most of the COX-related genes were significantly downregulated in AD patients and mouse models, and the AD-associated variants in COX6B1, SURF1, and COX10 were linked to altered mRNA levels in brain tissues. Furthermore, mRNA levels of Ndufa4, Cox5a, Cox10, Cox6b2, Cox7a2, and Lrpprc were significantly correlated with Aβ plaque burden in hippocampus of AD mice. Convergent functional genomics analysis revealed strong supportive evidence for the roles of COX6B1, COX10, NDUFA4, and SURF1 in AD. As the result of our comprehensive analysis of the COX-related genes at the genetic, expression, and pathology levels, we have been able to provide a systematic view for understanding the relationships of the COX-related genes in the pathology of AD.
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页码:2264 / 2276
页数:12
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