- 作者:Olivier C. Maes ; Suying Xu ; Bo Yu ; Howard M. Chertkow ; Eugenia Wang ; Hyman M. Schipper
- 关键词:Aging ; Alzheimer ; Amyloid-beta ; Blood mononuclear cell ; Cytoskeleton ; DNA repair ; Microarray ; Microtubule-associated protein tau ; Neurodegeneration ; Oxidative stress
- 刊名:Neurobiology of Aging
- 出版年:2007
- 出版时间:December 2007
- 年:2007
- 卷:28
- 期:12
- 页码:1795-1809
- 全文大小:1162 K
Relative to the NEC samples, the Alzheimer BMC exhibited a significant decline in the expression of genes concerned with cytoskeletal maintenance, cellular trafficking, cellular stress response, redox homeostasis, transcription and DNA repair. We observed decreased expression of several genes which may impact amyloid-beta production and the processing of the microtubule-associated protein tau. The microarray results were validated by quantitative real time PCR and revealed gender differences in the levels of altered gene expression.
Our findings attest to the systemic nature of gene dys-regulation in sporadic AD, implicate disruption of cytoskeletal integrity, DNA repair mechanisms and cellular defenses in this condition, and suggest novel pathways of β-amyloid deposition in this disease. BMC are highly accessible and may reflect molecular events germane to the neuropathophysiology of AD.