Lewy body pathology is associated with mitochondrial DNA damage in Parkinson's disease
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- 作者:Sarina K. Mü ; llera ; 1 ; Andreas Bendera ; b ; 1 ; andreas.bender@med.uni-muenchen.de ; Christoph Lauba ; Tobias Hö ; gena ; Falk Schlaudraffc ; Birgit Lissc ; Thomas Klopstocka ; d ; e ; f ; Matthias Elstnera ; d
- 关键词:Mitochondrial DNA ; mtDNA deletions ; Parkinson's disease ; Alzheimer's disease ; Aging ; Mitochondrial dysfunction ; Laser capture microdissection ; LMD
- 刊名:Neurobiology of Aging
- 出版年:2013
- 出版时间:September, 2013
- 年:2013
- 卷:34
- 期:9
- 页码:2231-2233
- 全文大小:189 K
文摘
Mitochondrial dysfunction has been strongly implicated in the pathogenesis of Parkinson's disease (PD) and Alzheimer's disease (AD), but its relation to protein aggregation is unclear. PD is characterized by synuclein aggregation (i.e., Lewy body [LB] formation). In AD, the abnormal accumulation of tau protein forms neurofibrillary tangles. In this study, we laser-dissected LB-positive and -negative neurons from the substantia nigra of postmortem PD brains, and tau-positive and -negative hippocampal neurons from AD brains. We quantified mitochondrial DNA deletions in relation to the cellular phenotype and in comparison with age-matched controls. Deletion levels were highest in LB-positive neurons of PD brains (40.5 ¡À 16.8 % ), followed by LB-negative neurons of PD cases (31.8 ¡À 14.4 % ) and control subjects (25.6 ¡À 17.5 % ; analysis of variance p < 0.005). In hippocampal neurons, deletion levels were 25 % -30 % , independent of disease status and neurofibrillary tangles. The presented findings imply increased mitochondrial DNA damage in LB-positive midbrain neurons, but do not support a direct causative link of respiratory chain dysfunction and protein aggregation.