4.6 Article

Progressive striatonigral degeneration in a transgenic mouse model of multiple system atrophy: translational implications for interventional therapies

期刊

出版社

BMC
DOI: 10.1186/s40478-017-0504-y

关键词

Multiple system atrophy; Striatonigral degeneration; alpha-synuclein; transgenic mouse; Neuroinflammation

资金

  1. Austrian Science Fund (FWF) [W01206-08, F4404, F4414, P25161]
  2. European Community's Seventh Framework Programme (FP7) [603, 646]
  3. Swedish Parkinson Foundation
  4. Network of European Neuroscience School
  5. Austrian Science Fund (FWF) [W1206] Funding Source: Austrian Science Fund (FWF)

向作者/读者索取更多资源

Multiple system atrophy (MSA) is a rapidly progressive neurodegenerative disorder characterized by widespread oligodendroglial cytoplasmic inclusions of filamentous alpha-synuclein, and neuronal loss in autonomic centres, basal ganglia and cerebellar circuits. It has been suggested that primary oligodendroglial alpha-synucleinopathy may represent a trigger in the pathogenesis of MSA, but the mechanisms underlying selective vulnerability and disease progression are unclear. The post-mortem analysis of MSA brains provides a static final picture of the disease neuropathology, but gives no clear indication on the sequence of pathogenic events in MSA. Therefore, alternative methods are needed to address these issues. We investigated selective vulnerability and disease progression in the transgenic PLP-a-syn mouse model of MSA characterized by targeted oligodendroglial alpha-synuclein overexpression aiming to provide a neuropathological correlate of motor deterioration. We show progressive motor deficits that emerge at 6 months of age and deteriorate up to 18 months of follow-up. The motor phenotype was associated with dopaminergic cell loss in the substantia nigra pars compacta at 6 months, followed by loss of striatal dopaminergic terminals and DARPP32 positive medium sized projection neurons at 12 months. Olivopontocerebellar motor loops remained spared in the PLP-a-syn model of MSA. These findings replicate progressive striatonigral degeneration underlying Parkinson-variant MSA. The initiation of the degenerative process was linked to an increase of soluble oligomeric alpha-synuclein species between 2 and 6 months. Early region-specific alpha-synuclein-associated activation profile of microglia was found in MSA substantia nigra. The role of abnormal neuroinflammatory signalling in disease progression was further supported by increased levels of CD68, CCL3, CCL5 and M-CSF with a peak in aged PLP-a-syn mice. In summary, transgenic PLP-a-syn mice show a distinctive oligodendroglial alpha-synucleinopathy that is associated with progressive striatonigral degeneration linked to abnormal neuroinflammatory response. The model provides a relevant tool for preclinical therapeutic target discovery for human Parkinson-variant MSA.

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