期刊
CURRENT ALZHEIMER RESEARCH
卷 12, 期 8, 页码 772-784出版社
BENTHAM SCIENCE PUBL LTD
DOI: 10.2174/1567205012666150710112147
关键词
Adult neurogenesis; hippocampus; intracerebroventricular; microglia; oligodendrocytes; sporadic Alzheimer's disease; streptozotocin
资金
- Croatian Ministry of Science, Sport and education (MZOS) [108-1080003-0020]
- Deutscher Akademischer Austauschdienst (DAAD) [A/00/200017]
- Dr. Edda Neele foundation
- Chinese Research council
Altered adult hippocampal neurogenesis (AN) plays a role in the etiopathology of Alzheimer's disease (AD), a disorder characterized by a progressive loss of memory and spatial orientation impairment. Diabetes is shown to be one risk factor for the development of the sporadic form of AD (sAD), which affects >95% of AD patients. Streptozotocin intracerebroventricularily (STZ icv) treated rats, which develop an insulin-resistant brain state and learning and memory deficits preceding amyloid beta and tau pathology, may act as an appropriate animal model for sAD. The goal of our quantitative immunohistochemistry study was to compare short-term (1 month) and long-term (3 months) effects of STZ icv treatment on different AN stages. Applying MCM2 antibodies we quantified cell (e.g. stem cell) proliferation, by the use of NeuroD and DCX antibodies we analyzed immature neurons. BrdU incorporation with approximately 27 days of survival before sacrifice allowed us to quantify and identify surviving newborn cells. Performing co-localization studies with antibodies detecting BrdU and cell-type specific markers we could confirm that STZ treatment does not affect the differentiation fate of newly generated cells. Whereas STZ icv treatment does not seem to considerably influence cell proliferation over a short-term period (1 month), in the long-term (3 months) it significantly decreased generation of immature and mature neurons. This reduction seen after 3 months was specific for the septal hippocampus, discussed to be important for spatial learning. Moreover, AN changes display the same timeline as the development of amyloid beta pathology in this animal model of sAD.
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