AnatomyOrganismsDiseasesChemicals and Drugs
CuprizoneDemyelinating DiseasesCorpus CallosumMyelin SheathOligodendrogliaMonoamine Oxidase InhibitorsChelating AgentsMicrogliaGlial Fibrillary Acidic ProteinGliosisMice, Inbred C57BLAstrocytes

Age-dependent epigenetic control of differentiation inhibitors is critical for remyelination efficiency. (33/102)

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Statin therapy inhibits remyelination in the central nervous system. (34/102)

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Comparative prion disease gene expression profiling using the prion disease mimetic, cuprizone. (35/102)

Identification of genes expressed in response to prion infection may elucidate biomarkers for disease, identify factors involved in agent replication, mechanisms of neuropathology and therapeutic targets. Although several groups have sought to identify gene expression changes specific to prion disease, expression profiles rife with cell population changes have consistently been identified. Cuprizone, a neurotoxicant, qualitatively mimics the cell population changes observed in prion disease, resulting in both spongiform change and astrocytosis. The use of cuprizone-treated animals as an experimental control during comparative expression profiling allows for the identification of transcripts whose expression increases during prion disease and remains unchanged during cuprizone-triggered neuropathology. In this study, expression profiles from the brains of mice preclinically and clinically infected with Rocky Mountain Laboratory (RML) mouse-adapted scrapie agent and age-matched controls were profiled using Affymetrix gene arrays. In total, 164 genes were differentially regulated during prion infection. Eighty-three of these transcripts have been previously undescribed as differentially regulated during prion disease. A 0.4% cuprizone diet was utilized as a control for comparative expression profiling. Cuprizone treatment induced spongiosis and astrocyte proliferation as indicated by glial fibrillary acidic protein (Gfap) transcriptional activation and immunohistochemistry. Gene expression profiles from brain tissue obtained from cuprizone-treated mice identified 307 differentially regulated transcript changes. After comparative analysis, 17 transcripts unaffected by cuprizone treatment but increasing in expression from preclinical to clinical prion infection were identified. Here we describe the novel use of the prion disease mimetic, cuprizone, to control for cell population changes in the brain during prion infection.  (+info)

Downregulation of oligodendrocyte transcripts is associated with impaired prefrontal cortex function in rats. (36/102)

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HDAC1 nuclear export induced by pathological conditions is essential for the onset of axonal damage. (37/102)

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CXCR2-positive neutrophils are essential for cuprizone-induced demyelination: relevance to multiple sclerosis. (38/102)

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Inhibiting poly(ADP-ribose) polymerase: a potential therapy against oligodendrocyte death. (39/102)

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17beta-estradiol protects male mice from cuprizone-induced demyelination and oligodendrocyte loss. (40/102)

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