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Glycosylation-related gene expression profiling in the brain and spleen of scrapie-affected mouse

机译:瘙痒病小鼠脑和脾中糖基化相关基因的表达谱

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A central event in the formation of infectious prions is the conformational change of a host-encoded glycoprotein, PrPC, into a pathogenic isoform, PrPSc. The molecular requirements for efficient PrP conversion remain unknown. Altered glycosylation has been linked to various pathologies and the N-glycans harbored by two prion protein isoforms are different. In order to search for glycosylation-related genes that could mark prion infection, we used a glycosylation-dedicated microarray that allowed the simultaneous analysis of the expression of 165 glycosylation-related genes encoding proteins of the glycosyltransferase, glycosidase, lectin, and sulfotransferase families to compare the gene expression profiles of normal and scrapie-infected mouse brain and spleen. Eight genes were found upregulated in “scrapie brain” at the final state of the disease. In the spleen, five genes presented a modified expression. Three genes were also upregulated in the spleen of infected mice, and two (Pigq and St3gal5) downregulated. All changes were confirmed by qPCR and biochemical analyses applied to Pigq and St3gal5 proteins.
机译:感染性ions病毒形成的中心事件是宿主编码的糖蛋白PrP C 向致病同工型PrP Sc 的构象变化。有效PrP转化的分子要求仍然未知。改变的糖基化与各种病理学有关,并且两种two病毒蛋白同工型所具有的N-聚糖是不同的。为了搜索可能标记病毒感染的糖基化相关基因,我们使用了糖基化专用芯片,可以同时分析165个糖基化相关基因的表达,这些基因编码糖基转移酶,糖苷酶,凝集素和磺基转移酶家族的蛋白,比较正常和瘙痒病感染的小鼠脑和脾的基因表达谱。发现八种基因在疾病的最终状态在“ sc脑”中被上调。在脾脏中,五个基因呈现出修饰的表达。在被感染小鼠的脾脏中,三个基因也被上调,而两个基因(Pigq和St3gal5)被下调。所有变化均通过qPCR和应用于Pigq和St3gal5蛋白的生化分析证实。

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