首页> 外文期刊>BMC Genomics >Similar striatal gene expression profiles in the striatum of the YAC128 and HdhQ150 mouse models of Huntington’s disease are not reflected in mutant Huntingtin inclusion prevalence
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Similar striatal gene expression profiles in the striatum of the YAC128 and HdhQ150 mouse models of Huntington’s disease are not reflected in mutant Huntingtin inclusion prevalence

机译:亨廷顿病的YAC128和HdhQ150小鼠模型的纹状体中相似的纹状体基因表达谱未反映在突变的亨廷顿蛋白包涵体患病率中

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The YAC128 model of Huntington’s disease (HD) shows substantial deficits in motor, learning and memory tasks and alterations in its transcriptional profile. We examined the changes in the transcriptional profile in the YAC128 mouse model of HD at 6, 12 and 18?months and compared these with those seen in other models and human HD caudate. Differential gene expression by genotype showed that genes related to neuronal function, projection outgrowth and cell adhesion were altered in expression. A Time-course ANOVA revealed that genes downregulated with increased age in wild-type striata were likely to be downregulated in the YAC128 striata. There was a substantial overlap of concordant gene expression changes in the YAC128 striata compared with those in human HD brain. Changes in gene expression over time showed fewer striatal YAC128 RNAs altered in abundance than in the HdhQ150 striata but there was a very marked overlap in transcriptional changes at all time points. Despite the similarities in striatal expression changes at 18?months the HdhQ150 mice showed widespread mHTT and ubiquitin positive inclusion staining in the striatum whereas this was absent in the YAC128 striatum. The gene expression changes in YAC128 striata show a very closely matched profile to that of HdhQ150 striata and are already significantly different between genotypes by six months of age, implying that the temporal molecular gene expression profiles of these models match very closely, despite differences in the prevalence of brain inclusion formation between the models. The YAC128 gene expression changes appear to correlate well with gene expression differences caused by ageing. A relatively small number of genes showed significant differences in expression between the striata of the two models and these could explain some of the phenotypic differences between the models.
机译:亨廷顿舞蹈病(HD)的YAC128模型显示出运动,学习和记忆任务的大量缺陷以及其转录谱的改变。我们检查了HD的YAC128小鼠模型在6、12、18个月时转录谱的变化,并将其与其他模型和人类HD尾状中观察到的变化进行了比较。不同基因型的基因表达差异表明与神经元功能,突起生长和细胞粘附相关的基因表达发生了改变。时程方差分析显示,野生型纹状体中随着年龄增长而下调的基因很可能在YAC128纹状体中下调。与人类HD脑中的一致,YAC128纹状体中一致的基因表达变化存在大量重叠。基因表达随时间的变化显示,与HdhQ150纹状体相比,纹状体YAC128 RNA的丰度变化较少,但在所有时间点的转录变化都存在非常明显的重叠。尽管在18个月时纹状体表达变化相似,但HdhQ150小鼠在纹状体中显示出广泛的mHTT和泛素阳性包涵体染色,而在YAC128纹状体中则没有。 YAC128纹状体的基因表达变化与HdhQ150纹状体的匹配非常接近,并且在六个月大的基因型之间基因型之间已经存在显着差异,这意味着尽管这些模型之间存在差异,但这些模型的时间分子基因表达谱非常匹配。模型之间脑包涵形成的普遍性。 YAC128基因表达的变化似乎与衰老引起的基因表达差异密切相关。相对较少的基因显示出两个模型的纹状体之间表达上的显着差异,这些基因可以解释模型之间的某些表型差异。

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