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Wheel running from a juvenile age delays onset of specific motor deficits but does not alter protein aggregate density in a mouse model of Huntingtons disease

机译：从幼年时代开始的车轮行驶会延迟特定运动缺陷的发作但不会改变亨廷顿氏病小鼠模型中的蛋白质聚集密度

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BackgroundHuntington's disease (HD) is a neurodegenerative disorder predominantly affecting the cerebral cortex and striatum. Transgenic mice (R6/1 line), expressing a CAG repeat encoding an expanded polyglutamine tract in the N-terminus of the huntingtin protein, closely model HD. We have previously shown that environmental enrichment of these HD mice delays the onset of motor deficits. Furthermore, wheel running initiated in adulthood ameliorates the rear-paw clasping motor sign, but not an accelerating rotarod deficit.

机译：背景亨廷顿舞蹈病（HD）是一种神经退行性疾病，主要影响大脑皮层和纹状体。转基因小鼠（R6 / 1系）在亨廷顿蛋白的N末端表达编码扩展的聚谷氨酰胺束的CAG重复序列，与HD密切相关。先前我们已经证明，这些HD小鼠的环境富集会延迟运动功能障碍的发作。此外，成年后开始的车轮行驶可以改善后爪扣紧的运动迹象，但不会加速旋转式脚架不足。

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期刊名称 BMC Neuroscience
作者
Anton van Dellen; Patricia M Cordery; Tara L Spires; Colin Blakemore; Anthony J Hannan;
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作者单位

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年(卷),期 2008(9),-1
年度 2008
页码 34
总页数 12
原文格式 PDF
正文语种
中图分类神经科学;
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专利

1. Wheel running from a juvenile age delays onset of specific motor deficits but does not alter protein aggregate density in a mouse model of Huntington's disease [J] . Anton van Dellen, Patricia M Cordery, Tara L Spires, BMC Neuroscience . 2008,第1期

机译：少年时代的车轮行驶会延迟特定运动功能障碍的发作，但不会改变亨廷顿舞蹈病小鼠模型中的蛋白质聚集密度
2. Early motor deficits in mouse disease models are reliably uncovered using an automated home-cage wheel-running system: a cross-laboratory validation [J] . Alessandro Giuliani, Glauco P. Tocchini-Valentini, Ines Heise, Disease models & mechanisms: DMM . 2014,第3期

机译：使用自动家用笼轮运行系统可可靠地发现小鼠疾病模型中的早期运动缺陷：跨实验室验证
3. Early onset deficits on the delayed alternation task in the Hdh Q92 knock-in mouse model of Huntington's disease [J] . TruemanR.C., JonesL., DunnettS.B., Brain research bulletin . 2012,第2a3期

机译：亨廷顿舞蹈病Hdh Q92敲入小鼠模型中延迟交替任务的早期发作缺陷
4. Isolated Synaptosomes from Cortex and Striatum of Huntington Disease Mice Show Selective Loss of Synaptosome-Specific Proteins but No Bioenergetics Deficit [C] . Birgit Schilling, R. Ng, J. Holcomb, ASMS Conference on Mass Spectrometry and Allied Topics . 2014

机译：来自皮质的孤立的突触体和亨廷顿疾病小鼠的纹状体表现出突触肌肉组特异性蛋白的选择性丧失，但没有生物共生学赤字
5. A neuroanatomical analysis of striosome-matrix compartmentalization and motor deficits in YAC mouse models of Huntington's disease. [D] . Lawhorn, Collene. 2009

机译：在亨廷顿舞蹈病的YAC小鼠模型中，纹状体-基质分隔和运动缺陷的神经解剖学分析。
6. Inhibition of DREAM-ATF6 interaction delays onset of cognition deficit in a mouse model of Huntington’s disease [O] . Alejandro López-Hurtado, Daniel F. Burgos, Paz González, 2018

机译：在亨廷顿舞蹈症小鼠模型中抑制DREAM-ATF6相互作用可延迟认知功能障碍的发作
7. Wheel running from a juvenile age delays onset of specific motor deficits but does not alter protein aggregate density in a mouse model of Huntington's disease [O] . van Dellen Anton, Cordery Patricia M., Spires Tara L., 2011

机译：从幼年时代开始的车轮行驶会延迟特定运动缺陷的发作，但不会改变亨廷顿氏病小鼠模型中的蛋白质聚集密度

Wheel running from a juvenile age delays onset of specific motor deficits but does not alter protein aggregate density in a mouse model of Huntingtons disease

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