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首页> 外文期刊>Brain research bulletin >The detection and measurement of locomotor deficits in a transgenic mouse model of Huntington's disease are task- and protocol-dependent: influence of non-motor factors on locomotor function.
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The detection and measurement of locomotor deficits in a transgenic mouse model of Huntington's disease are task- and protocol-dependent: influence of non-motor factors on locomotor function.

机译:在亨廷顿舞蹈病的转基因小鼠模型中,运动缺陷的检测和测量取决于任务和方案:非运动因素对运动功能的影响。

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Locomotor performance of transgenic R6/2 mice carrying the Huntington's disease (HD) mutation was assessed using four different tasks, fixed speed rotarod, accelerating rotarod, Digigait and footprint test. The tasks were compared directly in age- and CAG repeat-matched R6/2 mice. Accelerating rotarod was more sensitive than fixed speed rotarod for detecting early motor deficits in R6/2 mice. The sensitivity of accelerating rotarod increased with the acceleration rate and/or the start speed from which the rod accelerated. Differences between tasks were not due to inability of R6/2 mice to maintain balance at high speeds or increased fatigue on accelerating rotarod, but to difficulties in coordinating gait changes required by the constant change in speed on accelerating rotarod. The footprint test was sensitive to gait disturbances. However, surprisingly, R6/2 mice did not show major gait abnormalities on an automated treadmill task (Digigait), even though they showed overt gait deficits in the home cage. The fact that the sensitivity for detecting motor deficits depended strongly on the individual task, and on the protocol used, suggests that non-motor factors were differentially engaged in the different paradigms. We thus recommend that more than one task should be used for detecting and tracking different aspects of motor decay in animal models of HD. Since deficits in non-motor factors such as executive function and motivation may differentially influence motor outcome in each task, our results call for a more thorough investigation of the importance of higher level control of locomotion in animal models of HD.
机译:使用四个不同的任务评估了携带亨廷顿氏病(HD)突变的转基因R6 / 2小鼠的运动能力,这些任务包括定速旋转脚架,加速旋转脚架,Digigait和足迹测试。在年龄和CAG重复匹配的R6 / 2小鼠中直接比较任务。对于检测R6 / 2小鼠的早期运动缺陷,加速旋转脚架比固定速度旋转脚架更敏感。旋转旋转脚架的灵敏度随杆的加速速度和/或起始速度而增加。任务之间的差异并不是由于R6 / 2小鼠无法在高速下保持平衡或在加速旋转脚踏车上增加疲劳感,而是由于难以协调步态变化,而步伐变化是加速旋转脚踏车所需的恒定速度。足迹测试对步态干扰敏感。但是,令人惊讶的是,R6 / 2小鼠在自动跑步机上没有表现出严重的步态异常(Digigait),即使它们在笼中显示出明显的步态缺陷。检测运动缺陷的敏感性很大程度上取决于个人任务和所使用的协议,这一事实表明,非运动因素在不同范式中的作用不同。因此,我们建议在高清动物模型中应使用多个任务来检测和跟踪运动衰减的不同方面。由于非运动因素(例如执行功能和动机)的不足可能会不同地影响每个任务中的运动结果,因此我们的结果要求对HD动物模型中较高水平的运动控制的重要性进行更彻底的研究。

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