首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >High-resolution imaging reveals indirect coordination of opposite motors and a role for LIS1 in high-load axonal transport
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High-resolution imaging reveals indirect coordination of opposite motors and a role for LIS1 in high-load axonal transport

机译:高分辨率成像揭示了相对马达的间接协调以及LIS1在高负荷轴突运输中的作用

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摘要

The specific physiological roles of dynein regulatory factors remain poorly understood as a result of their functional complexity and the interdependence of dynein and kinesin motor activities. We used a novel approach to overcome these challenges, combining acute in vivo inhibition with automated high temporal and spatial resolution particle tracking. Acute dynein inhibition in nonneuronal cells caused an immediate dispersal of diverse forms of cargo, resulting from a sharp decrease in microtubule minus-end run length followed by a gradual decrease in plus-end runs. Acute LIS1 inhibition or LIS1 RNA interference had little effect on lysosomes/late endosomes but severely inhibited axonal transport of large, but not small, vesicular structures. Our acute inhibition results argue against direct mechanical activation of opposite-directed motors and offer a novel approach of potential broad utility in the study of motor protein function in vivo. Our data also reveal a specific but cell type–restricted role for LIS1 in large vesicular transport and provide the first quantitative support for a general role for LIS1 in high-load dynein functions.
机译:由于其功能复杂性以及动力蛋白和驱动蛋白运动活动的相互依赖性,动力蛋白调节因子的具体生理作用仍然知之甚少。我们采用了一种新颖的方法来克服这些挑战,将急性体内抑制与自动化的高时空分辨率结合起来。非神经元细胞中的急性动力蛋白抑制作用导致多种形式的货物立即分散,这是由于微管负端行程长度急剧减少,随后正端行程逐渐减少所致。急性LIS1抑制或LIS1 RNA干扰对溶酶体/晚期内体的影响很小,但严重抑制了大但不小的水泡结构的轴突转运。我们的急性抑制结果反对反向运动的直接机械激活,并提供了一种在体内运动蛋白功能研究中潜在的广泛用途的新方法。我们的数据还揭示了LIS1在大水泡运输中的一种特定但受细胞类型限制的作用,并为LIS1在高负荷动力蛋白功能中的一般作用提供了第一个定量支持。

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