【2h】

Cytoplasmic dynein is associated with slow axonal transport.

机译:细胞质动力蛋白与轴突运输缓慢有关。

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摘要

Neuronal function is dependent on the transport of materials from the cell body to the synapse via anterograde axonal transport. Anterograde axonal transport consists of several components that differ in both rate and protein composition. In fast transport, membranous organelles are moved along microtubules by the motor protein kinesin. The cytoskeleton and the cytomatrix proteins move in the two components of slow transport. While the mechanisms underlying slow transport are unknown, it has been hypothesized that the movement of microtubules in slow transport is generated by sliding. To determine whether dynein, a motor protein that causes microtubule sliding in flagella, may play a role in slow axonal transport, we identified the transport rate components with which cytoplasmic dynein is associated in rat optic nerve. Nearly 80% of the anterogradely moving dynein was associated with slow transport, whereas only approximately 15% of the dynein was associated with the membranous organelles of anterograde fast axonal transport. A segmental analysis of the transport of dynein through contiguous regions of the optic nerve and tract showed that dynein is associated with the microfilaments and other proteins of slow component b. Dynein from this transport component has the capacity to bind microtubules in vitro. These results are consistent with the hypothesis that cytoplasmic dynein generates the movement of microtubules in slow axonal transport. A model is presented to illustrate how dynein attached to the slow component b complex of proteins is appropriately positioned to generate force of the correct polarity to slide microtubules down the axon.
机译:神经元功能取决于通过顺行轴突运输从物质到突触的物质运输。顺行轴突运输由速率和蛋白质组成不同的几种成分组成。在快速运输中,膜细胞器通过运动蛋白驱动蛋白沿着微管移动。细胞骨架和细胞基质蛋白在缓慢运输的两个部分中移动。尽管缓慢运输的机制尚不清楚,但据推测,缓慢运输中的微管运动是通过滑动产生的。为了确定动力蛋白(导致鞭毛中微管滑动的动力蛋白)是否可能在缓慢的轴突运输中发挥作用,我们确定了大鼠视神经中与胞质动力相关的运输速率成分。顺行运动的动力蛋白中有近80%与缓慢运输有关,而顺反运动的轴突运输中只有约15%的动力蛋白与膜细胞器有关。对动力蛋白通过视神经和呼吸道连续区域的运输进行的分段分析表明,动力蛋白与微丝和慢成分b的其他蛋白质有关。来自该转运成分的动力蛋白具有体外结合微管的能力。这些结果与细胞质动力蛋白在缓慢的轴突运输中产生微管运动的假设相一致。提出了一个模型来说明附着在蛋白质慢成分b复合体上的动力蛋白如何适当定位,以产生正确极性的力将微管滑到轴突上。

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