首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Preferential binding of a kinesin-1 motor to GTP-tubulin–rich microtubules underlies polarized vesicle transport
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Preferential binding of a kinesin-1 motor to GTP-tubulin–rich microtubules underlies polarized vesicle transport

机译:kinesin-1马达与富含GTP-微管蛋白的微管的优先结合是极化囊泡运输的基础。

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摘要

Polarized transport in neurons is fundamental for the formation of neuronal circuitry. A motor domain–containing truncated KIF5 (a kinesin-1) recognizes axonal microtubules, which are enriched in EB1 binding sites, and selectively accumulates at the tips of axons. However, it remains unknown what cue KIF5 recognizes to result in this selective accumulation. We found that axonal microtubules were preferentially stained by the anti–GTP-tubulin antibody hMB11. Super-resolution microscopy combined with EM immunocytochemistry revealed that hMB11 was localized at KIF5 attachment sites. In addition, EB1, which binds preferentially to guanylyl-methylene-diphosphate (GMPCPP) microtubules in vitro, recognized hMB11 binding sites on axonal microtubules. Further, expression of hMB11 antibody in neurons disrupted the selective accumulation of truncated KIF5 in the axon tips. In vitro studies revealed approximately threefold stronger binding of KIF5 motor head to GMPCPP microtubules than to GDP microtubules. Collectively, these data suggest that the abundance of GTP-tubulin in axonal microtubules may underlie selective KIF5 localization and polarized axonal vesicular transport.
机译:神经元中的极化转运对于神经元回路的形成至关重要。含有运动域的截短的KIF5(驱动蛋白1)识别轴突微管,该微管富含EB1结合位点,并选择性地聚集在轴突尖端。然而,仍然不清楚KIF5识别出什么导致这种选择性积累。我们发现轴突微管优先被抗-GTP-微管蛋白抗体hMB11染色。超分辨率显微镜与EM免疫细胞化学相结合揭示hMB11位于KIF5附着位点。另外,在体外优先结合鸟苷基-亚甲基-二磷酸(GMPCPP)微管的EB1识别轴突微管上的hMB11结合位点。此外,hMB11抗体在神经元中的表达破坏了截短的KIF5在轴突尖端的选择性积累。体外研究表明,KIF5马达头部与GMPCPP微管的结合比与GDP微管的结合强大约三倍。总体而言,这些数据表明,轴突微管中GTP微管蛋白的丰富可能是选择性KIF5定位和极化的轴突囊泡运输的基础。

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