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微管动力学对于SRC家族激酶依赖性生长锥转向是必需的。

Microtubule dynamics are necessary for SRC family kinase-dependent growth cone steering.

作者信息

Suter Daniel M, Schaefer Andrew W, Forscher Paul

机构信息

Department of Molecular, Cellular, and Developmental Biology, Yale University, P.O. Box 208103, New Haven, CT 06520, USA.

出版信息

Curr Biol. 2004 Jul 13;14(13):1194-9. doi: 10.1016/j.cub.2004.06.049.

Abstract

Dynamic microtubules explore the peripheral (P) growth cone domain using F actin bundles as polymerization guides. Microtubule dynamics are necessary for growth cone guidance; however, mechanisms of microtubule reorganization during growth cone turning are not well understood. Here, we address these issues by analyzing growth cone steering events in vitro, evoked by beads derivatized with the Ig superfamily cell adhesion protein apCAM. Pharmacological inhibition of microtubule assembly with low doses of taxol or vinblastine resulted in rapid clearance of microtubules from the P domain with little effect on central (C) axonal microtubules or actin-based motility. Early during target interactions, we detected F actin assembly and activated Src, but few microtubules, at apCAM bead binding sites. The majority of microtubules extended toward bead targets after F actin flow attenuation occurred. Microtubule extension during growth cone steering responses was strongly suppressed by dampening microtubule dynamics with low doses of taxol or vinblastine. These treatments also inhibited growth cone turning responses, as well as focal actin assembly and accumulation of active Src at bead binding sites. These results suggest that dynamic microtubules carry signals involved in regulating Src-dependent apCAM adhesion complexes involved in growth cone steering.

摘要

动态微管利用肌动蛋白丝束作为聚合导向,探索外周(P)生长锥区域。微管动力学对于生长锥导向是必需的;然而,生长锥转向过程中微管重组的机制尚未完全了解。在这里,我们通过分析体外生长锥转向事件来解决这些问题,这些事件由用免疫球蛋白超家族细胞粘附蛋白apCAM衍生化的珠子诱发。用低剂量紫杉醇或长春碱对微管组装进行药理学抑制,导致微管从P区域快速清除,对中央(C)轴突微管或基于肌动蛋白的运动性影响很小。在与靶点相互作用的早期,我们在apCAM珠子结合位点检测到肌动蛋白丝组装和活化的Src,但微管很少。在肌动蛋白丝流动减弱后,大多数微管向珠子靶点延伸。在生长锥转向反应过程中,微管延伸受到低剂量紫杉醇或长春碱抑制微管动力学的强烈抑制。这些处理还抑制了生长锥转向反应,以及在珠子结合位点的局部肌动蛋白组装和活性Src的积累。这些结果表明,动态微管携带参与调节与生长锥转向有关的Src依赖性apCAM粘附复合物的信号。

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