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Microtubules cut loose at the cell cortex

机译:微管在细胞皮层切开松散

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The ability of the microtubule cytoskeleton to rapidly and locally reorganize itself in response to intra- and extracellular signals is essential to its wide range of functions. A site of tightly regulated microtubule dynamics-and the major interface between the microtubule cytoskeleton and the extracellular environment-is the cell cortex, where the selective stabilization and destabilization of microtubule plus-ends is required for normal cell division, morphogenesis and migration. In a recent study, we found that the cortex of Drosophila S2 and D17 cells is coated with the microtubule severing enzyme and plus-end depolymerase, Kat-60, which actively suppresses microtubule growth and stability along the cell edge. We have proposed that cortical Kat-60 functions by uncapping plus-ends, thereby activating another microtubule depolymerase, KLP10A, preloaded onto the end. The localized destruction of microtubule plus-ends at a specific cortical could feed into larger regulatory pathways, such as those in control of the actin cytoskeleton, to influence cell polarization and motility.
机译:微管细胞骨架响应于细胞内和细胞外信号而迅速和局部重组的能力对于其广泛的功能至关重要。细胞皮层是受到严格调节的微管动力学部位,并且是微管细胞骨架与细胞外环境之间的主要界面。在这里,正常的细胞分裂,形态发生和迁移需要微管正端的选择性稳定和去稳定作用。在最近的一项研究中,我们发现果蝇S2和D17细胞的皮层被微管切断酶和正向末端解聚酶Kat-60覆盖,该酶积极抑制微管的生长和沿细胞边缘的稳定性。我们已经提出,通过打开末端的末端来使皮质Kat-60发挥功能,从而激活另一种预加载到末端的微管解聚酶KLP10A。在特定皮层的微管正端的局部破坏可能会进入更大的调节途径,例如控制肌动蛋白细胞骨架的那些,从而影响细胞极化和运动性。

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