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计算机模拟揭示了组织核动力蛋白力量以分离中心体的机制。

Computer simulations reveal mechanisms that organize nuclear dynein forces to separate centrosomes.

作者信息

De Simone Alessandro, Gönczy Pierre

机构信息

Swiss Institute for Experimental Cancer Research, School of Life Sciences, Swiss Federal Institute of Technology, 1015 Lausanne, Switzerland.

Swiss Institute for Experimental Cancer Research, School of Life Sciences, Swiss Federal Institute of Technology, 1015 Lausanne, Switzerland

出版信息

Mol Biol Cell. 2017 Nov 7;28(23):3165-3170. doi: 10.1091/mbc.E16-12-0823. Epub 2017 Jul 12.

Abstract

Centrosome separation along the surface of the nucleus at the onset of mitosis is critical for bipolar spindle assembly. Dynein anchored on the nuclear envelope is known to be important for centrosome separation, but it is unclear how nuclear dynein forces are organized in an anisotropic manner to promote the movement of centrosomes away from each other. Here we use computational simulations of embryos to address this fundamental question, testing three potential mechanisms by which nuclear dynein may act. First, our analysis shows that expansion of the nuclear volume per se does not generate nuclear dynein-driven separation forces. Second, we find that steric interactions between microtubules and centrosomes contribute to robust onset of nuclear dynein-mediated centrosome separation. Third, we find that the initial position of centrosomes, between the male pronucleus and cell cortex at the embryo posterior, is a key determinant in organizing microtubule aster asymmetry to power nuclear dynein-dependent separation. Overall our work reveals that accurate initial centrosome position, together with steric interactions, ensures proper anisotropic organization of nuclear dynein forces to separate centrosomes, thus ensuring robust bipolar spindle assembly.

摘要

在有丝分裂开始时,中心体沿细胞核表面分离对于双极纺锤体组装至关重要。已知锚定在核膜上的动力蛋白对于中心体分离很重要,但尚不清楚核动力蛋白的力是如何以各向异性的方式组织起来,以促进中心体彼此远离移动的。在这里,我们使用胚胎的计算模拟来解决这个基本问题,测试核动力蛋白可能起作用的三种潜在机制。首先,我们的分析表明,核体积本身的扩大并不会产生由核动力蛋白驱动的分离力。其次,我们发现微管与中心体之间的空间相互作用有助于核动力蛋白介导的中心体分离的强劲起始。第三,我们发现中心体在胚胎后部雄原核与细胞皮层之间的初始位置,是组织微管星状体不对称以驱动依赖核动力蛋白的分离的关键决定因素。总体而言,我们的研究表明,准确的中心体初始位置与空间相互作用一起,确保了核动力蛋白力的适当各向异性组织以分离中心体,从而确保强劲的双极纺锤体组装。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e25/5687019/d511c96aa9da/3165fig1.jpg

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