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首页> 外文期刊>Molecular biology of the cell >A theoretical model of cytokinesis implicates feedback between membrane curvature and cytoskeletal organization in asymmetric cytokinetic furrowing
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A theoretical model of cytokinesis implicates feedback between membrane curvature and cytoskeletal organization in asymmetric cytokinetic furrowing

机译:细胞分裂的理论模型牵涉在不对称的细胞动力学犁沟中膜曲率和细胞骨架组织之间的反馈

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摘要

During cytokinesis, the cell undergoes a dramatic shape change as it divides into two daughter cells. Cell shape changes in cytokinesis are driven by a cortical ring rich in actin filaments and nonmuscle myosin II. The ring closes via actomyosin contraction coupled with actin depolymerization. Of interest, ring closure and hence the furrow ingression are nonconcentric (asymmetric) within the division plane across Metazoa. This nonconcentricity can occur and persist even without preexisting asymmetric cues, such as spindle placement or cellular adhesions. Cell-autonomous asymmetry is not explained by current models. We combined quantitative high-resolution live-cell microscopy with theoretical modeling to explore the mechanistic basis for asymmetric cytokinesis in the Caenorhabditis elegans zygote, with the goal of uncovering basic principles of ring closure. Our theoretical model suggests that feedback among membrane curvature, cytoskeletal alignment, and contractility is responsible for asymmetric cytokinetic furrowing. It also accurately predicts experimental perturbations of conserved ring proteins. The model further suggests that curvature-mediated filament alignment speeds up furrow closure while promoting energy efficiency. Collectively our work underscores the importance of membrane–cytoskeletal anchoring and suggests conserved molecular mechanisms for this activity.
机译:在胞质分裂过程中,细胞分裂为两个子细胞,经历了剧烈的形状变化。胞质分裂的细胞形状变化是由富含肌动蛋白丝和非肌球蛋白II的皮质环驱动的。该环通过肌动球蛋白收缩结合肌动蛋白解聚而闭合。有趣的是,在后生动物的分裂平面内,闭环和因此的沟进入是非同心的(不对称的)。即使没有预先存在的不对称提示(例如纺锤放置或细胞粘附),这种非同心性也会发生并持续存在。当前模型没有解释单元自治的不对称性。我们结合定量高分辨率活细胞显微镜与理论模型,以探索秀丽隐杆线虫合子不对称胞质分裂的机制基础,目的是揭示闭环的基本原理。我们的理论模型表明,膜曲率,细胞骨架排列和收缩力之间的反馈是造成不对称细胞动力学犁沟的原因。它还准确地预测了保守环蛋白的实验扰动。该模型进一步表明,曲率介导的灯丝排列加快了沟闭合,同时提高了能源效率。我们的工作共同强调了膜-细胞骨架锚固的重要性,并提出了保守的分子机制进行这项活动。

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