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调节RhoA效应器可诱导受精卵向振荡性更强且更具波状的RhoA动力学转变。

Modulating RhoA effectors induces transitions to oscillatory and more wavelike RhoA dynamics in zygotes.

作者信息

Yao Baixue, Donoughe Seth, Michaux Jonathan, Munro Edwin

机构信息

Department of Molecular Genetics and Cell Biology, University of Chicago, Chicago, IL 60637.

Committee on Cell Biology, University of Chicago, Chicago, IL 60637.

出版信息

Mol Biol Cell. 2022 May 15;33(6):ar58. doi: 10.1091/mbc.E21-11-0542. Epub 2022 Feb 9.

Abstract

Pulsatile RhoA dynamics underlie a wide range of cell and tissue behaviors. The circuits that produce these dynamics in different cells share common architectures based on fast positive and delayed negative feedback through F-actin, but they can produce very different spatiotemporal patterns of RhoA activity. However, the underlying causes of this variation remain poorly understood. Here we asked how this variation could arise through modulation of actin network dynamics downstream of active RhoA in early embryos. We find that perturbing two RhoA effectors-formin and anillin-induce transitions from nonrecurrent focal pulses to either large noisy oscillatory pulses (formin depletion) or noisy oscillatory waves (anillin depletion). In both cases these transitions could be explained by changes in local F-actin levels and depletion dynamics, leading to changes in spatial and temporal patterns of RhoA inhibition. However, the underlying mechanisms for F-actin depletion are distinct, with different dependencies on myosin II activity. Thus, modulating actomyosin network dynamics could shape the spatiotemporal dynamics of RhoA activity for different physiological or morphogenetic functions.

摘要

脉动的RhoA动力学是多种细胞和组织行为的基础。在不同细胞中产生这些动力学的回路基于通过F-肌动蛋白的快速正反馈和延迟负反馈具有共同的架构,但它们可以产生非常不同的RhoA活性时空模式。然而,这种变化的根本原因仍知之甚少。在这里,我们研究了这种变化如何通过早期胚胎中活性RhoA下游的肌动蛋白网络动力学调节而产生。我们发现,干扰两种RhoA效应器——formin和膜收缩蛋白——会导致从非重复性局灶性脉冲转变为大的噪声振荡脉冲(formin缺失)或噪声振荡波(膜收缩蛋白缺失)。在这两种情况下,这些转变都可以通过局部F-肌动蛋白水平和消耗动力学的变化来解释,从而导致RhoA抑制的时空模式发生变化。然而,F-肌动蛋白消耗的潜在机制是不同的,对肌球蛋白II活性有不同的依赖性。因此,调节肌动球蛋白网络动力学可以塑造RhoA活性的时空动力学,以实现不同的生理或形态发生功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e314/9265151/0572e5e708eb/mbc-33-ar58-g001.jpg

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