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Assembling actin filaments for protrusion

机译:组装肌动蛋白长丝进行突出

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摘要

Cell migration entails a plethora of activities combining the productive exertion of protrusive and contractile forces to allow cells to push and squeeze themselves through cell clumps, interstitial tissues or tissue borders. All these activities require the generation and turnover of actin filaments that arrange into specific, subcellular structures. The most prominent structures mediating the protrusion at the leading edges of cells include lamellipodia and filopodia as well as plasma membrane blebs. Moreover, in cells migrating on planar substratum, mechanical support is being provided by an additional, more proximally located structure termed the lamella. Here, we systematically dissect the literature concerning the mechanisms driving actin filament nucleation and elongation in the best-studied protrusive structure, the lamellipodium. Recent work has shed light on open questions in lamellipodium protrusion, including the relative contributions of nucleation versus elongation to the assembly of both individual filaments and the lamellipodial network as a whole. However, much remains to be learned concerning the specificity and relevance of individual factors, their cooperation and their site-specific functions relative to the importance of global actin monomer and filament homeostasis.
机译:细胞迁移需要一种相结合突出和收缩力的生产性积累的多种活动,使细胞通过细胞团块,间质组织或组织边界来推动和挤压自己。所有这些活动都需要肌动蛋白细丝的一代和营业型,这些细丝安排成特定的亚细胞结构。在细胞的前缘处介导突起的最突出的结构包括层层斑块和氟化绦虫以及质膜脑膜膜。此外,在迁移平面底皮上的细胞中,由薄片赋予薄片的另外的更近侧定位的结构提供机械载体。在这里,我们系统地将文献描述了关于驱动肌动蛋白长丝成核的机制和最佳研究的突出结构,层状斑块的机制。最近的工作在层状突起中的开放性问题上阐明了阐明的问题,包括整体核切割与伸长率的相对贡献。然而,关于个人因素,合作及其特定职能的特殊性和相关性相对于全球肌动蛋白单体和长丝稳态的重要性,还有很多遗留情况。

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