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细胞骨架蛋白组装体的重建用于大规模的膜转化。

Reconstitution of cytoskeletal protein assemblies for large-scale membrane transformation.

机构信息

Centro de Investigaciones Biológicas, CSIC, 28040 Madrid, Spain.

Max Planck Institute for Biochemistry, Martinsried, Germany.

出版信息

Curr Opin Chem Biol. 2014 Oct;22:18-26. doi: 10.1016/j.cbpa.2014.07.018. Epub 2014 Aug 12.

Abstract

Membranes determine two-dimensional and three-dimensional biochemical reaction spaces in living systems. Defining size and shape of surfaces and volumes encompassed by membrane is of key importance for cellular metabolism and homeostasis, and the maintenance and controlled transformation of membrane shapes are coordinated by a large number of different protein assemblies. The orchestration of spatial elements over distances orders of magnitudes larger than protein molecules, as required for cell division, is a particularly challenging task, requiring large-scale ordered protein filaments and networks. The structure and function of these networks, particularly of cytoskeletal elements, have been characterized extensively in cells and reconstituted systems. However, their co-reconstitution with membranes from the bottom-up under defined conditions, to elucidate their mode of action in detail, is still a relatively new field of research. In this short review, we discuss recent approaches and achievements with regard to the study of cytoskeletal protein assemblies on model membranes, with specific focus on contractile elements as those based on the bacterial division FtsZ protein and eukaryotic actomyosin structures.

摘要

膜在生命系统中决定了二维和三维生化反应空间。定义膜所包含的表面和体积的大小和形状对于细胞代谢和内稳态至关重要,并且膜形状的维持和受控转化是由大量不同的蛋白质组装协调的。在细胞分裂等需要远远超过蛋白质分子的距离尺度上,对空间元素进行协调是一项特别具有挑战性的任务,需要大规模的有序蛋白质丝和网络。这些网络的结构和功能,特别是细胞骨架元件的结构和功能,已经在细胞和重建系统中得到了广泛的描述。然而,在定义的条件下从底部向上重建它们与膜的共组装,以详细阐明其作用模式,仍然是一个相对较新的研究领域。在这篇简短的综述中,我们讨论了关于在模型膜上研究细胞骨架蛋白组装的最新方法和进展,特别关注基于细菌分裂 FtsZ 蛋白和真核肌动球蛋白结构的收缩元件。

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