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是什么促使细胞移动:自发细胞运动的要求和障碍。

What makes cells move: requirements and obstacles for spontaneous cell motility.

作者信息

Binamé Fabien, Pawlak Geraldine, Roux Pierre, Hibner Urszula

机构信息

CNRS, UMR 5535, IGMM, 1919 route de Mende, 34293 Montpellier, France.

出版信息

Mol Biosyst. 2010 Apr;6(4):648-61. doi: 10.1039/b915591k. Epub 2010 Jan 25.

Abstract

Movement of individual cells and of cellular cohorts, chains or sheets requires physical forces that are established through interactions of cells with their environment. In vivo, migration occurs extensively during embryonic development and in adults during wound healing and tumorigenesis. In order to identify the molecular events involved in cell movement, in vitro systems have been developed. These have contributed to the definition of a number of molecular pathways put into play in the course of migratory behaviours, such as mesenchymal and amoeboid movement. More recently, our knowledge of migratory modes has been enriched by analyses of cells exploring and moving through three-dimensional (3D) matrices. While the cells' morphologies differ in 2D and 3D environments, the basic mechanisms that put a cellular body into motion are remarkably similar. Thus, in both 2D and 3D, the polarity of the migrating cell is initially defined by a specific subcellular localization of signalling molecules and components of molecular machines required for motion. While the polarization can be initiated either in response to extracellular signalling or be a chance occurrence, it is reinforced and sustained by positive feedback loops of signalling molecules. Second, adhesion to a substratum is necessary to generate forces that will propel the cell engaged in either mesenchymal or ameboid migration. For collective cell movement, intercellular coordination constitutes an additional requirement: a cell cohort remains stationary if individual cells pull in opposite directions. Finally, the availability of space to move into is a general requirement to set cells into motion. Lack of free space is probably the main obstacle for migration of most healthy cells in an adult multicellular organism. Thus, the requirements for cell movement are both intrinsic to the cell, involving coordinated signalling and interactions with molecular machines, and extrinsic, imposed by the physicochemical nature of the environment. In particular, the geometry and stiffness of the support act on a range of signalling pathways that induce specific cell migratory responses. These issues are discussed in the present review in the context of published work and our own data on collective migration of hepatocyte cohorts.

摘要

单个细胞以及细胞群体、细胞链或细胞层的移动需要通过细胞与其环境的相互作用建立的物理力。在体内,迁移在胚胎发育过程中广泛发生,在成体中则发生在伤口愈合和肿瘤发生过程中。为了确定参与细胞移动的分子事件,人们开发了体外系统。这些系统有助于定义在迁移行为过程中发挥作用的一些分子途径,如间充质运动和阿米巴样运动。最近,通过对探索并在三维(3D)基质中移动的细胞的分析,我们对迁移模式的认识得到了丰富。虽然细胞在二维(2D)和三维环境中的形态不同,但使细胞体运动的基本机制非常相似。因此,在二维和三维环境中,迁移细胞的极性最初都是由信号分子和运动所需分子机器组件的特定亚细胞定位来定义的。虽然极化可以响应细胞外信号启动,也可能是偶然发生,但它会通过信号分子的正反馈回路得到加强和维持。其次,与基质的粘附对于产生推动参与间充质或阿米巴样迁移的细胞的力是必要的。对于集体细胞移动,细胞间协调是另一个要求:如果单个细胞向相反方向拉扯,细胞群体就会保持静止。最后,有可移动的空间是使细胞运动的一个普遍要求。缺乏自由空间可能是成年多细胞生物体中大多数健康细胞迁移的主要障碍。因此,细胞移动的要求既有细胞内在的,涉及协调的信号传导和与分子机器的相互作用,也有外在的,由环境的物理化学性质决定。特别是,支持物的几何形状和硬度作用于一系列诱导特定细胞迁移反应的信号通路。在本综述中,我们将结合已发表的研究工作以及我们自己关于肝细胞群体集体迁移的数据来讨论这些问题。

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