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细胞内压力的动态不稳定性驱动泡状运动。

Dynamic instability of the intracellular pressure drives bleb-based motility.

机构信息

Institut Curie, Centre de Recherche, Paris, 75248, France.

出版信息

J Cell Sci. 2010 Nov 15;123(Pt 22):3884-92. doi: 10.1242/jcs.065672. Epub 2010 Oct 27.

Abstract

We have demonstrated that the two- and three-dimensional motility of the human pathogenic parasite Entamoeba histolytica (Eh) depends on sustained instability of the intracellular hydrostatic pressure. This instability drives the cyclic generation and healing of membrane blebs, with typical protrusion velocities of 10-20 μm/second over a few hundred milliseconds and healing times of 10 seconds. The use of a novel micro-electroporation method to control the intracellular pressure enabled us to develop a qualitative model with three parameters: the rate of the myosin-driven internal pressure increase; the critical disjunction stress of membrane-cytoskeleton bonds; and the turnover time of the F-actin cortex. Although blebs occur randomly in space and irregularly time, they can be forced to occur with a defined periodicity in confined geometries, thus confirming our model. Given the highly efficient bleb-based motility of Eh in vitro and in vivo, Eh cells represent a unique model for studying the physical and biological aspects of amoeboid versus mesenchymal motility in two- and three-dimensional environments.

摘要

我们已经证明,人类病原体溶组织内阿米巴(Eh)的二维和三维运动依赖于细胞内静压的持续不稳定性。这种不稳定性驱动了膜泡的循环产生和愈合,典型的突起速度为 10-20μm/秒,持续几百毫秒,愈合时间为 10 秒。我们使用一种新颖的微电穿孔方法来控制细胞内压力,从而开发了一个具有三个参数的定性模型:肌球蛋白驱动的内部压力增加率;膜-细胞骨架键的临界分离应力;以及 F-肌动蛋白皮层的周转率。尽管膜泡在空间中随机发生,在时间上不规则,但它们可以在受限的几何形状中被强制以定义的周期性发生,从而证实了我们的模型。鉴于 Eh 在体外和体内的高效基于膜泡的运动,Eh 细胞代表了研究阿米巴样和间质样运动在二维和三维环境中的物理和生物学方面的独特模型。

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