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一个注定要发生凋亡的上皮细胞通过一种肌动蛋白和肌球蛋白依赖的机制向其相邻细胞发出信号,使其将自身挤出。

An epithelial cell destined for apoptosis signals its neighbors to extrude it by an actin- and myosin-dependent mechanism.

作者信息

Rosenblatt J, Raff M C, Cramer L P

机构信息

Medical Research Council-Laboratory for Molecular Cell Biology, University College London, WC1E 6BT, United Kingdom.

出版信息

Curr Biol. 2001 Nov 27;11(23):1847-57. doi: 10.1016/s0960-9822(01)00587-5.

DOI:10.1016/s0960-9822(01)00587-5
PMID:11728307
Abstract

BACKGROUND

Simple epithelia encase developing embryos and organs. Although these epithelia consist of only one or two layers of cells, they must provide tight barriers for the tissues that they envelop. Apoptosis occurring within these simple epithelia could compromise this barrier. How, then, does an epithelium remove apoptotic cells without disrupting its function as a barrier?

RESULTS

We show that apoptotic cells are extruded from a simple epithelium by the concerted contraction of their neighbors. A ring of actin and myosin forms both within the apoptotic cell and in the cells surrounding it, and contraction of the ring formed in the live neighbors is required for apoptotic cell extrusion, as injection of a Rho GTPase inhibitor into these cells completely blocks extrusion. Addition of apoptotic MDCK cells to an intact monolayer induces the formation of actin cables in the cells contacted, suggesting that the signal to form the cable comes from the dying cell. The signal is produced very early in the apoptotic process, before procaspase activation, cell shrinkage, or phosphatidylserine exposure. Remarkably, electrical resistance studies show that epithelial barrier function is maintained, even when large numbers of dying cells are being extruded.

CONCLUSIONS

We propose that apoptotic cell extrusion is important for the preservation of epithelial barrier function during cell death. Our results suggest that an early signal from the dying cell activates Rho in live neighbors to extrude the apoptotic cell out of the epithelium.

摘要

背景

单层上皮包裹着发育中的胚胎和器官。尽管这些上皮仅由一层或两层细胞组成,但它们必须为其所包裹的组织提供紧密的屏障。发生在这些单层上皮内的细胞凋亡可能会损害这一屏障。那么,上皮是如何在不破坏其屏障功能的情况下清除凋亡细胞的呢?

结果

我们发现凋亡细胞是通过其相邻细胞的协同收缩而从单层上皮中被挤出的。肌动蛋白和肌球蛋白环在凋亡细胞及其周围的细胞内均形成,而存活相邻细胞中形成的环的收缩对于凋亡细胞的挤出是必需的,因为向这些细胞中注射 Rho GTPase 抑制剂会完全阻断挤出过程。将凋亡的 MDCK 细胞添加到完整的单层细胞中会诱导与其接触的细胞中形成肌动蛋白束,这表明形成肌动蛋白束的信号来自即将死亡的细胞。该信号在凋亡过程的早期产生,早于半胱天冬酶原激活、细胞收缩或磷脂酰丝氨酸暴露。值得注意的是,电阻研究表明,即使有大量即将死亡的细胞被挤出,上皮屏障功能仍能维持。

结论

我们提出凋亡细胞挤出对于细胞死亡期间上皮屏障功能的维持很重要。我们的结果表明,来自即将死亡细胞的早期信号激活存活相邻细胞中的 Rho,从而将凋亡细胞挤出上皮。

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