梯度检测机制:轴突寻路与真核细胞迁移的比较。

Anne von Philipsborn, Martin Bastmeyer
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引用次数: 64

摘要

趋化线索的梯度检测是迁移细胞和生长轴突的共同任务。真核生物的梯度检测采用空间机制,这意味着外部梯度必须转化为细胞内的信号梯度,从而影响细胞的极化和定向运动。梯度检测的灵敏度受信号放大和自适应机制的影响。比较三种典型的趋化细胞类型(盘状骨细胞、中性粒细胞和成纤维细胞)和神经元生长锥中梯度检测的主要信号转导途径,揭示了保守的机制,如局部PI3激酶/PIP3信号传导和共同输出,即Rho GTPases对细胞骨架的调节。局部蛋白翻译在成纤维细胞和神经元生长锥的定向运动中都起作用。Ca(2+)信号在生长锥梯度检测中起重要作用。不同细胞类型之间信号的多样性及其功能意义在生物学背景下是有意义的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mechanisms of gradient detection: a comparison of axon pathfinding with eukaryotic cell migration.

The detection of gradients of chemotactic cues is a common task for migrating cells and outgrowing axons. Eukaryotic gradient detection employs a spatial mechanism, meaning that the external gradient has to be translated into an intracellular signaling gradient, which affects cell polarization and directional movement. The sensitivity of gradient detection is governed by signal amplification and adaptation mechanisms. Comparison of the major signal transduction pathways underlying gradient detection in three exemplary chemotaxing cell types, Dictyostelium, neutrophils, and fibroblasts and in neuronal growth cones, reveals conserved mechanisms such as localized PI3 kinase/PIP3 signaling and a common output, the regulation of the cytoskeleton by Rho GTPases. Local protein translation plays a role in directional movement of both fibroblasts and neuronal growth cones. Ca(2+) signaling is prominently involved in growth cone gradient detection. The diversity of signaling between different cell types and its functional implications make sense in the biological context.

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