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两步搜索和运行梯度响应形状白细胞在体内导航。

A two-step search and run response to gradients shapes leukocyte navigation in vivo.

机构信息

Department of Physiology, Development and Neuroscience, Downing Site, University of Cambridge, Cambridge, UK.

Max Planck Institute of Immunobiology and Epigenetics, Freiburg, Germany.

出版信息

J Cell Biol. 2022 Aug 1;221(8). doi: 10.1083/jcb.202103207. Epub 2022 Jun 22.

Abstract

Migrating cells must interpret chemical gradients to guide themselves within tissues. A long-held principle is that gradients guide cells via reorientation of leading-edge protrusions. However, recent evidence indicates that protrusions can be dispensable for locomotion in some contexts, raising questions about how cells interpret endogenous gradients in vivo and whether other mechanisms are involved. Using laser wound assays in zebrafish to elicit acute endogenous gradients and quantitative analyses, we demonstrate a two-stage process for leukocyte chemotaxis in vivo: first a "search" phase, with stimulation of actin networks at the leading edge, cell deceleration, and turning. This is followed by a "run" phase, with fast actin flows, cell acceleration, and persistence. When actin dynamics are perturbed, cells fail to resolve the gradient, suggesting that pure spatial sensing of the gradient is insufficient for navigation. Our data suggest that cell contractility and actin flows provide memory for temporal sensing, while expansion of the leading edge serves to enhance gradient sampling.

摘要

迁移细胞必须解释化学梯度,以便在组织内为自己导航。一个长期以来的原则是,梯度通过引导前沿突起的重新定向来引导细胞。然而,最近的证据表明,在某些情况下,突起对于运动是可有可无的,这就提出了一些问题,即细胞如何在体内解释内源性梯度,以及是否涉及其他机制。我们使用斑马鱼中的激光划痕实验来引发急性内源性梯度,并进行定量分析,结果表明白细胞在体内的趋化作用是一个两阶段的过程:首先是“搜索”阶段,在前沿刺激肌动蛋白网络,细胞减速并转向。然后是“奔跑”阶段,伴随着快速的肌动蛋白流动、细胞加速和持续运动。当肌动蛋白动力学受到干扰时,细胞无法分辨梯度,这表明对梯度的纯空间感知不足以进行导航。我们的数据表明,细胞收缩性和肌动蛋白流为时间感知提供记忆,而前沿的扩展则有助于增强梯度采样。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/576f/9225946/7f9b689184aa/JCB_202103207_Fig1.jpg

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