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细胞铺展过程中的初始接触导向与收缩性无关。

Initial contact guidance during cell spreading is contractility-independent.

机构信息

Max Planck Institute for Intelligent Systems, Department of New Materials and Biosystems, Heisenbergstrasse 3, 70569 Stuttgart, Germany.

出版信息

Soft Matter. 2017 Aug 2;13(30):5158-5167. doi: 10.1039/c6sm02685k.

Abstract

A wide variety of cell types exhibit substrate topography-based behavior, also known as contact guidance. However, the precise cellular mechanisms underlying this process are still unknown. In this study, we investigated contact guidance by studying the reaction of human endothelial cells (ECs) to well-defined microgroove topographies, both during and after initial cell spreading. As the cytoskeleton plays a major role in cellular adaptation to topographical features, two methods were used to perturb cytoskeletal structures. Inhibition of actomyosin contractility with the chemical inhibitor blebbistatatin demonstrated that initial contact guidance events are independent of traction force generation. However, cell alignment to the grooved substrate was altered at later time points, suggesting an initial 'passive' phase of contact guidance, followed by a contractility-dependent 'active' phase that relies on mechanosensitive feedback. The actin cytoskeleton was also perturbed in an indirect manner by culturing cells upside down, resulting in decreased levels of contact guidance and suggesting that a possible loss of contact between the actin cytoskeleton and the substrate could lead to cytoskeleton impairment. The process of contact guidance at the microscale was found to be primarily lamellipodia driven, as no bias in filopodia extension was observed on micron-scale grooves.

摘要

多种细胞类型表现出基于基质形貌的行为,也称为接触导向。然而,这一过程的确切细胞机制仍不清楚。在这项研究中,我们通过研究人内皮细胞(ECs)对明确定义的微沟槽形貌的反应,研究了接触导向,包括在初始细胞铺展期间和之后。由于细胞骨架在细胞适应形貌特征方面起着重要作用,因此使用了两种方法来干扰细胞骨架结构。用化学抑制剂 blebbistatatin 抑制肌动球蛋白收缩性表明,初始接触导向事件与牵引力的产生无关。然而,细胞在稍后的时间点对沟槽基底的排列发生了改变,这表明存在一个初始的“被动”接触导向阶段,然后是依赖于细胞收缩性的“主动”阶段,该阶段依赖于机械敏感性反馈。细胞倒置培养也以间接方式干扰了肌动蛋白细胞骨架,导致接触导向水平降低,这表明肌动蛋白细胞骨架与基底之间可能失去接触,从而导致细胞骨架损伤。在微尺度上,接触导向过程主要由片状伪足驱动,因为在微米尺度的沟槽上没有观察到丝状伪足延伸的偏差。

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