Topographical depth reveals contact guidance mechanism distinct from focal adhesion confinement

IF 2.4 4区 生物学 Q4 CELL BIOLOGY Cytoskeleton Pub Date : 2024-01-16 DOI:10.1002/cm.21810
Michael C. Robitaille, Chunghwan Kim, Joseph A. Christodoulides, Patrick J. Calhoun, Wonmo Kang, Jinny Liu, Jeff M. Byers, Marc P. Raphael
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Abstract

Cellular response to the topography of their environment, known as contact guidance, is a crucial aspect to many biological processes yet remains poorly understood. A prevailing model to describe cellular contact guidance involves the lateral confinement of focal adhesions (FA) by topography as an underlying mechanism governing how cells can respond to topographical cues. However, it is not clear how this model is consistent with the well-documented depth-dependent contact guidance responses in the literature. To investigate this model, we fabricated a set of contact guidance chips with lateral dimensions capable of confining focal adhesions and relaxing that confinement at various depths. We find at the shallowest depth of 330 nm, the model of focal adhesion confinement is consistent with our observations. However, the cellular response at depths of 725 and 1000 nm is inadequately explained by this model. Instead, we observe a distinct reorganization of F-actin at greater depths in which topographically induced cell membrane deformation alters the structure of the cytoskeleton. These results are consistent with an alternative curvature-hypothesis to explain cellular response to topographical cues. Together, these results indicate a confluence of two molecular mechanisms operating at increased induced membrane curvature that govern how cells sense and respond to topography.

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地形深度揭示了不同于病灶粘附限制的接触引导机制。
细胞对其所处环境地形的反应,即接触引导,是许多生物过程的一个重要方面,但人们对它的了解仍然很少。描述细胞接触引导的一个流行模型涉及地形对焦点粘附(FA)的横向限制,这是细胞如何对地形线索做出反应的基本机制。然而,目前还不清楚这一模型如何与文献中记录详实的深度依赖性接触引导反应相一致。为了研究这一模型,我们制作了一组接触引导芯片,其横向尺寸能够限制病灶粘附,并在不同深度放松这种限制。我们发现,在 330 纳米的最浅深度,病灶粘附限制模型与我们的观察结果一致。然而,在 725 纳米和 1000 纳米深度的细胞反应却无法用该模型充分解释。相反,我们在更深的深度观察到了 F-肌动蛋白的明显重组,其中拓扑诱导的细胞膜变形改变了细胞骨架的结构。这些结果与解释细胞对地形线索反应的另一种曲率假说是一致的。总之,这些结果表明,在诱导膜曲率增加的情况下,有两种分子机制在起作用,它们支配着细胞如何感知地形并做出反应。
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来源期刊
Cytoskeleton
Cytoskeleton CELL BIOLOGY-
CiteScore
5.50
自引率
3.40%
发文量
24
审稿时长
6-12 weeks
期刊介绍: Cytoskeleton focuses on all aspects of cytoskeletal research in healthy and diseased states, spanning genetic and cell biological observations, biochemical, biophysical and structural studies, mathematical modeling and theory. This includes, but is certainly not limited to, classic polymer systems of eukaryotic cells and their structural sites of attachment on membranes and organelles, as well as the bacterial cytoskeleton, the nucleoskeleton, and uncoventional polymer systems with structural/organizational roles. Cytoskeleton is published in 12 issues annually, and special issues will be dedicated to especially-active or newly-emerging areas of cytoskeletal research.
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