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肌动球蛋白控制上皮细胞的平面性和折叠,以响应压缩。

Actomyosin controls planarity and folding of epithelia in response to compression.

机构信息

London Centre for Nanotechnology, University College London, London, UK.

Centre for Computation, Mathematics and Physics in the Life Sciences and Experimental Biology, University College London, London, UK.

出版信息

Nat Mater. 2020 Jan;19(1):109-117. doi: 10.1038/s41563-019-0461-x. Epub 2019 Aug 26.

Abstract

Throughout embryonic development and adult life, epithelia are subjected to compressive deformations. While these have been shown to trigger mechanosensitive responses such as cell extrusion and differentiation, which span tens of minutes, little is known about how epithelia adapt to compression over shorter timescales. Here, using suspended epithelia, we uncover the immediate response of epithelial tissues to the application of in-plane compressive strains (5-80%). We show that fast compression induces tissue buckling followed by actomyosin-dependent tissue flattening that erases the buckle within tens of seconds, in both mono- and multi-layered epithelia. Strikingly, we identify a well-defined limit to this response, so that stable folds form in the tissue when compressive strains exceed a 'buckling threshold' of ~35%. A combination of experiment and modelling shows that this behaviour is orchestrated by adaptation of the actomyosin cytoskeleton as it re-establishes tissue tension following compression. Thus, tissue pre-tension allows epithelia to both buffer against deformation and sets their ability to form and retain folds during morphogenesis.

摘要

在胚胎发育和成年期,上皮细胞会受到压缩变形。尽管这些变形已被证明会引发机械敏感反应,如细胞外排和分化,其持续时间长达数十分钟,但对于上皮细胞如何在更短的时间内适应压缩知之甚少。在这里,我们使用悬浮上皮细胞,揭示了上皮组织对平面压缩应变(5-80%)施加的即时反应。我们表明,快速压缩会引起组织弯曲,随后是肌动球蛋白依赖性的组织变平,在单层和多层上皮组织中,在数十秒内消除了褶皱。引人注目的是,我们确定了这种反应的明确限制,因此当压缩应变超过~35%的“屈曲阈值”时,组织中会形成稳定的褶皱。实验和模型的组合表明,这种行为是由肌动球蛋白细胞骨架的适应性协调的,因为它在压缩后重新建立组织张力。因此,组织预张力使上皮细胞既能缓冲变形,又能在形态发生过程中形成和保留褶皱。

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