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细胞簇的软化触发了体内的集体细胞迁移。

Cell clusters softening triggers collective cell migration in vivo.

机构信息

Mechanisms of Morphogenesis Laboratory, Gulbenkian Institute of Science (IGC), Oeiras, Portugal.

Computational Biological Physics Laboratory, Department of Chemistry and Physics, Augusta University, Augusta, GA, USA.

出版信息

Nat Mater. 2022 Nov;21(11):1314-1323. doi: 10.1038/s41563-022-01323-0. Epub 2022 Aug 15.

Abstract

Embryogenesis, tissue repair and cancer metastasis rely on collective cell migration. In vitro studies propose that cells are stiffer while migrating in stiff substrates, but softer when plated in compliant surfaces which are typically considered as non-permissive for migration. Here we show that cells within clusters from embryonic tissue dynamically decrease their stiffness in response to the temporal stiffening of their native substrate to initiate collective cell migration. Molecular and mechanical perturbations of embryonic tissues reveal that this unexpected mechanical response involves a mechanosensitive pathway relying on Piezo1-mediated microtubule deacetylation. We further show that decreasing microtubule acetylation and consequently cluster stiffness is sufficient to trigger collective cell migration in soft non-permissive substrates. This suggests that reaching an optimal cluster-to-substrate stiffness ratio is essential to trigger the onset of this collective process. Overall, these in vivo findings challenge the current understanding of collective cell migration and its physiological and pathological roles.

摘要

胚胎发生、组织修复和癌症转移依赖于细胞的集体迁移。体外研究表明,细胞在刚性基质中迁移时更硬,而在顺应性表面上(通常被认为不利于迁移)更软。在这里,我们表明,胚胎组织中的细胞簇会根据其天然基质的时间依赖性变硬而动态降低其刚度,从而启动细胞的集体迁移。对胚胎组织的分子和力学扰动表明,这种出乎意料的力学反应涉及一个依赖 Piezo1 介导的微管去乙酰化的机械敏感途径。我们进一步表明,降低微管乙酰化水平,从而降低细胞簇的硬度,足以在软的非允许基质中触发细胞的集体迁移。这表明,达到最佳的细胞簇-基质硬度比对于触发这一集体过程的开始至关重要。总的来说,这些体内发现挑战了对细胞的集体迁移及其生理和病理作用的现有理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e4cf/9622418/19a0c4f1c307/41563_2022_1323_Fig1_HTML.jpg

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