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膀胱癌细胞对基质刚性的形态和机械稳定性的响应。

Morphological and mechanical stability of bladder cancer cells in response to substrate rigidity.

机构信息

Institute of Nuclear Physics, Polish Academy of Sciences, PL-31341 Kraków, Poland.

Institute of Nuclear Physics, Polish Academy of Sciences, PL-31341 Kraków, Poland.

出版信息

Biochim Biophys Acta Gen Subj. 2019 Jun;1863(6):1006-1014. doi: 10.1016/j.bbagen.2019.03.010. Epub 2019 Mar 14.

Abstract

BACKGROUND

Morphology of cells can be considered as an interplay between the accessibility of substrate anchoring sites, cytoskeleton properties and cellular deformability. To withstand tension induced by cell's environment, cells tend to spread out and, simultaneously, to remodel actin filament organization.

METHODS

In this context, the use of polyacrylamide hydrogel substrates with a surface coated with laminin allows to trace remodeling of actin cytoskeleton during the interaction of cells with laminin-rich basement membrane. Reorganization of actin cortex can be quantified by a surface spreading area and deformability of single cells.

RESULTS

In our study, we demonstrated that morphological and mechanical alterations of bladder cancer cells in response to altered microenvironment stiffness are of biphasic nature. Threshold-dependent relations are induced by mechanical properties of cell microenvironment. Initially, fast alterations in cellular capability to spread and to deform are followed by slow-rate changes. A switch provided by cellular deformability threshold, in the case of non-malignant cells, triggers the formation of thick actin bundles accompanied by matured focal adhesions. For cancer cells, cell spreading and deformability thresholds switch between slow and fast rate of changes with weak reorganization of actin filaments and focal adhesions formation.

CONCLUSIONS

The presence of transition region enables the cells to achieve a morphological and mechanical stability, which together with altered expression of vinculin and integrins, can contribute to invasiveness of bladder cancers.

GENERAL SIGNIFICANCE

Our findings show that morphological and mechanical stability is directly related to actin filament organization used by cancer cells to adapt to altered laminin-rich microenvironment.

摘要

背景

细胞的形态可以被认为是基质附着点的可及性、细胞骨架特性和细胞可变形性之间的相互作用。为了承受细胞环境引起的张力,细胞倾向于展开,同时重塑肌动蛋白丝组织。

方法

在这种情况下,使用表面涂有层粘连蛋白的聚丙烯酰胺水凝胶底物,可以在细胞与富含层粘连蛋白的基底膜相互作用过程中追踪肌动蛋白细胞骨架的重塑。通过细胞表面扩展面积和单个细胞的可变形性来量化肌动蛋白皮质的重排。

结果

在我们的研究中,我们证明了膀胱癌细胞对微环境刚度改变的形态和力学改变具有双相性。由细胞微环境力学特性引起的阈值相关关系。最初,细胞扩展和变形能力的快速变化之后是缓慢变化。细胞变形能力阈值的开关,在非恶性细胞的情况下,触发了厚肌动蛋白束的形成,伴随着成熟的焦点粘连。对于癌细胞,细胞扩展和变形能力阈值在肌动蛋白丝和焦点粘连形成的弱重组之间在慢和快变化率之间切换。

结论

过渡区域的存在使细胞能够获得形态和力学稳定性,这与 vinculin 和整合素的改变表达一起,可能有助于膀胱癌的侵袭性。

一般意义

我们的研究结果表明,形态和力学稳定性与癌细胞用来适应改变的富含层粘连蛋白的微环境的肌动蛋白丝组织直接相关。

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