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通过在微图案化表面上接种来放大乳腺癌细胞的核变形,以更好地区分它们的恶性程度。

Amplification of nuclear deformation of breast cancer cells by seeding on micropatterned surfaces to better distinguish their malignancies.

机构信息

BIOMATEN, Middle East Technical University (METU) Center of Excellence in Biomaterials and Tissue Engineering, Ankara, Turkey; METU, Department of Biotechnology, Ankara, Turkey.

Department of Radiology, School of Medicine, Stanford University, Palo Alto, CA, 94304, USA.

出版信息

Colloids Surf B Biointerfaces. 2019 Nov 1;183:110402. doi: 10.1016/j.colsurfb.2019.110402. Epub 2019 Jul 30.

Abstract

Information about the mechanical properties of cancer cells leads to new insights about their malignancy levels. The more flexible the cancer cells and their nuclei are, the more aggressive and invasive they are. Flexibility is a result of composition and properties of molecular constituents of cells and its extent is expressed by deformation. Differences in the mechanical properties could be modulated by topography and chemistry of the substrate. In this study, the main hypothesis is that the difference in the mechanical properties of malignant and benign breast cancer cells could be used as a discriminator of these cells and reflected by the extent of nuclear deformation on micropatterned substrates. We compared benign (MCF10A), malignantnoninvasive (MCF7), and malignant highly invasive (MDAMB231) breast cancer cell lines using their nuclear deformability on micropatterned surfaces designed with square prism-shaped micropillars of poly(methyl methacrylate) (PMMA) (8 μm high, 4 × 4 μm area, 4 μm gap). Several shape descriptors (circularity, solidity, roundness, aspect ratio) were used to analyze nuclear deformation. We were able to discriminate the three cells when the descriptor circularity and hydrophobic micropatterned surfaces were used. The cells showed nuclear deformability in the order following the extent of their malignancies. The most aggressive cell, MDAMB231, had the lowest circularity value, 0.37, whereas the noninvasive malignant, MCF7, and benign, MCF10A, cells had higher values 0.47 and 0.77, respectively. Mechanism of the deformation was shown at the molecular level that the expression of Lamin A/C and Nesprin-2 genes decreased with increased nuclear deformation. In summary, biomechanical properties of cells can provide useful information about their cancer state and they can be reflected in the biological markers.

摘要

癌细胞力学特性的信息可提供有关其恶性程度的新见解。癌细胞及其核的灵活性越高,其侵袭性和侵略性就越强。细胞的灵活性是由细胞分子成分的组成和性质决定的,其程度通过变形来表达。细胞的力学特性差异可以通过基底的形貌和化学性质进行调节。在这项研究中,主要假设是恶性和良性乳腺癌细胞在力学特性上的差异可用作这些细胞的鉴别标准,并通过在微图案化基底上的核变形程度来反映。我们使用良性(MCF10A)、恶性非侵袭性(MCF7)和恶性高侵袭性(MDAMB231)乳腺癌细胞系在由聚甲基丙烯酸甲酯(PMMA)制成的具有正方形棱柱形微柱的微图案化表面(8 μm 高、4 × 4 μm 面积、4 μm 间隙)上的核变形来比较它们。使用了几个形状描述符(圆形度、密实度、圆度、纵横比)来分析核变形。当使用描述符圆形度和疏水性微图案化表面时,我们能够区分这三种细胞。根据其恶性程度的大小,细胞表现出核变形能力。最具侵略性的细胞 MDAMB231 的圆形度值最低,为 0.37,而非侵袭性恶性细胞 MCF7 和良性细胞 MCF10A 的圆形度值分别为 0.47 和 0.77。变形的机制在分子水平上得到了显示,即 Lamin A/C 和 Nesprin-2 基因的表达随着核变形的增加而减少。总之,细胞的生物力学特性可以提供有关其癌症状态的有用信息,并且可以反映在生物标志物中。

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