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通过反射干涉对比显微镜(RICM)进行细胞膜拓扑分析可实现无标记的粘附强度定量分析。

Cell membrane topology analysis by RICM enables marker-free adhesion strength quantification.

作者信息

Klein Katharina, Rommel Christina E, Hirschfeld-Warneken Vera C, Spatz Joachim P

机构信息

Department of New Materials and Biosystems, Max Planck Institute for Intelligent Systems, Stuttgart, Germany, and Department of Biophysical Chemistry, University of Heidelberg, Heidelberg, Germany,

出版信息

Biointerphases. 2013 Dec;8(1):28. doi: 10.1186/1559-4106-8-28. Epub 2013 Oct 28.

Abstract

Reflection interference contrast microscopy (RICM) allows the visualization of the cell's adhesion topology on substrates. Here it is applied as a new label-free method to measure adhesion forces between tumor cells and their substrate without any external manipulation, i.e., the application of force or adjustments in the substrate elasticity. Malignant cancer transformation is closely associated with the down-regulation of adhesion proteins and the consequent reduction of adhesion forces. By analyzing the size and distribution of adhesion patches from a benign and a malignant human pancreatic tumor cell line, we established a model for calculating the adhesion strength based on RICM images. Further, we could show that the cell's spread area does not necessarily scale with adhesion strength. Despite the larger projected cell area of the malignant cell line, adhesion strength was clearly reduced. This underscores the importance of adhesion patch analysis. The calculated force values were verified by microfluidic detachment assays. Static and dynamic RICM measurements produce numerous adhesion-related parameters from which characteristic cell signatures can be derived. Such a cellular fingerprint can refine the process of categorizing cell lines according to their grade of differentiation.

摘要

反射干涉对比显微镜(RICM)可用于观察细胞在底物上的黏附拓扑结构。在此,它作为一种新的无标记方法,用于测量肿瘤细胞与其底物之间的黏附力,无需任何外部操作,即施加力或调整底物弹性。恶性肿瘤转化与黏附蛋白的下调以及随之而来的黏附力降低密切相关。通过分析来自良性和恶性人胰腺肿瘤细胞系的黏附斑的大小和分布,我们建立了一个基于RICM图像计算黏附强度的模型。此外,我们可以表明,细胞的铺展面积不一定与黏附强度成比例。尽管恶性细胞系的投影细胞面积较大,但其黏附强度明显降低。这突出了黏附斑分析的重要性。通过微流控分离试验验证了计算出的力值。静态和动态RICM测量产生了许多与黏附相关的参数,从中可以得出特征性的细胞特征。这样的细胞指纹可以完善根据细胞系分化程度进行分类的过程。

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