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Membrane allocation profiling: a method to characterize three-dimensional cell shape and attachment based on surface reconstruction.

机译:膜分配分析:一种基于表面重建表征三维单元形状和附着的方法。

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Three-dimensional surface reconstructions from high resolution image stacks of biological specimens, observed by confocal microscopy, have changed the perspective of morphological understanding. In the field of cell-cell or cell-substrate interfaces, combining these two techniques leads to new insights yet also creates a tremendous amount of data. In this article, we present a technique to reduce large, multidimensional data sets from confocal microscopy into one single curve: a membrane allocation profile. Reconstructed cells are represented in a three-dimensional surface from image sections of individual cells. We virtually cut segments of the reconstructed cell membrane parallel to the substrate and calculate the surface areas of each segment. The obtained membrane allocation profiles lead to morphological insights and yield an in vivo ratio of attached and free membrane areas without cell fixation. As an example, glass substrates were modified with different proteins (fibronectin, laminin, concavalin A, extracellular matrix gel, and both isomers of poly-lysine) and presented to HEK293 cells to examine differences in cell morphology and adhesion. We proved that proteins on a substrate could increase the attached portion of a cell membrane, facing the modified substrate, from an average of 32% (glass) to 45% (poly-lysine) of the total membrane surface area.
机译:通过共聚焦显微镜观察,从生物标本的高分辨率图像堆栈进行的三维表面重建改变了形态学理解的观点。在细胞-细胞或细胞-基质界面领域,将这两种技术结合起来不仅可以带来新的见解,还可以创建大量数据。在本文中,我们提出了一种将来自共聚焦显微镜的大型多维数据集缩减为一条曲线的技术:膜分配曲线。从单个细胞的图像部分在三维表面上表示重建的细胞。我们实际上切割了平行于底物的细胞膜片段,并计算了每个片段的表面积。获得的膜分配曲线导致形态学见解,并在没有细胞固定的情况下产生附着和自由膜面积的体内比率。例如,用不同的蛋白质(纤连蛋白,层粘连蛋白,刀豆球蛋白A,细胞外基质凝胶和聚赖氨酸的两种异构体)修饰玻璃基板,然后将其呈现给HEK293细胞以检查细胞形态和粘附力的差异。我们证明了底物上的蛋白质可以使面对修饰的底物的细胞膜附着部分从平均总膜表面积的32%(玻璃)增加到45%(聚赖氨酸)。

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