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钛基底复合微沟槽和亚微米形貌的纹理方向影响人原代细胞的黏附、增殖和分化。

Texture direction of combined microgrooves and submicroscale topographies of titanium substrata influence adhesion, proliferation, and differentiation in human primary cells.

机构信息

Department of Dentistry, Graduate School of Dentistry, Kyung Hee University, 1 Hoegi-dong, Seoul 130-701, Republic of Korea.

出版信息

Arch Oral Biol. 2012 Jul;57(7):898-905. doi: 10.1016/j.archoralbio.2011.11.013. Epub 2011 Dec 19.

Abstract

OBJECTIVE

This study aimed to identify the optimal micro- and submicroscale topographies of titanium (Ti) substrata that would most significantly influence adhesion, proliferation, and other activities of these cells.

DESIGN

Truncated V-shaped microgrooves in 60 μm-wide and 10 μm-deep cross-sections with 0°, 30°, 60°, or 90° angles between the microgrooves and ridge-top submicroscale texture were created on the Ti substrata (designated NE60/10-0°, NE60/10-30°, NE60/10-60° and NE60/10-90°, respectively). Ground titanium with submicroscale texture but with no microgrooves was used as the control substratum, NE0. Scanning electron microscopic observation and the assays determining the cell adhesion, cell proliferation and osteoblast differentiation were performed.

RESULTS

Cells more actively migrated into the microgrooves on NE60/10-30° than into the microgrooves on any other substrata tested, suggesting that the cells utilise the increased surface area of the substrata at the microscale level. NE60/10-0° and NE60/10-30° substrata generally enhanced adhesion, proliferation, alkaline phosphatase activity, and osteoblast differentiation of human primary cells when compared to other Ti substrata, and significant correlations were observed between these cellular activities.

CONCLUSIONS

Here, we show that the contact guidance of human primary cells grown on Ti substrata can be controlled more by specific submicroscale textures on ridge tops than by the dimensions of surface microgrooves only. Also, the degree of angles created between the submicroscale textures and microgrooves on Ti substrata significantly affect cell adhesion, proliferation and differentiation in human primary cells.

摘要

目的

本研究旨在确定钛(Ti)基底的最佳微观和亚微观形貌,以最显著地影响这些细胞的黏附、增殖和其他活性。

设计

在 Ti 基底上制作了横截面为 60 μm 宽、10 μm 深的截断 V 形微槽,微槽与脊顶亚微观纹理之间的夹角分别为 0°、30°、60°和 90°(分别命名为 NE60/10-0°、NE60/10-30°、NE60/10-60°和 NE60/10-90°)。具有亚微观纹理但无微槽的研磨钛被用作对照基底,命名为 NE0。进行了扫描电子显微镜观察和测定细胞黏附、细胞增殖和成骨细胞分化的实验。

结果

细胞更积极地迁移到 NE60/10-30°的微槽中,而不是迁移到其他测试基底的微槽中,这表明细胞利用了微尺度基底的增加表面积。与其他 Ti 基底相比,NE60/10-0°和 NE60/10-30°基底通常增强了人原代细胞的黏附、增殖、碱性磷酸酶活性和成骨细胞分化,并且这些细胞活性之间存在显著相关性。

结论

在这里,我们表明人原代细胞在 Ti 基底上的生长可以通过脊顶的特定亚微观纹理来更好地控制接触引导,而不仅仅是通过表面微槽的尺寸。此外,Ti 基底上亚微观纹理和微槽之间形成的角度的程度显著影响人原代细胞的黏附、增殖和分化。

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