Revealing the Cell–Material Interface with Nanometer Resolution by Focused Ion Beam/Scanning Electron Microscopy

纳米 材料科学 聚焦离子束 纳米技术 扫描电子显微镜 扫描共焦电子显微镜 电子束诱导沉积 分辨率(逻辑) 离子 显微镜 离子束 电子显微镜 电子 接口(物质) 光电子学 光学 透射电子显微镜 梁(结构) 扫描透射电子显微镜 化学 物理 复合材料 计算机科学 有机化学 人工智能 量子力学 毛细管数 毛细管作用
作者
Francesca Santoro,Wenting Zhao,Lydia‐Marie Joubert,Liting Duan,Jan Schnitker,Yoeri van de Burgt,Hsin-Ya Lou,Bofei Liu,Alberto Salleo,Lifeng Cui,Yi Cui,Bianxiao Cui
出处
期刊:ACS Nano [American Chemical Society]
卷期号:11 (8): 8320-8328 被引量:161
标识
DOI:10.1021/acsnano.7b03494
摘要

The interface between cells and nonbiological surfaces regulates cell attachment, chronic tissue responses, and ultimately the success of medical implants or biosensors. Clinical and laboratory studies show that topological features of the surface profoundly influence cellular responses; for example, titanium surfaces with nano- and microtopographical structures enhance osteoblast attachment and host–implant integration as compared to a smooth surface. To understand how cells and tissues respond to different topographical features, it is of critical importance to directly visualize the cell–material interface at the relevant nanometer length scale. Here, we present a method for in situ examination of the cell-to-material interface at any desired location, based on focused ion beam milling and scanning electron microscopy imaging to resolve the cell membrane-to-material interface with 10 nm resolution. By examining how cell membranes interact with topographical features such as nanoscale protrusions or invaginations, we discovered that the cell membrane readily deforms inward and wraps around protruding structures, but hardly deforms outward to contour invaginating structures. This asymmetric membrane response (inward vs outward deformation) causes the cleft width between the cell membrane and the nanostructure surface to vary by more than an order of magnitude. Our results suggest that surface topology is a crucial consideration for the development of medical implants or biosensors whose performances are strongly influenced by the cell-to-material interface. We anticipate that the method can be used to explore the direct interaction of cells/tissue with medical devices such as metal implants in the future.

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