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利用金表面的链烷硫醇自组装单分子层控制细胞在异形表面上的附着。

Controlling cell attachment on contoured surfaces with self-assembled monolayers of alkanethiolates on gold.

作者信息

Mrksich M, Chen C S, Xia Y, Dike L E, Ingber D E, Whitesides G M

机构信息

Department of Chemistry, Harvard University, Cambridge, MA 02138, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Oct 1;93(20):10775-8. doi: 10.1073/pnas.93.20.10775.

Abstract

This paper describes a method based on experimentally simple techniques--microcontact printing and micromolding in capillaries--to prepare tissue culture substrates in which both the topology and molecular structure of the interface can be controlled. The method combines optically transparent contoured surfaces with self-assembled monolayers (SAMs) of alkanethiolates on gold to control interfacial characteristics; these tailored interfaces, in turn, control the adsorption of proteins and the attachment of cells. The technique uses replica molding in poly(dimethylsiloxane) molds having micrometer-scale relief patterns on their surfaces to form a contoured film of polyurethane supported on a glass slide. Evaporation of a thin (< 12 nm) film of gold on this surface-contoured polyurethane provides an optically transparent substrate, on which SAMs of terminally functionalized alkanethiolates can be formed. In one procedure, a flat poly(dimethylsiloxane) stamp was used to form a SAM of hexadecanethiolate on the raised plateaus of the contoured surface by contact printing hexadecanethiol [HS(CH2)15CH3]; a SAM terminated in tri(ethylene glycol) groups was subsequently formed on the bare gold remaining in the grooves by immersing the substrate in a solution of a second alkanethiol [HS(CH2)11(OCH2CH2)3OH]. Then this patterned substrate was immersed in a solution of fibronectin, the protein adsorbed only on the methyl-terminated plateau regions of the substrate [the tri(ethylene glycol)-terminated regions resisted the adsorption of protein]; bovine capillary endothelial cells attached only on the regions that adsorbed fibronectin. A complementary procedure confined protein adsorption and cell attachment to the grooves in this substrate.

摘要

本文描述了一种基于实验上简单技术——微接触印刷和毛细管微成型——来制备组织培养底物的方法,该方法能够控制界面的拓扑结构和分子结构。该方法将光学透明的轮廓表面与金上的链烷硫醇自组装单分子层(SAMs)相结合以控制界面特性;这些经过定制的界面进而控制蛋白质的吸附和细胞的附着。该技术利用表面具有微米级浮雕图案的聚二甲基硅氧烷模具进行复制成型,以在载玻片上形成一层聚氨酯轮廓膜。在这种表面轮廓化的聚氨酯上蒸发一层薄(<12纳米)的金膜,可提供一个光学透明的底物,在其上可以形成末端功能化链烷硫醇的SAMs。在一个步骤中,使用一个平坦的聚二甲基硅氧烷印章通过接触印刷十六烷硫醇[HS(CH2)15CH3]在轮廓表面的凸起平台上形成十六烷硫醇盐的SAM;随后通过将底物浸入第二种链烷硫醇[HS(CH2)11(OCH2CH2)3OH]的溶液中,在凹槽中剩余的裸金上形成以三(乙二醇)基团为末端的SAM。然后将这种图案化的底物浸入纤连蛋白溶液中,蛋白质仅吸附在底物的甲基末端平台区域[三(乙二醇)末端区域抵制蛋白质的吸附];牛毛细血管内皮细胞仅附着在吸附纤连蛋白的区域。一个互补的步骤将蛋白质吸附和细胞附着限制在该底物的凹槽中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0d5/38231/433729214d73/pnas01524-0249-a.jpg

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