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通过贻贝粘蛋白的直接涂层实现糖胺聚糖的简便表面功能化。

Facile surface functionalization with glycosaminoglycans by direct coating with mussel adhesive protein.

机构信息

Department of Chemical Engineering, Pohang University of Science and Technology, Pohang, Korea.

出版信息

Tissue Eng Part C Methods. 2012 Jan;18(1):71-9. doi: 10.1089/ten.TEC.2011.0384. Epub 2011 Nov 8.

Abstract

The use of mussel adhesive proteins (MAPs) as a surface coating for cell adhesion has been suggested due to their unique properties of biocompatibility and effective adhesion on diverse inorganic and organic surfaces. The surface functionalization of scaffolds or implants using extracellular matrix (ECM) molecules is important for the enhancement of target cell behaviors such as proliferation and differentiation. In the present work, we suggest a new, simple surface functionalization platform based on the charge interactions between the positively charged MAP linker and negatively charged ECM molecules, such as glycosaminoglycans (GAGs). MAP was efficiently coated onto a titanium model surface using its adhesion ability. Then, several GAG molecules, including hyaluronic acid (HA), heparin sulfate (HS), chondroitin sulfate (CS), and dermatan sulfate (DS), were effectively immobilized on the MAP-coated surfaces by charge interactions. Using HA as a model GAG molecule, we found that the proliferation, spreading, and differentiation behaviors of mouse preosteoblast cells were all significantly improved on MAP/HA-layered titanium. In addition, we successfully constructed a multilayer film on a titanium surface with oppositely charged layer-by-layer coatings of MAP and HA. Collectively, our simple MAP-based surface functionalization strategy can be successfully used for the efficient surface immobilization of negatively charged ECM molecules in various tissue engineering and medical implantation applications.

摘要

由于贻贝类黏附蛋白 (MAPs) 具有独特的生物相容性和在各种无机和有机表面有效黏附的特性,因此有人建议将其用作细胞黏附的表面涂层。通过细胞外基质 (ECM) 分子对支架或植入物进行表面功能化对于增强靶细胞的行为(如增殖和分化)非常重要。在本工作中,我们提出了一种新的、简单的基于带正电荷的 MAP 连接子与带负电荷的 ECM 分子(如糖胺聚糖 (GAGs))之间的电荷相互作用的表面功能化平台。通过其黏附能力,MAP 可有效地涂覆在钛模型表面上。然后,通过电荷相互作用,几种 GAG 分子(包括透明质酸 (HA)、肝素硫酸盐 (HS)、硫酸软骨素 (CS) 和硫酸皮肤素 (DS))被有效地固定在 MAP 涂覆的表面上。使用 HA 作为模型 GAG 分子,我们发现 MAP/HA 层状钛上的小鼠前成骨细胞的增殖、扩展和分化行为均显著改善。此外,我们还成功地在钛表面上构建了具有相反电荷的多层膜,通过 MAP 和 HA 的层层涂层。总之,我们基于简单 MAP 的表面功能化策略可成功用于在各种组织工程和医学植入应用中有效固定带负电荷的 ECM 分子。

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