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金刚石表面改性对生物分子粘附的影响。

Effect by Diamond Surface Modification on Biomolecular Adhesion.

作者信息

Tian Yuan, Larsson Karin

机构信息

Department of Chemistry-Ångström Laboratory, Uppsala University, BOX 538, 75121 Uppsala, Sweden.

出版信息

Materials (Basel). 2019 Mar 15;12(6):865. doi: 10.3390/ma12060865.

Abstract

Diamond, as material, show very attractive properties. They include superior electronic properties (when doped), chemical inertness, controllable surface termination, and biocompatibility. It is thus clear that surface termination is very important for those applications where the implant material is based on diamond. The present theoretical work has focused on the effect of diamond surface termination, in combination with type of surface plane, on the adhesion of important biomolecules for vascularization and bone regeneration. These biomolecules include Arginine-Glycine-Aspartic acid (RGD), Chitosan, Heparin, Bone Morphogenetic Protein 2 (BMP2), Angiopoietin 1 (AGP1), Fibronectin and Vascular Endothelial Growth Factor (VEGF). The various surface planes are diamond diamond (100)-2x1 and (111). The theoretical results show that the non-covalent binding of these biomolecules is in proportion with their molecular weights. Moreover, three groups of biomolecules were observed for both types of surface planes. The most strongly binding biomolecule was the BMP2 molecule. The smaller polypeptides (RGD, Chitosan and Heparin) formed a less strongly binding group. Finally, the biomolecules VEGF, Fibronectin and Angiopoietin showed bond strengths numerically in between the other two groups (thereby forming a third group). Moreover, the (111) surface was generally observed to display a stronger bonding of the biomolecules, as compared with the (100)-2x1 surface.

摘要

作为一种材料,钻石具有非常吸引人的特性。这些特性包括卓越的电子性能(掺杂时)、化学惰性、可控的表面终止以及生物相容性。因此很明显,对于基于钻石的植入材料的那些应用而言,表面终止非常重要。目前的理论研究集中在钻石表面终止与表面平面类型相结合,对血管生成和骨再生的重要生物分子的粘附作用上。这些生物分子包括精氨酸 - 甘氨酸 - 天冬氨酸(RGD)、壳聚糖、肝素、骨形态发生蛋白2(BMP2)、血管生成素1(AGP1)、纤连蛋白和血管内皮生长因子(VEGF)。各种表面平面为钻石(100)-2x1和(111)。理论结果表明,这些生物分子的非共价结合与其分子量成正比。此外,对于两种类型的表面平面都观察到了三组生物分子。结合最强的生物分子是BMP2分子。较小的多肽(RGD、壳聚糖和肝素)形成了结合较弱的一组。最后,生物分子VEGF、纤连蛋白和血管生成素显示出的结合强度在数值上介于其他两组之间(从而形成第三组)。此外,与(100)-2x1表面相比,通常观察到(111)表面对生物分子的结合更强。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/48e8/6471043/b93422a4ffc3/materials-12-00865-g001.jpg

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