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Self-Assembled Monolayer-Based Surface Modification of Stainless Steel for Oriented Antibody Immobilization: Towards Improved Stent Biocompatibility.

机译:自组装基于单层的不锈钢表面修饰的定向抗体固定化:改善支架生物相容性。

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摘要

Stenting is a common surgical procedure for the widening of arteries narrowed by atherosclerosis. The stent is an expandable cylindrical scaffold that is implanted within the lumen of arteries and is commonly constructed from stainless steel. Despite the benefits of stenting, post-stent re-narrowing of arteries due to neointimal hyperplasia and biocompatibility associated challenges continues to limit the efficacy of bare metal stents. In order to mitigate these problems, drug-eluting stents have been developed to pharmaceutically interrupt these processes. While successful, concerns regarding late stent thrombosis and delayed healing continue to surround this drug-based approach. The primary objective of this thesis is the development of a proof-of-concept stainless steel coating that could eventually be applied to stent technology for the reduction of neointima formation and stent surface fouling for improved healing and decreased use of therapeutic agents. The overall approach attempts to covalently attach oriented antibodies to 316L stainless steel surfaces through a crosslinking self-assembled monolayer (SAM). The employed linker for SAM formation, termed TUBTS, is a novel silane recently developed by our research group. It is a bifunctional molecule that bears a trichlorosilyl anchoring group and a thiol-reactive head function. The antibody of interest is one capable of binding endothelial progenitor cells (EPCs). Attachment of these cells to the stent surface confers the antifouling properties to the coating as these cells have been found to participate in the re-endothelialization of damaged arterial vessels and the inhibition of neointima formation. Successful cell attachment requires the antibodies to be properly oriented on the SAM surface. To meet this requirement, the antibodies were modified with a thiol moiety opposite to the paratope such that the thiol reactivity of TUBTS could be used to orient the antibody as it is immobilized to the SAM. TUBTS SAMs were successfully formed on steel and used to immobilize intact antibodies and their Fab' fragments. While covalent attachment could not be directly proven, the immobilized proteins were found to be strongly bound and both the intact antibodies and Fab' fragments were shown to retain their antigen binding capabilities upon immobilization. Another key finding was the observation that the Fab' fragment strategy would constitute a preferential option to that involving intact antibodies when considered in the context of in vivo capture of EPCs in stent applications. From the foundational work presented here, EPC binding to both forms of biofunctionalized TUBTS-modified steel surfaces is now being investigated. In anticipation of potential problems in this on-going work, a strategy for increasing the spacing between the TUBTS-modified surface and immobilized Fab' fragments is also presented alongside suggested methods for assessing the mode of Fab fragment attachment.
机译:支架置入术是使动脉粥样硬化狭窄的动脉变宽的常见手术方法。支架是植入动脉腔内的可扩张的圆柱形支架,通常由不锈钢制成。尽管有支架置入术的好处,但由于新内膜增生和与生物相容性相关的挑战,支架后动脉再狭窄进一步限制了裸金属支架的疗效。为了减轻这些问题,已经开发了药物洗脱支架以药学上中断这些过程。虽然成功,但有关晚期支架内血栓形成和延迟愈合的担忧仍围绕着这种基于药物的方法。本论文的主要目的是开发一种概念验证的不锈钢涂层,该涂层最终可用于支架技术,以减少新内膜形成和支架表面结垢,从而改善治疗效果并减少治疗剂的使用。整体方法试图通过交联自组装单层(SAM)将定向抗体共价连接到316L不锈钢表面。用于SAM形成的连接子称为TUBTS,是我们研究小组最近开发的新型硅烷。它是具有三氯甲硅烷基锚定基团和硫醇反应性头基功能的双功能分子。目的抗体是一种能够结合内皮祖细胞(EPC)的抗体。这些细胞附着于支架表面赋予了涂层防污性能,因为已发现这些细胞参与受损动脉血管的再内皮化和新内膜形成的抑制。成功的细胞附着需要抗体在SAM表面正确定向。为了满足该要求,用与互补位相反的巯基部分修饰抗体,使得当将抗体固定在SAM上时,TUBTS的巯基反应性可用于定向抗体。 TUBTS SAM成功地在钢上形成,并用于固定完整的抗体及其Fab'片段。虽然不能直接证明共价结合,但是发现固定的蛋白质被牢固地结合,并且完整的抗体和Fab'片段均显示出在固定后保留其抗原结合能力。另一个关键发现是观察到,在支架应用中体内捕获EPC的情况下,Fab'片段策略将比涉及完整抗体的策略构成优先选择。通过此处介绍的基础工作,现在正在研究EPC与两种形式的生物功能化TUBTS改性钢表面的结合。为了预期这项正在进行的工作中可能存在的问题,还提出了一种增加TUBTS修饰的表面和固定化Fab'片段之间间隔的策略,以及用于评估Fab片段附着方式的建议方法。

著录项

  • 作者

    Benvenuto, Pasquale.;

  • 作者单位

    University of Toronto (Canada).;

  • 授予单位 University of Toronto (Canada).;
  • 学科 Biomedical engineering.;Inorganic chemistry.
  • 学位 Ph.D.
  • 年度 2015
  • 页码 208 p.
  • 总页数 208
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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