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仿生分段型聚氨酯的合成及其作为抗污生物材料的应用。

Synthesis of biomimetic segmented polyurethanes as antifouling biomaterials.

机构信息

Department of Chemistry, Sapienza University of Rome, Piazzale Aldo Moro, 5, 00185 Rome, Italy.

出版信息

Acta Biomater. 2012 Feb;8(2):549-58. doi: 10.1016/j.actbio.2011.10.024. Epub 2011 Oct 22.

DOI:10.1016/j.actbio.2011.10.024
PMID:22051237
Abstract

Controlling the non-specific adsorption of proteins, cells and bacteria onto biomaterial surfaces is of crucial importance for the development of medical devices with specific levels of performance. Among the strategies pursued to control the interactions between material surfaces and biological tissues, the immobilization of non-fouling polymers on biomaterial surfaces as well as the synthesis of the so-called biomimetic polymers are considered promising approaches to elicit specific cellular responses. In this study, in order to obtain materials able to prevent infectious and thrombotic complications related to the use of blood-contacting medical devices, heparin-mimetic segmented polyurethanes were synthesized and fully characterized. Specifically, sulfate or sulfamate groups, known to be responsible for the biological activity of heparin, were introduced into the side chain of a carboxylated polyurethane. Due to the introduction of these groups, the obtained polymers possessed a higher hard/soft phase segregation (lower glass transition temperatures) and a greater hydrophilicity than the pristine polymer. In addition, the synthesized polymers were able to significantly delay the activated partial thromboplastin time, this increased hemocompatibility being related both to polymer hydrophilicity and to the presence of the -SO3H groups. This last feature was also responsible for the ability of these biomimetic polymers to prevent the adhesion of a strain of Staphylococcus epidermidis.

摘要

控制蛋白质、细胞和细菌在生物材料表面的非特异性吸附对于开发具有特定性能水平的医疗设备至关重要。在控制材料表面与生物组织之间相互作用的策略中,将抗污聚合物固定在生物材料表面以及合成所谓的仿生聚合物被认为是引发特定细胞反应的有前途的方法。在这项研究中,为了获得能够防止与使用接触血液的医疗设备相关的感染和血栓并发症的材料,合成并充分表征了肝素模拟的嵌段型聚氨酯。具体而言,已知负责肝素生物活性的硫酸酯或磺酸盐基团被引入到羧酸化聚氨酯的侧链中。由于这些基团的引入,所得聚合物具有更高的硬/软相分离(更低的玻璃化转变温度)和更高的亲水性,比原始聚合物更高。此外,合成的聚合物能够显著延长激活部分凝血活酶时间,这种增加的血液相容性与聚合物的亲水性以及-SO3H 基团的存在有关。后一特性还使这些仿生聚合物能够防止表皮葡萄球菌菌株的黏附。

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