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Incorporation of a Clot-Binding Peptide into Polythiophene: Properties of Composites for Biomedical Applications

机译:凝结结合肽掺入聚噻吩:生物医学应用复合材料的性能

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Biocomposites formed by a pentapeptide (CREKA), which recognizes clotted plasma proteins, entrapped into the poly(3,4-ethylenedioxythiophene) (PEDOT) matrix have been prepared using three very different procedures. X-ray photoelectron spectroscopy analyses indicate that PEDOT-CREKA films, prepared by chronoamperom- etry in basic aqueous solution (pH = 10.3) and deposited onto a PEDOT internal layer, present the higher concentration of peptide: one CREKA molecule per six polymer repeat units. The surface of this bilayered system shows numerous folds homogeneously distributed, which have been exhaustively characterized by scanning electron microscopy and atomic force microscopy. Indeed, the morphology and topography of such bilayered films is completely different from those of biocomposite-prepared acid aqueous and organic solutions as polymerization media. The impact of the entrapped peptide molecules in the electrochemical properties of the conducting polymer has been found to be practically negligible. In contrast, biocompatibility assays with two different cellular lines indicate that PEDOT-CREKA favors cellular proliferation, which has been attributed to the binding of the peptide to the fibrin molecules from the serum used as a supplement in the culture medium. The latter assumption has been corroborated examining the ability of PEDOT-CREKA to bind fibrin. The latter ability has been also used to explore an alternative strategy based on the treatment of PEDOT-CREKA with fibrin to promote cell attachment and growth. Overall, the results suggest that PEDOT-CREKA is appropriated for multiple biomedical applications combining the electrochemical properties of conducting polymer and the ability of the peptide to recognize and bind proteins.
机译:由五肽(CREKA)形成的生物复合物可以识别截留的血浆蛋白,并被困在聚(3,4-乙撑二氧噻吩)(PEDOT)基质中,已使用三种截然不同的方法制备。 X射线光电子能谱分析表明,通过计时安培法在碱性水溶液(pH = 10.3)中沉积并沉积到PEDOT内层上的PEDOT-CREKA膜呈现出更高的肽浓度:每六个聚合物重复单元一个CREKA分子。 。该双层系统的表面显示出许多均匀分布的褶皱,已通过扫描电子显微镜和原子力显微镜详尽地表征了这些褶皱。实际上,这种双层膜的形态和形貌与生物复合制备的酸性水溶液和有机溶液作为聚合介质完全不同。已经发现,被包裹的肽分子对导电聚合物的电化学性能的影响实际上是可以忽略的。相反,具有两种不同细胞系的生物相容性分析表明,PEDOT-CREKA有利于细胞增殖,这归因于多肽与血清中作为补充剂的血清中纤维蛋白分子的结合。检验PEDOT-CREKA结合血纤蛋白的能力已证实了后者的假设。后者的功能也已被用于探索基于血纤蛋白治疗PEDOT-CREKA的替代策略,以促进细胞附着和生长。总体而言,结果表明,PEDOT-CREKA适用于多种生物医学应用,其结合了导电聚合物的电化学特性以及该肽识别和结合蛋白质的能力。

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