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首页> 外文期刊>Journal of biomedical materials research, Part A >Student award for outstanding research winner in the Ph.D. category for the 2017 society for biomaterials annual meeting and exposition, april 5–8, 2017, Minneapolis, Minnesota: Characterization of protein interactions with molecularly imprinted hydrogels that possess engineered affinity for high isoelectric point biomarkers
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Student award for outstanding research winner in the Ph.D. category for the 2017 society for biomaterials annual meeting and exposition, april 5–8, 2017, Minneapolis, Minnesota: Characterization of protein interactions with molecularly imprinted hydrogels that possess engineered affinity for high isoelectric point biomarkers

机译:博士学位的杰出研究获奖者的学生奖。 2017年生物材料社会的类别年会和博览会,2017年4月5日至8日,明尼阿波利斯,明尼苏达州:与分子印迹水凝胶的蛋白质相互作用具有对高等电点生物标志物的工程亲和力的表征

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Abstract Molecularly imprinted polymers (MIPs) with selective affinity for protein biomarkers could find extensive utility as environmentally robust, cost‐efficient biomaterials for diagnostic and therapeutic applications. In order to develop recognitive, synthetic biomaterials for prohibitively expensive protein biomarkers, we have developed a molecular imprinting technique that utilizes structurally similar, analogue proteins. Hydrogel microparticles synthesized by molecular imprinting with trypsin, lysozyme, and cytochrome c possessed an increased affinity for alternate high isoelectric point biomarkers both in isolation and plasma‐mimicking adsorption conditions. Imprinted and non‐imprinted P(MAA‐co‐AAm‐co‐DEAEMA) microgels containing PMAO‐PEGMA functionalized polycaprolactone nanoparticles were net‐anionic, polydisperse, and irregularly shaped. MIPs and control non‐imprinted polymers (NIPs) exhibited regions of Freundlich and BET isotherm adsorption behavior in a range of non‐competitive protein solutions, where MIPs exhibited enhanced adsorption capacity in the Freundlich isotherm regions. In a competitive condition, imprinting with analogue templates (trypsin, lysozyme) increased the adsorption capacity of microgels for cytochrome c by 162% and 219%, respectively, as compared to a 122% increase provided by traditional bulk imprinting with cytochrome c. Our results suggest that molecular imprinting with analogue protein templates is a viable synthetic strategy for enhancing hydrogel‐biomarker affinity and promoting specific protein adsorption behavior in biological fluids. ? 2017 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 105A: 1565–1574, 2017.
机译:摘要分子印迹聚合物(MIPS)对蛋白质生物标志物的选择性亲和力可以发现广泛的效用,以适应环境稳健,具有成本效益的诊断和治疗应用的生物材料。为了开发识别的蛋白质生物标志物的识别性,合成生物材料,我们开发了一种利用结构相似的类似物蛋白的分子印迹技术。通过与胰蛋白酶,溶菌酶,细胞色素C的分子印迹合成的水凝胶微粒对分离和等离子体模拟的吸附条件具有增加的亲和力的亲和力。含有PMAO-PEGMA官能化聚己内酯纳米颗粒的印迹和非印记P(MAA-CO-AAM-CO-DEAMA)微凝胶是净阴离子,多分散和不规则形状的。 MIPS和控制非印记聚合物(NIPS)在一系列非竞争性蛋白质溶液中表现出Freundlich和Bet等温度吸附行为的区域,其中MIPS表现出Freundlich等温地区的增强的吸附能力。在竞争条件下,与模拟模板(胰蛋白酶,溶菌酶)的印迹分别增加了细胞色素C的微凝胶的吸附能力,分别增加了162%和219%,而通过传统体积压印与细胞色素C的传统体积增加122%。我们的研究结果表明,与类似物蛋白模板的分子印迹是一种可行的合成策略,用于增强水凝胶 - 生物标志物亲和力并促进生物流体中的特定蛋白质吸附行为。还2017年Wiley期刊,Inc。J生物保罗A部分:105A:1565-1574,2017。

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