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A theoretical and experimental approach toward the development of affinity adsorbents for GFP and GFP-fusion proteins purification

机译:开发用于GFP和GFP融合蛋白的亲和吸附剂的理论和实验方法

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摘要

The green fluorescent protein (GFP) is widely employed to report on a variety of molecular phenomena, but its selective recovery is hampered by the lack of a low-cost and robust purification alternative. This work reports an integrated approach combining rational design and experimental validation toward the optimization of a small fully-synthetic ligand for GFP purification. A total of 56 affinity ligands based on a first-generation lead structure were rationally designed through molecular modeling protocols. The library of ligands was further synthesized by solid-phase combinatorial methods based on the Ugi reaction and screened against Escherichia coli extracts containing GFP. Ligands A4C2, A5C5 and A5C6 emerged as the new lead structures based on the high estimated theoretical affinity constants and the high GFP binding percentages and enrichment factors. The elution of GFP from these adsorbents was further characterized, where the best compromise between mild elution conditions, yield and purity was found for ligands A5C5 and A5C6. These were tested for purifying a model GFP-fusion protein, where ligand A5C5 yielded higher protein recovery and purity. The molecular interactions between the lead ligands and GFP were further assessed by molecular dynamics simulations, showing a wide range of potential hydrophobic and hydrogen-bond interactions. (C) 2014 Elsevier B. V. All rights reserved.
机译:绿色荧光蛋白(GFP)被广泛用于报告各种分子现象,但是由于缺乏低成本和强大的纯化替代品,其选择性回收受到了阻碍。这项工作报告了一种综合的方法,将合理的设计和实验验证相结合,以优化用于GFP纯化的小的完全合成配体。通过分子建模方案合理设计了总共56个基于第一代前导结构的亲和配体。基于Ugi反应,通过固相组合方法进一步合成了配体文库,并针对含有GFP的大肠杆菌提取物进行了筛选。基于高估计的理论亲和常数以及高GFP结合百分比和富集因子,配体A4C2,A5C5和A5C6成为新的先导结构。进一步表征了从这些吸附剂中洗脱GFP的情况,其中发现在适度洗脱条件,收率和纯度之间最佳的平衡是针对配体A5C5和A5C6。测试了这些蛋白以纯化模型GFP融合蛋白,其中配体A5C5产生更高的蛋白回收率和纯度。通过分子动力学模拟进一步评估了铅配体与GFP之间的分子相互作用,显示出广泛的潜在疏水和氢键相互作用。 (C)2014 Elsevier B. V.保留所有权利。

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