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Integration of Diverse Research Methods to Analyze and Engineer Ca2+-Binding Proteins: From Prediction to Production

机译:整合了多种研究方法来分析和工程化Ca2 +结合蛋白:从预测到生产

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摘要

In recent years, increasingly sophisticated computational and bioinformatics tools have evolved for the analyses of protein structure, function, ligand interactions, modeling and energetics. This includes the development of algorithms to recursively evaluate side-chain rotamer permutations, identify regions in a 3D structure that meet some set of search parameters, calculate and minimize energy values, and provide high-resolution visual tools for theoretical modeling. Here we discuss the interdependency between different areas of bioinformatics, the evolution of different algorithm design approaches, and finally the transition from theoretical models to real-world design and application as they relate to Ca2+-binding proteins. Within this context, it has become evident that significant pre-experimental design and calculations can be modeled through computational methods, thus eliminating potentially unproductive research and increasing our confidence in the correlation between real and theoretical models. Moving from prediction to production, it is anticipated that bioinformatics tools will play an increasingly significant role in research and development, improving our ability to both understand the physiological roles of Ca2+ and other metals and to extend that knowledge to the design of function-specific synthetic proteins capable of fulfilling different roles in medical diagnostics and therapeutics.
机译:近年来,用于分析蛋白质结构,功能,配体相互作用,建模和能量学的进化出越来越先进的计算和生物信息学工具。这包括算法开发,以递归地评估侧链旋转异构体排列,识别3D结构中满足某些搜索参数集的区域,计算并最小化能量值,并为理论建模提供高分辨率的可视化工具。在这里,我们讨论了生物信息学不同领域之间的相互依存关系,不同算法设计方法的演变,最后讨论了与Ca2 +结合蛋白相关的理论模型到实际设计和应用的过渡。在这种情况下,很明显可以通过计算方法对重要的实验前设计和计算进行建模,从而消除了潜在的无用研究,并提高了我们对真实模型与理论模型之间相关性的信心。从预测到生产,预计生物信息学工具将在研发中发挥越来越重要的作用,从而提高我们理解Ca2 +和其他金属的生理作用并将这一知识扩展到功能特定的合成材料设计的能力。能够在医学诊断和治疗中发挥不同作用的蛋白质。

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