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Recent Progress on Structural Bioinformatics Research of Cytochrome P450 and Its Impact on Drug Discovery

机译:细胞色素P450的结构生物信息学研究及其对药物发现的影响的最新进展

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摘要

Cytochrome P450 is predominantly responsible for human drug metabolism, which is of critical importance for drug discovery and development. Structural bioinformatics focuses on analysis and prediction of three-dimentional structure of biological macromolecules and elucidation of structure-function relationship as well as identification of important binding interactions. Rapid advancement of structural bioinformatics has been made over the last decade. With more information available for CYP structures, the methods of structural bioinformatics may be used in the CYP field. In this review, we demonstrate three previous studies on CYP using the methods of structural bioinformatics, including the investigation of reasons for decrease of enzymatic activity of CYP1A2 caused by a peripheral mutation, the construction of a pharmacophore model specific to active site of CYP1A2 and the prediction of the functional consequences of single residue mutation in CYP. By illustrating these studies we attempt to show the potential role of structural bioinformatics in CYP research and help better understanding the importance of structural bioinformatics in drug designing.
机译:细胞色素P450主要负责人的药物代谢,这对药物发现和开发至关重要。结构生物信息学专注于分析和预测生物大分子的三维结构,阐明结构-功能关系以及识别重要的结合相互作用。在过去的十年中,结构生物信息学得到了飞速发展。有了有关CYP结构的更多信息,结构生物信息学的方法可用于CYP领域。在这篇综述中,我们证明了以前使用结构生物信息学方法进行的有关CYP的三项研究,包括调查由外围突变引起的CYP1A2酶活性降低的原因,构建针对CYP1A2活性位点的药效团模型和CYP单残基突变的功能后果的预测。通过说明这些研究,我们试图显示结构生物信息学在CYP研究中的潜在作用,并帮助更好地理解结构生物信息学在药物设计中的重要性。

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