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Platinum: a database of experimentally measured effects of mutations on structurally defined protein–ligand complexes

机译:铂:通过实验测量的突变对结构定义的蛋白质-配体复合物影响的数据库

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摘要

Drug resistance is a major challenge for the treatment of many diseases and a significant concern throughout the drug development process. The ability to understand and predict the effects of mutations on protein–ligand affinities and their roles in the emergence of resistance would significantly aid treatment and drug design strategies. In order to study and understand the impacts of missense mutations on the interaction of ligands with the proteome, we have developed Platinum (http://structure.bioc.cam.ac.uk/platinum). This manually curated, literature-derived database, comprising over 1000 mutations, associates for the first time experimental information on changes in affinity with three-dimensional structures of protein–ligand complexes. To minimize differences arising from experimental techniques and to directly compare binding affinities, Platinum considers only changes measured by the same group and with the same amino-acid sequence used for structure determination, providing a direct link between protein structure, how a ligand binds and how mutations alter the affinity of the ligand of the protein. We believe Platinum will be an invaluable resource for understanding the effects of mutations that give rise to drug resistance, a major problem emerging in pandemics including those caused by the influenza virus, in infectious diseases such as tuberculosis, in cancer and in many other life-threatening illnesses.
机译:耐药性是治疗许多疾病的主要挑战,也是整个药物开发过程中的重大关注。了解和预测突变对蛋白质-配体亲和力的影响及其在耐药性产生中的作用的能力将大大有助于治疗和药物设计策略。为了研究和理解错义突变对配体与蛋白质组相互作用的影响,我们开发了Platinum(http://structure.bioc.cam.ac.uk/platinum)。这个由人工整理的,源自文献的数据库,包括1000多个突变,首次将有关配体与蛋白质-配体复合物三维结构亲和力变化的实验信息相关联。为了最大程度地减少实验技术产生的差异并直接比较结合亲和力,Platinum仅考虑由相同的基团和具有相同氨基酸序列(用于结构确定)测量的变化,从而提供蛋白质结构,配体如何结合以及如何之间的直接联系。突变会改变蛋白质配体的亲和力。我们认为,铂金将是了解引起耐药性的突变的影响的宝贵资源,这是在大流行中出现的主要问题,包括由流感病毒引起的大流行,在结核病等传染性疾病中,在癌症以及许多其他生活中,威胁疾病。

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