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蛋白质数据库中蛋白质-碳水化合物相互作用的系统分析。

A systematic analysis of protein-carbohydrate interactions in the Protein Data Bank.

作者信息

Cao Yiwei, Park Sang-Jun, Im Wonpil

机构信息

Departments of Biological Sciences, Chemistry, Bioengineering, and Computer Sciences and Engineering, Lehigh University, Bethlehem, PA 18015, USA.

School of Computational Sciences, Korea Institute for Advanced Study, Seoul 02455, Republic of Korea.

出版信息

Glycobiology. 2021 Feb 9;31(2):126-136. doi: 10.1093/glycob/cwaa062.

Abstract

Protein-carbohydrate interactions underlie essential biological processes. Elucidating the mechanism of protein-carbohydrate recognition is a prerequisite for modeling and optimizing protein-carbohydrate interactions, which will help in discovery of carbohydrate-derived therapeutics. In this work, we present a survey of a curated database consisting of 6,402 protein-carbohydrate complexes in the Protein Data Bank (PDB). We performed an all-against-all comparison of a subset of nonredundant binding sites, and the result indicates that the interaction pattern similarity is not completely relevant to the binding site structural similarity. Investigation of both binding site and ligand promiscuities reveals that the geometry of chemical feature points is more important than local backbone structure in determining protein-carbohydrate interactions. A further analysis on the frequency and geometry of atomic interactions shows that carbohydrate functional groups are not equally involved in binding interactions. Finally, we discuss the usefulness of protein-carbohydrate complexes in the PDB with acknowledgement that the carbohydrates in many structures are incomplete.

摘要

蛋白质与碳水化合物的相互作用是基本生物学过程的基础。阐明蛋白质与碳水化合物的识别机制是对蛋白质与碳水化合物相互作用进行建模和优化的前提条件,这将有助于发现碳水化合物衍生的治疗方法。在这项工作中,我们对蛋白质数据库(PDB)中一个由6402个蛋白质 - 碳水化合物复合物组成的精选数据库进行了综述。我们对一个非冗余结合位点子集进行了全对全比较,结果表明相互作用模式的相似性与结合位点结构的相似性并不完全相关。对结合位点和配体混杂性的研究表明,在确定蛋白质与碳水化合物的相互作用时,化学特征点的几何形状比局部主链结构更重要。对原子相互作用的频率和几何形状的进一步分析表明,碳水化合物官能团在结合相互作用中的参与程度并不相同。最后,我们讨论了PDB中蛋白质 - 碳水化合物复合物的实用性,同时承认许多结构中的碳水化合物并不完整。

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