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基于蛋白质结构域三维形状的分类(CPD3DS)。

Classification of protein domains based on their three-dimensional shapes (CPD3DS).

作者信息

Yang Zhaochang, Liu Mingkang, Wang Bin, Wang Beibei

机构信息

School of Life Science and Technology, University of Electronic Science and Technology of China, China.

School of Information and Software Engineering, University of Electronic Science and Technology of China, China.

出版信息

Synth Syst Biotechnol. 2021 Sep 8;6(3):224-230. doi: 10.1016/j.synbio.2021.08.003. eCollection 2021 Sep.

Abstract

Protein design has become a powerful method to expand the number of natural proteins and design customized proteins according to demands. Domain-based protein design spares the need to create novel elements from scratch, which makes it a more efficient strategy than scratch-based protein design in designing multi-domain proteins, protein complexes and biomaterials. As the surface shape plays a central role in domain-domain and protein-protein interactions, a global map of the surface shapes of all domains should be very beneficial for domain-based protein design. Therefore, in this study, we characterized the surface shapes of protein domains, collected from CATH and SCOP databases, with their 3D-Zernike descriptors (3DZDs). Then similarities of domain shape features were identified, and all domains were classified accordingly. The preferences of the combinations of domains between different clusters were analyzed in natural proteins from the Protein Data Bank. A user-friendly website, termed CPD3DS, was also developed for storage, retrieval, analyses and visualization of our results. This work not only provides an overall view of protein domain shapes by showing their variety and similarities, but also opens up a new avenue to understand the properties of protein structural domains, and design principles of protein architectures.

摘要

蛋白质设计已成为一种强大的方法,可用于增加天然蛋白质的数量并根据需求设计定制蛋白质。基于结构域的蛋白质设计无需从头创建新的元件,这使得它在设计多结构域蛋白质、蛋白质复合物和生物材料方面比从头开始的蛋白质设计更有效。由于表面形状在结构域-结构域和蛋白质-蛋白质相互作用中起着核心作用,所有结构域表面形状的全局图谱对于基于结构域的蛋白质设计应该非常有帮助。因此,在本研究中,我们用其三维泽尼克描述符(3DZD)对从CATH和SCOP数据库收集的蛋白质结构域的表面形状进行了表征。然后确定了结构域形状特征的相似性,并据此对所有结构域进行了分类。分析了来自蛋白质数据库的天然蛋白质中不同簇之间结构域组合的偏好。还开发了一个名为CPD3DS的用户友好型网站,用于存储、检索、分析和可视化我们的结果。这项工作不仅通过展示蛋白质结构域形状的多样性和相似性提供了一个整体视图,还开辟了一条理解蛋白质结构域特性和蛋白质结构设计原则的新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a427/8429105/695efd939709/gr1.jpg

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