Python(编程语言)
源代码
计算机科学
成对比较
钥匙(锁)
变构调节
功能(生物学)
R包
编码(集合论)
数据挖掘
理论计算机科学
计算生物学
人工智能
生物
程序设计语言
遗传学
受体
集合(抽象数据类型)
计算机安全
作者
Mustafa Tekpinar,Bertrand Néron,Marc Delarue
标识
DOI:10.1021/acs.jcim.1c00742
摘要
Extracting dynamical pairwise correlations and identifying key residues from large molecular dynamics trajectories or normal-mode analysis of coarse-grained models are important for explaining various processes like ligand binding, mutational effects, and long-distance interactions. Efficient and flexible tools to perform this task can provide new insights about residues involved in allosteric regulation and protein function. In addition, combining and comparing dynamical coupling information with sequence coevolution data can help to understand better protein function. To this aim, we developed a Python package called correlationplus to calculate, visualize, and analyze pairwise correlations. In this way, the package aids to identify key residues and interactions in proteins. The source code of correlationplus is available under LGPL version 3 at https://github.com/tekpinar/correlationplus. The current version of the package (0.2.0) can be installed with common installation methods like conda or pip in addition to source code installation. Moreover, docker images are also available for usage of the code without installation.
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