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气道平滑肌细胞:研究酶活性位点的氨基酸多样性。

ASMC: investigating the amino acid diversity of enzyme active sites.

作者信息

Bailly Thomas, Elisée Eddy, Vallenet David

机构信息

LABGeM, Génomique Métabolique, Genoscope, Institut François Jacob, CEA, CNRS, Université Evry, Université Paris-Saclay, 91057 Evry, France.

出版信息

Bioinformatics. 2025 Jun 2;41(6). doi: 10.1093/bioinformatics/btaf307.

Abstract

MOTIVATION

The analysis of enzyme active sites is essential for understanding their activity in terms of catalyzed reaction and substrate specificity, providing insights for engineering to obtain targeted properties or modify the substrate scope. In 2010, a first version of the Active Site Modeling and Clustering (ASMC) workflow was published. ASMC predicts isofunctional clusters from enzyme families, based on structural modeling and clustering of active sites. Since then, structure- and sequence-based methods have developed considerably.

RESULTS

We present here a redesign of the ASMC workflow. This new major version includes recent pocket prediction, structural alignment and clustering methods, as well as a refined amino acid distance matrix, thereby improving the relevance of results and reducing the need for laborious manual analysis to obtain relevant clusters. In addition, we have implemented multiple sequence alignment as a possible input for the clustering step, along with an additional script to compare 2D and 3D active sites. Finally, the code has been unified from three to one programming language (Python) to facilitate its installation and maintenance. This new version of ASMC was evaluated on a set of protein families, resulting in overall better performances compared to its original version.

AVAILABILITY AND IMPLEMENTATION

ASMC is supported on Linux operating system and freely available at https://github.com/labgem/ASMC, along with a complete documentation (wiki, tutorial).

摘要

动机

对酶活性位点进行分析对于从催化反应和底物特异性方面理解其活性至关重要,可为工程设计提供见解,以获得靶向特性或改变底物范围。2010年,发布了活性位点建模与聚类(ASMC)工作流程的首个版本。ASMC基于活性位点的结构建模和聚类,从酶家族中预测同功能簇。从那时起,基于结构和序列的方法有了很大发展。

结果

我们在此展示了ASMC工作流程的重新设计。这个新的主要版本包括了最新的口袋预测、结构比对和聚类方法,以及一个经过改进的氨基酸距离矩阵,从而提高了结果的相关性,并减少了为获得相关簇而进行费力的手动分析的需求。此外,我们已将多序列比对作为聚类步骤的一种可能输入方式,并添加了一个用于比较二维和三维活性位点的脚本。最后,代码已从三种编程语言统一为一种(Python),以方便其安装和维护。在一组蛋白质家族上对ASMC的这个新版本进行了评估,与原始版本相比,整体性能更佳。

可用性与实现

ASMC在Linux操作系统上得到支持,可在https://github.com/labgem/ASMC上免费获取,同时还提供完整的文档(维基、教程)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2c35/12133276/ed802a1310e5/btaf307f1.jpg

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