AAclust:用于选择减少冗余的氨基酸尺度集的 k 优化聚类。

IF 2.4 Q2 MATHEMATICAL & COMPUTATIONAL BIOLOGY
Bioinformatics advances Pub Date : 2024-10-30 eCollection Date: 2024-01-01 DOI:10.1093/bioadv/vbae165
Stephan Breimann, Dmitrij Frishman
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引用次数: 0

摘要

摘要:氨基酸尺度对于基于序列的蛋白质预测任务至关重要,但目前还没有黄金标准尺度集或简单的尺度选择方法。我们开发了 AAclust,它是需要预定义簇数 k 的聚类模型(如 k-means)的包装器。AAclust 通过聚类并为每个聚类选择一个具有代表性的标度,从而获得减少冗余的标度集,其中 k 既可以由 AAclust 优化,也可以由用户定义。通过将机器学习模型应用于 24 个蛋白质基准数据集,对 AAclust 标度选择的实用性进行了评估。我们发现,每个基准数据集的最佳规模集都不尽相同,而且明显优于以往研究中使用的规模集。值得注意的是,模型的性能与标度集的大小密切相关。AAclust 能够系统地优化机器学习应用中基于规模的特征工程:AAclust算法是AAanalysis的一部分,AAanalysis是一个基于Python的框架,用于基于序列的可解释蛋白质预测,其文档和访问地址为https://aaanalysis.readthedocs.io/en/latest 和 https://github.com/breimanntools/aaanalysis。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
AAclust: k-optimized clustering for selecting redundancy-reduced sets of amino acid scales.

Summary: Amino acid scales are crucial for sequence-based protein prediction tasks, yet no gold standard scale set or simple scale selection methods exist. We developed AAclust, a wrapper for clustering models that require a pre-defined number of clusters k, such as k-means. AAclust obtains redundancy-reduced scale sets by clustering and selecting one representative scale per cluster, where k can either be optimized by AAclust or defined by the user. The utility of AAclust scale selections was assessed by applying machine learning models to 24 protein benchmark datasets. We found that top-performing scale sets were different for each benchmark dataset and significantly outperformed scale sets used in previous studies. Noteworthy is the strong dependence of the model performance on the scale set size. AAclust enables a systematic optimization of scale-based feature engineering in machine learning applications.

Availability and implementation: The AAclust algorithm is part of AAanalysis, a Python-based framework for interpretable sequence-based protein prediction, which is documented and accessible at https://aaanalysis.readthedocs.io/en/latest and https://github.com/breimanntools/aaanalysis.

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CiteScore
1.60
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