PreMLS: The undersampling technique based on ClusterCentroids to predict multiple lysine sites.

IF 3.8 2区生物学 Q1 BIOCHEMICAL RESEARCH METHODS PLoS Computational Biology Pub Date : 2024-10-22 eCollection Date: 2024-10-01 DOI:10.1371/journal.pcbi.1012544

Yun Zuo, Xingze Fang, Jiayong Wan, Wenying He, Xiangrong Liu, Xiangxiang Zeng, Zhaohong Deng

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Abstract

The translated protein undergoes a specific modification process, which involves the formation of covalent bonds on lysine residues and the attachment of small chemical moieties. The protein's fundamental physicochemical properties undergo a significant alteration. The change significantly alters the proteins' 3D structure and activity, enabling them to modulate key physiological processes. The modulation encompasses inhibiting cancer cell growth, delaying ovarian aging, regulating metabolic diseases, and ameliorating depression. Consequently, the identification and comprehension of post-translational lysine modifications hold substantial value in the realms of biological research and drug development. Post-translational modifications (PTMs) at lysine (K) sites are among the most common protein modifications. However, research on K-PTMs has been largely centered on identifying individual modification types, with a relative scarcity of balanced data analysis techniques. In this study, a classification system is developed for the prediction of concurrent multiple modifications at a single lysine residue. Initially, a well-established multi-label position-specific triad amino acid propensity algorithm is utilized for feature encoding. Subsequently, PreMLS: a novel ClusterCentroids undersampling algorithm based on MiniBatchKmeans was introduced to eliminate redundant or similar major class samples, thereby mitigating the issue of class imbalance. A convolutional neural network architecture was specifically constructed for the analysis of biological sequences to predict multiple lysine modification sites. The model, evaluated through five-fold cross-validation and independent testing, was found to significantly outperform existing models such as iMul-kSite and predML-Site. The results presented here aid in prioritizing potential lysine modification sites, facilitating subsequent biological assays and advancing pharmaceutical research. To enhance accessibility, an open-access predictive script has been crafted for the multi-label predictive model developed in this study.

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PreMLS：基于 ClusterCentroids 的欠采样技术可预测多个赖氨酸位点。

翻译后的蛋白质会经历一个特定的修饰过程，其中包括在赖氨酸残基上形成共价键和附着小的化学分子。蛋白质的基本物理化学特性会发生重大改变。这种变化极大地改变了蛋白质的三维结构和活性，使其能够调节关键的生理过程。这种调节包括抑制癌细胞生长、延缓卵巢衰老、调节代谢疾病和改善抑郁症。因此，识别和理解翻译后赖氨酸修饰在生物学研究和药物开发领域具有重要价值。赖氨酸（K）位点的翻译后修饰（PTM）是最常见的蛋白质修饰之一。然而，对 K-PTMs 的研究主要集中在识别单个修饰类型上，相对缺乏平衡的数据分析技术。本研究开发了一个分类系统，用于预测单个赖氨酸残基上并发的多种修饰。首先，利用成熟的多标签特定位置三元氨基酸倾向算法进行特征编码。随后，引入了 PreMLS：一种基于 MiniBatchKmeans 的新型 ClusterCentroids 欠采样算法，以消除冗余或相似的主要类别样本，从而缓解类别不平衡问题。专门为分析生物序列构建了一个卷积神经网络架构，以预测多个赖氨酸修饰位点。通过五倍交叉验证和独立测试对该模型进行了评估，发现其性能明显优于 iMul-kSite 和 predML-Site 等现有模型。本文介绍的结果有助于确定潜在赖氨酸修饰位点的优先次序，促进后续的生物检测并推动药物研究。为了提高可访问性，我们为本研究中开发的多标签预测模型制作了一个开放访问的预测脚本。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

PLoS Computational Biology BIOCHEMICAL RESEARCH METHODS-MATHEMATICAL & COMPUTATIONAL BIOLOGY

CiteScore

7.10

自引率

4.70%

发文量

820

审稿时长

2.5 months

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