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MultiP-Apo: A Multilabel Predictor for Identifying Subcellular Locations of Apoptosis Proteins

机译:MultiP-APO:用于鉴定细胞凋亡蛋白的亚细胞位置的多标签预测器

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摘要

Apoptosis proteins play an important role in the mechanism of programmed cell death. Predicting subcellular localization of apoptosis proteins is an essential step to understand their functions and identify drugs target. Many computational prediction methods have been developed for apoptosis protein subcellular localization. However, these existing works only focus on the proteins that have one location; proteins with multiple locations are either not considered or assumed as not existing when constructing prediction models, so that they cannot completely predict all the locations of the apoptosis proteins with multiple locations. To address this problem, this paper proposes a novel multilabel predictor named MultiP-Apo, which can predict not only apoptosis proteins with single subcellular location but also those with multiple subcellular locations. Specifically, given a query protein, GO-based feature extraction method is used to extract its feature vector. Subsequently, the GO feature vector is classified by a new multilabel classifier based on the label-specific features. It is the first multilabel predictor ever established for identifying subcellular locations of multilocation apoptosis proteins. As an initial study, MultiP-Apo achieves an overall accuracy of 58.49% by jackknife test, which indicates that our proposed predictor may become a very useful high-throughput tool in this area.
机译:细胞凋亡蛋白在编程的细胞死亡机制中发挥着重要作用。预测细胞凋亡蛋白的亚细胞定位是了解其功能并鉴定药物靶标的基本步骤。已经开发了许多计算预测方法用于凋亡蛋白亚细胞定位。然而,这些现有的作品仅关注有一个位置的蛋白质;具有多个位置的蛋白质不考虑或假设在构建预测模型时不存在,因此它们不能完全预测具有多个位置的细胞凋亡蛋白的所有位置。为了解决这个问题,本文提出了一种名为MultiP-APO的新型多标签预测器,其可以预测具有单个亚细胞位置的细胞凋亡蛋白,而且可以预测具有多个亚细胞位置的细胞蛋白。具体地,给定查询蛋白质,基于Go的特征提取方法用于提取其特征向量。随后,Go特征向量由新的Multilabel分类器基于特定标签特征来分类。它是迄今为止用于鉴定多算子凋亡蛋白的亚细胞位置的第一兆位预测器。作为初步研究,Multip-APO通过千刀测试实现了58.49%的整体准确性,这表明我们所提出的预测器可能成为该领域非常有用的高吞吐工具。

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