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A multi-objective optimization approach accurately resolves protein domain architectures

机译:多目标优化方法可准确解析蛋白质结构域架构

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摘要

>Motivation: Given a protein sequence and a number of potential domains matching it, what are the domain content and the most likely domain architecture for the sequence? This problem is of fundamental importance in protein annotation, constituting one of the main steps of all predictive annotation strategies. On the other hand, when potential domains are several and in conflict because of overlapping domain boundaries, finding a solution for the problem might become difficult. An accurate prediction of the domain architecture of a multi-domain protein provides important information for function prediction, comparative genomics and molecular evolution.>Results: We developed DAMA (Domain Annotation by a Multi-objective Approach), a novel approach that identifies architectures through a multi-objective optimization algorithm combining scores of domain matches, previously observed multi-domain co-occurrence and domain overlapping. DAMA has been validated on a known benchmark dataset based on CATH structural domain assignments and on the set of Plasmodium falciparum proteins. When compared with existing tools on both datasets, it outperforms all of them.>Availability and implementation: DAMA software is implemented in C++ and the source code can be found at .>Contact: or >Supplementary information: are available at Bioinformatics online.
机译:>动机:给定一个蛋白质序列和与其匹配的许多潜在结构域,该序列的结构域内容和最可能的结构域是什么?这个问题在蛋白质注释中至关重要,是所有预测性注释策略的主要步骤之一。另一方面,当潜在域为多个且由于域边界重叠而发生冲突时,找到该问题的解决方案可能会变得困难。准确预测多域蛋白质的域结构可为功能预测,比较基因组学和分子进化提供重要信息。>结果:我们开发了DAMA(通过多目标方法进行域注释),一种新颖的方法,该方法通过多目标优化算法来识别架构,该算法结合了多个域匹配项,先前观察到的多域共现和域重叠。 DAMA已在基于CATH结构域分配和恶性疟原虫蛋白质集的已知基准数据集中进行了验证。与两个数据集上的现有工具相比,它的性能都优于所有数据。>可用性和实现:DAMA软件是用C ++实现的,其源代码可以在以下网址找到。>联系方式:或>补充信息:可在线访问生物信息学。

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