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IIIDB: a database for isoform-isoform interactions and isoform network modules

机译:IIIDB:用于异构体-异构体相互作用和异构体网络模块的数据库

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Background Protein-protein interactions (PPIs) are key to understanding diverse cellular processes and disease mechanisms. However, current PPI databases only provide low-resolution knowledge of PPIs, in the sense that "proteins" of currently known PPIs generally refer to "genes." It is known that alternative splicing often impacts PPI by either directly affecting protein interacting domains, or by indirectly impacting other domains, which, in turn, impacts the PPI binding. Thus, proteins translated from different isoforms of the same gene can have different interaction partners. Results Due to the limitations of current experimental capacities, little data is available for PPIs at the resolution of isoforms, although such high-resolution data is crucial to map pathways and to understand protein functions. In fact, alternative splicing can often change the internal structure of a pathway by rearranging specific PPIs. To fill the gap, we systematically predicted genome-wide isoform-isoform interactions (IIIs) using RNA-seq datasets, domain-domain interaction and PPIs. Furthermore, we constructed an III database (IIIDB) that is a resource for studying PPIs at isoform resolution. To discover functional modules in the III network, we performed III network clustering, and then obtained 1025 isoform modules. To evaluate the module functionality, we performed the GO/pathway enrichment analysis for each isoform module. Conclusions The IIIDB provides predictions of human protein-protein interactions at the high resolution of transcript isoforms that can facilitate detailed understanding of protein functions and biological pathways. The web interface allows users to search for IIIs or III network modules. The IIIDB is freely available at http://syslab.nchu.edu.tw/IIIDB .
机译:背景技术蛋白质-蛋白质相互作用(PPI)是了解多种细胞过程和疾病机制的关键。但是,就目前已知的PPI的“蛋白质”通常指“基因”的意义而言,当前的PPI数据库仅提供有关PPI的低分辨率知识。众所周知,选择性剪接通常通过直接影响蛋白质相互作用域或间接影响其他域而影响PPI,这反过来又影响PPI结合。因此,从同一基因的不同同工型翻译的蛋白质可以具有不同的相互作用伴侣。结果由于当前实验能力的限制,在异构体的分辨率下,PPI的数据很少,尽管此类高分辨率数据对于绘制途径和理解蛋白质功能至关重要。实际上,替代剪接通常可以通过重新排列特定的PPI来改变路径的内部结构。为了填补空白,我们使用RNA-seq数据集,域-域相互作用和PPI系统预测了全基因组范围的亚型-亚型的相互作用。此外,我们构建了III数据库(IIIDB),该数据库可用于以同工型分辨率研究PPI。为了发现III网络中的功能模块,我们进行了III网络聚类,然后获得1025个异构体模块。为了评估模块功能,我们对每个同工型模块进行了GO /途径富集分析。结论IIIDB在高分辨率的转录本亚型上提供了人类蛋白质-蛋白质相互作用的预测,可以促进对蛋白质功能和生物学途径的详细了解。 Web界面允许用户搜索III或III网络模块。 IIIDB可从http://syslab.nchu.edu.tw/IIIDB免费获得。

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