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Reconstructing the ubiquitin network - cross-talk with other systems and identification of novel functions

机译:重建泛素网络-与其他系统的串扰和新颖功能的识别

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ABSTRACT: BACKGROUND: The ubiquitin system (Ub-system) can be defined as the ensemble of components including Ub/ubiquitin-like proteins, their conjugation and deconjugation apparatus, binding partners and the proteasomal system. While several studies have concentrated on structure-function relationships and evolution of individual components of the Ub-system, a study of the system as a whole is largely lacking. RESULTS: Using numerous genome-scale datasets, we assemble for the first time a comprehensive reconstruction of the budding yeast Ub-system revealing static and dynamic properties. We devised two novel representations, the rank plot to understand the functional diversification of different components and the clique-specific point-wise mutual-information network to identify significant interactions in the Ub-system. CONCLUSIONS: Using these representations, evidence is provided for the functional diversification of components such as SUMO-dependent Ub-ligases. We also identify novel components of SCF (Skp1-cullin-F-box) -dependent complexes, receptors in the ERAD (endoplasmic reticulum associated degradation) system and a key role for Sus1 in coordinating multiple Ub-related processes in chromatin dynamics. We present evidence for a major impact of the Ub-system on large parts of the proteome via its interaction with the transcription regulatory network. Furthermore, the dynamics of the Ub-network suggests that Ub and SUMO modifications might function cooperatively with transcription control in regulating cell-cycle-stage-specific complexes and in reinforcing periodicities in gene expression. Combined with evolutionary information, the structure of this network helps in understanding the lineage-specific expansion of SCF complexes with a potential role in pathogen response and the origin of the ERAD and ESCRT systems.
机译:摘要:背景:泛素系统(Ub系统)可以定义为包括Ub /泛素样蛋白,其结合和解结合装置,结合伴侣和蛋白酶体系统在内的各种成分的集合。尽管一些研究集中在Ub系统的结构-功能关系和单个组件的演化上,但仍缺乏对整个系统的研究。结果:我们使用大量的基因组规模的数据集,第一次组装了芽的酵母Ub系统的全面重建,揭示了静态和动态特性。我们设计了两种新颖的表示形式,即用于了解不同组件功能多样化的等级图,以及用于识别Ub系统中重大交互作用的特定群体的点式互信息网络。结论:使用这些表示,提供了证据证明诸如SUMO依赖性Ub连接酶等成分的功能多样化。我们还确定了SCF(Skp1-cullin-F-box)依赖复合物,ERAD(内质网相关降解)系统中的受体和Sus1在染色质动力学中协调多个Ub相关过程的关键作用中的新型成分。我们提供了证据,证明Ub系统通过与转录调控网络的相互作用对蛋白质组的大部分产生了重大影响。此外,Ub网络的动力学表明,Ub和SUMO修饰可能与转录控制协同作用,以调节细胞周期阶段特异性复合物并增强基因表达的周期性。结合进化信息,该网络的结构有助于理解SCF复合物的谱系特异性扩展,在病原体应答以及ERAD和ESCRT系统的起源中具有潜在作用。

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