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Profiling of ubiquitin-like modifications reveals features of mitotic control

机译:泛素样修饰的分析揭示了有丝分裂控制的特征

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摘要

Ubiquitin and ubiquitin-like (Ubl) protein modifications affect protein stability, activity, and localization, but we still lack broad understanding of the functions of Ubl modifications. We have profiled the protein targets of ubiquitin and six additional Ubls in mitosis using a functional assay that utilizes active mammalian cell extracts and protein microarrays and identified 1,500 potential substrates; 80-200 protein targets were exclusive to each Ubl. The network structure is nonrandom, with most targets mapping to a single Ubl. There are distinct molecular functions for each Ubl, suggesting divergent biological roles. Analysis of differential profiles between mitosis and G1 highlighted a previously underappreciated role for the Ubl, FAT10, in mitotic regulation. In addition to its role as a resource for Ubl modifications, our study provides a systematic approach to analyze changes in posttranslational modifications at various cellular states.
机译:泛素和类泛素(Ubl)蛋白质修饰会影响蛋白质的稳定性,活性和定位,但我们仍然对Ubl修饰的功能缺乏广泛的了解。我们利用功能性测定法,利用了活跃的哺乳动物细胞提取物和蛋白质微阵列,分析了泛素和六个其他Ubls在有丝分裂中的蛋白质靶标,并确定了1,500种潜在底物。每个Ubl都排斥80-200个蛋白质靶标。网络结构是非随机的,大多数目标都映射到单个Ubl。每个Ubl具有不同的分子功能,表明生物学作用不同。分析有丝分裂和G1之间的差异概况,突显了Ubl FAT10在有丝分裂调控中的作用先前未被充分认识。除了其作为Ubl修饰的资源以外,我们的研究还提供了一种系统的方法来分析各种细胞状态下翻译后修饰的变化。

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