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A fly view of a SUMO-targeted ubiquitin ligase

机译:靶向SUMO的泛素连接酶的示意图

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Posttranscriptional modifications of proteins by the ubiquitin and SUMO (Small Ubiquitin-related Modifier) pathways regulate the function of protein networks, enable cells to respond to signaling cues during development, and to cope with the changing environment during adult life. Both modifications can impact protein stability, localization, protein-protein interactions and/or function. While both pathways have been well studied individually, the long-speculated nature of crosstalk between SUMO and ubiquitin pathways has been molecularly enigmatic. Recent work in yeast and mammalian cells identified the connection between the two pathways in the form of a conserved family of RING finger ubiquitin ligases termed SUMO-Targeted ubiquitin ligases (STUbLs). These proteins bind to SUMOylated substrates via their SUMO interaction motif and subsequently target them for ubiquitylation. Characterization of Degringolade (Dgrn), a STUbL gene in the fly genome, enabled us to evaluate the contribution of STUbLs to the development of multicellular organisms. Analysis of dgrn mutants showed that they are required for cyto-nuclear organization during early embryonic development, and are likely required to cope with mitotic stress and DNA damage. Furthermore, in transcription, STUbLs regulate protein-protein interactions, and are part of the molecular machinery that regulates co-repressor choice and gene-expression selectivity during development.
机译:泛素和SUMO(小泛素相关修饰剂)途径对蛋白质进行转录后修饰,调节蛋白质网络的功能,使细胞能够响应发育过程中的信号提示,并适应成年后不断变化的环境。两种修饰均可影响蛋白质稳定性,定位,蛋白质-蛋白质相互作用和/或功能。虽然对这两种途径进行了单独的深入研究,但长久以来人们推测SUMO和泛素途径之间的串扰性质在分子上是神秘的。酵母和哺乳动物细胞中的最新研究以称为SUMO靶向的泛素连接酶(STUbLs)的RING指泛素连接酶的保守家族的形式鉴定了两种途径之间的联系。这些蛋白质通过其SUMO相互作用基序与SUMO酰化的底物结合,随后将其靶向进行泛素化。蝇中基因组中的STUbL基因Degringolade(Dgrn)的表征使我们能够评估STUbLs对多细胞生物发展的贡献。对dgrn突变体的分析表明,它们是早期胚胎发育过程中细胞核组织所必需的,并且可能是应对有丝分裂压力和DNA损伤所必需的。此外,在转录中,STUbL调节蛋白质之间的相互作用,并且是调节发育过程中共阻遏物选择和基因表达选择性的分子机制的一部分。

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