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The Biology of SUMO-Targeted Ubiquitin Ligases in Drosophila Development Immunity and Cancer

机译:SUMO靶向遍在蛋白果蝇在果蝇发育免疫和癌症中的生物学。

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摘要

The ubiquitin and SUMO (small ubiquitin-like modifier) pathways modify proteins that in turn regulate diverse cellular processes, embryonic development, and adult tissue physiology. These pathways were originally discovered biochemically in vitro, leading to a long-standing challenge of elucidating both the molecular cross-talk between these pathways and their biological importance. Recent discoveries in Drosophila established that ubiquitin and SUMO pathways are interconnected via evolutionally conserved SUMO-targeted ubiquitin ligase (STUbL) proteins. STUbL are RING ubiquitin ligases that recognize SUMOylated substrates and catalyze their ubiquitination, and include Degringolade (Dgrn) in Drosophila and RNF4 and RNF111 in humans. STUbL are essential for early development of both the fly and mouse embryos. In the fly embryo, Dgrn regulates early cell cycle progression, sex determination, zygotic gene transcription, segmentation, and neurogenesis, among other processes. In the fly adult, Dgrn is required for systemic immune response to pathogens and intestinal stem cell regeneration upon infection. These functions of Dgrn are highly conserved in humans, where RNF4-dependent ubiquitination potentiates key oncoproteins, thereby accelerating tumorigenesis. Here, we review the lessons learned to date in Drosophila and highlight their relevance to cancer biology.
机译:遍在蛋白和SUMO(小的遍在蛋白样修饰剂)途径可修饰蛋白质,进而调节多种细胞过程,胚胎发育和成年组织生理。这些途径最初是在体外通过生物化学方法发现的,因此长期存在的挑战是阐明这些途径之间的分子串扰及其生物学重要性。果蝇中的最新发现确立了遍在蛋白和SUMO途径通过进化保守的靶向SUMO的遍在蛋白连接酶(STUbL)蛋白相互联系。 STUbL是RING泛素连接酶,可识别SUMO酰化底物并催化其泛素化,包括果蝇中的Degringolade(Dgrn)以及人类中的RNF4和RNF111。 STUbL对于果蝇和小鼠胚胎的早期发育至关重要。在果蝇胚胎中,Dgrn调控早期细胞周期进程,性别确定,合子基因转录,分段和神经发生,以及其他过程。在成年苍蝇中,Dgrn是感染后对病原体的全身免疫反应和肠道干细胞再生所必需的。 Dgrn的这些功能在人类中高度保守,其中依赖RNF4的泛素化增强了关键的癌蛋白,从而加速了肿瘤的发生。在这里,我们回顾了迄今为止在果蝇中吸取的经验教训,并强调了它们与癌症生物学的相关性。

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