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RBX1 (RING Box Protein 1) E3 Ubiquitin Ligase Is Required for Genomic Integrity by Modulating DNA Replication Licensing Proteins*

机译:RBX1(RING盒蛋白1)E3泛素连接酶是通过调节DNA复制许可蛋白实现基因组完整性所必需的*

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摘要

RBX1 (RING box protein 1), also known as ROC1 (Regulator of Cullin 1), is an essential component of SCF (Skp1/Cullins/F-box) E3 ubiquitin ligases, which target diverse proteins for proteasome-mediated degradation. Our recent study showed that RBX1 silencing triggered a DNA damage response (DDR) leading to G2-M arrest, senescence, and apoptosis, with the mechanism remaining elusive. Here, we show that, in human cancer cells, RBX1 silencing causes the accumulation of DNA replication licensing proteins CDT1 and ORC1, leading to DNA double-strand breaks, DDR, G2 arrest, and, eventually, aneuploidy. Whereas CHK1 activation by RBX1 silencing is responsible for the G2 arrest, enhanced DNA damage renders cancer cells more sensitive to radiation. In Caenorhabditis elegans, RBX-1 silencing causes CDT-1 accumulation, triggering DDR in intestinal cells, which is largely abrogated by simultaneous CDT-1 silencing. RBX-1 silencing also induces lethality during development of embryos and in adulthood. Thus, RBX1 E3 ligase is essential for the maintenance of mammalian genome integrity and the proper development and viability in C. elegans.
机译:RBX1(RING盒蛋白1),也称为ROC1(Cullin 1的调节物),是SCF(Skp1 / Cullins / F-box)E3泛素连接酶的重要组成部分,其针对蛋白酶体介导的降解的多种蛋白质。我们最近的研究表明,RBX1沉默引发DNA损伤反应(DDR),导致G2-M阻滞,衰老和细胞凋亡,但机制尚不清楚。在这里,我们表明,在人类癌细胞中,RBX1沉默导致DNA复制许可蛋白CDT1和ORC1的积累,导致DNA双链断裂,DDR,G2阻滞,并最终导致非整倍性。 RBX1沉默激活CHK1导致G2阻滞,而DNA损伤增强使癌细胞对放射线更加敏感。在秀丽隐杆线虫中,RBX-1沉默会导致CDT-1积累,从而触发肠道细胞中的DDR,而在同时进行CDT-1沉默的情况下,DDR会被消除。 RBX-1沉默还会在胚胎发育和成年期诱导致死性。因此,RBX1 E3连接酶对于维持哺乳动物基因组完整性以及秀丽隐杆线虫的适当发育和生存力至关重要。

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