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Myb-Binding Protein 1A (MYBBP1A) Is Essential for Early Embryonic Development Controls Cell Cycle and Mitosis and Acts as a Tumor Suppressor

机译:mYB结合蛋白1a(mYBBp1a)是必不可少的早期胚胎发育控制细胞周期和有丝分裂并作为一种肿瘤抑制基因

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摘要

MYBBP1A is a predominantly nucleolar transcriptional regulator involved in rDNA synthesis and p53 activation via acetylation. However little further information is available as to its function. Here we report that MYBBP1A is developmentally essential in the mouse prior to blastocyst formation. In cell culture, down-regulation of MYBBP1A decreases the growth rate of wild type mouse embryonic stem cells, mouse embryo fibroblasts (MEFs) and of human HeLa cells, where it also promotes apoptosis. HeLa cells either arrest at G2/M or undergo delayed and anomalous mitosis. At mitosis, MYBBP1A is localized to a parachromosomal region and gene-expression profiling shows that its down-regulation affects genes controlling chromosomal segregation and cell cycle. However, MYBBP1A down-regulation increases the growth rate of the immortalized NIH3T3 cells. Such Mybbp1a down-regulated NIH3T3 cells are more susceptible to Ras-induced transformation and cause more potent Ras-driven tumors. We conclude that MYBBP1A is an essential gene with novel roles at the pre-mitotic level and potential tumor suppressor activity.
机译:MYBBP1A是主要的核仁转录调节因子,参与rDNA合成和通过乙酰化激活p53。然而,关于其功能的进一步信息很少。在这里,我们报告MYBBP1A在胚泡形成之前在小鼠中发育至关重要。在细胞培养中,MYBBP1A的下调会降低野生型小鼠胚胎干细胞,小鼠胚胎成纤维细胞(MEF)和人HeLa细胞的生长速率,并在其中促进细胞凋亡。 HeLa细胞停滞在G2 / M或经历延迟和异常的有丝分裂。在有丝分裂时,MYBBP1A位于染色体旁区域,基因表达图谱显示其下调影响控制染色体分离和细胞周期的基因。但是,MYBBP1A下调增加了永生化NIH3T3细胞的生长速率。这种Mybbp1a下调的NIH3T3细胞更容易受到Ras诱导的转化,并导致更有效的Ras驱动的肿瘤。我们得出的结论是,MYBBP1A是必需基因,在有丝分裂前水平和潜在的肿瘤抑制活性上具有新颖的作用。

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