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The T-Box factor TBX3 is important in S-phase and is regulated by c-Myc and cyclin A-CDK2

机译:T-Box因子TBX3在S期很重要并受c-Myc和细胞周期蛋白A-CDK2调控

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摘要

The transcription factor, TBX3, is critical for the formation of, among other structures, the heart, limbs and mammary glands and haploinsufficiency of the human TBX3 gene result in ulnar-mammary syndrome which is characterized by hypoplasia of these structures. On the other hand, the overexpression of TBX3 is a feature of a wide range of cancers and it has been implicated in several aspects of the oncogenic process. This includes its ability to function as an immortalizing gene and to promote proliferation through actively repressing negative cell cycle regulators. Together this suggests that TBX3 levels may need to be tightly regulated during the cell cycle. Here we demonstrate that this is indeed the case and that TBX3 mRNA and protein levels peak at S-phase and that the TBX3 protein is predominantly localized to the nucleus of S-phase cells. The increased levels of TBX3 in S-phase are shown to occur transcriptionally through activation by c-Myc at E-box motifs located at −1210 and −701 bps and post-translationally by cyclin A-CDK2 phosphorylation. Importantly, when TBX3 is depleted by shRNA the cells accumulate in S-phase. These results suggest that TBX3 is required for cells to transit through S-phase and that this function may be linked to its role as a pro-proliferative factor.
机译:转录因子TBX3对于心脏,四肢和乳腺等结构的形成至关重要,人TBX3基因的单倍体不足会导致尺骨-乳腺综合症,其特征是这些结构的发育不全。另一方面,TBX3的过表达是多种癌症的特征,并且与致癌过程的多个方面有关。这包括其作为永生基因起作用并通过积极抑制细胞周期负调控因子促进增殖的能力。总之,这表明在细胞周期中可能需要严格调节TBX3的水平。在这里,我们证明确实如此,并且TBX3 mRNA和蛋白质水平在S期达到峰值,并且TBX3蛋白主要位于S期细胞的核内。在S期中,TBX3水平的增加显示为通过c-Myc激活位于-1210和-701 bps的E-box基序转录产生,以及通过细胞周期蛋白A-CDK2磷酸化在翻译后发生。重要的是,当shRNA耗尽了TBX3时,细胞会以S期积累。这些结果表明,TBX3是细胞通过S期转运所必需的,并且该功能可能与其作为增殖因子的作用有关。

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