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The transforming acidic coiled coil (TACC1) protein modulates the transcriptional activity of the nuclear receptors TR and RAR

机译:转化酸性卷曲螺旋蛋白(TACC1)调节核受体TR和RAR的转录活性

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The transcriptional activity of Nuclear hormone Receptors (NRs) is regulated by interaction with coactivator or corepressor proteins. Many of these cofactors have been shown to have a misregulated expression or to show a subcellular mislocalization in cancer cell lines or primary tumors. Therefore they can be factors involved in the process of oncogenesis. We describe a novel NR coregulator, TACC1, which belongs to the Transforming Acidic Coiled Coil (TACC) family. The interaction of TACC1 with Thyroid Hormone Receptors (TR) and several other NRs has been shown in a yeast two-hybrid screen and confirmed by GST pulldown, colocalization and co-immunoprecipitation experiments. TACC1 interacts preferentially with unliganded NRs. In F9 cells, endogenous TACC1 localized in the chromatin-enriched fraction of the nucleus and interacted with Retinoid Acid Receptors (RARα) in the nucleus. TACC1 depletion in the cell led to decreased RARα and TRα ligand-dependent transcriptional activity and to delocalization of TR from the nucleus to the cytoplasm. From these experimental studies we propose that TACC1 might be a scaffold protein building up a transcriptional complex around the NRs we studied. This function of TACC1 might account for its involvement in several forms of tumour development.
机译:核激素受体(NRs)的转录活性是通过与共激活蛋白或共加压蛋白相互作用来调节的。这些辅助因子中的许多已显示在癌细胞系或原发性肿瘤中表达失调或显示亚细胞错位。因此,它们可能是致癌过程中涉及的因素。我们描述了一种新型的NR磁化剂TACC1,它属于转化酸性线圈(TACC)家族。 TACC1与甲状腺激素受体(TR)和其他几种NR的相互作用已在酵母双杂交筛选中显示,并通过GST下拉,共定位和共免疫沉淀实验得到证实。 TACC1优先与未配体的NR相互作用。在F9细胞中,内源性TACC1定位于细胞核中富含染色质的部分,并与细胞核中的类维生素A受体(RARα)相互作用。细胞中TACC1的消耗导致RARα和TRα配体依赖性转录活性的降低,以及TR从细胞核到细胞质的脱位。从这些实验研究中,我们建议TACC1可能是在我们研究的NRs周围建立转录复合体的支架蛋白。 TACC1的这种功能可能是其参与多种形式的肿瘤发展的原因。

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