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Physical and functional interactions of human papillomavirus E2 protein with nuclear receptor coactivators

机译:人乳头瘤病毒E2蛋白与核受体共激活剂的物理和功能相互作用

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摘要

In addition to the human papillomavirus (HPV)-induced immortalization of epithelial cells, which usually requires integration of the viral DNA into the host cell genome, steroid hormone-activated nuclear receptors (NRs) are thought to bind to specific DNA sequences within transcriptional regulatory regions on the long control region to either increase or suppress transcription of dependent genes. In this study, our data suggest that the NR coactivator function of HPV E2 proteins might be mediated through physical and functional linteractions with not only NRs but also the NR coactivators GRIP1 (glucocorticoid receptor-interacting protein 1) and Zacl (zinc-finger protein which regulates apoptosis and cell cycle arrest 1), reciprocally regulating their transactivation activities. GRIP1 and Zacl both were able to act synergistically with HPV E2 proteins on the E2-, androgen receptor-, and estrogen receptor-dependent transcriptional activation systems. GRIP1 and Zacl might selectively function with HPV E2 proteins on thyroid receptor- and p53-dependent transcriptional activation, respectively. Hence, the transcriptional function of E2 might be mediated through NRs and NR coactivators to regulate E2-, NR-, and p53-dependent transcriptional activations. (c) 2007 Elsevier Inc. All rights reserved.
机译:除了人乳头瘤病毒(HPV)诱导的上皮细胞永生化(通常需要将病毒DNA整合到宿主细胞基因组中)外,类固醇激素激活的核受体(NRs)还被认为与转录调控内的特定DNA序列结合长控制区上的两个区域,以增加或抑制依赖性基因的转录。在这项研究中,我们的数据表明,HPV E2蛋白的NR共激活因子功能可能不仅通过与NR相互作用,而且还通过NR共激活因子GRIP1(糖皮质激素受体相互作用蛋白1)和Zacl(锌指蛋白调节细胞凋亡和细胞周期阻滞1),相互调节其反式激活活性。 GRIP1和Zacl都能够与HPV E2蛋白协同作用于依赖于E2-,雄激素受体和雌激素受体的转录激活系统。 GRIP1和Zacl可能与HPV E2蛋白选择性地分别作用于甲状腺受体依赖性和p53依赖性转录激活。因此,E2的转录功能可能通过NR和NR共激活因子介导,以调节E2-,NR-和p53依赖性转录激活。 (c)2007 Elsevier Inc.保留所有权利。

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