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转录因子YY1与人乳头瘤病毒8型E6启动子控制序列的调控相互作用。

Regulatory interactions of transcription factor YY1 with control sequences of the E6 promoter of human papillomavirus type 8.

作者信息

Pajunk H S, May C, Pfister H, Fuchs P G

机构信息

Institut für Virologie der Universität zu Köln, Germany.

出版信息

J Gen Virol. 1997 Dec;78 ( Pt 12):3287-95. doi: 10.1099/0022-1317-78-12-3287.

Abstract

Human papillomavirus type 8 (HPV-8) is a strictly cutaneous oncogenic virus known to induce malignant skin lesions in epidermodysplasia verruciformis patients. Our study shows that sequences surrounding transcription start sites of the HPV-8 oncogene E6 (nt 175-179) and comprising the presumable CCAAC and TATA boxes of the E6 promoter P175 contain a cluster of four motifs similar to the DNA recognition site of the multifunctional cellular transcription factor yin-yang 1 (YY1). Using DNase I footprinting and gel retardation tests it could be demonstrated that three of these motifs indeed act as YY1 binding sites. To test their functional relevance for P175 activity, engineered YY1 binding site mutants were analysed in the context of a P175 test vector using transient expression assays with human keratinocytes. YY1 turned out to exert both positive and negative effects upon the activity of the HPV-8 E6 promoter; binding of YY1 to a site upstream of the promoter's cap-position (BS1) activated transcription, whereas the downstream site (BS2) mediated repression. The second downstream YY1 binding site (BS3) seemed to play an auxiliary role, enhancing the negative effect of YY1 BS2. These observations define YY1 as an important cellular protein involved in the control of E6 oncogene expression of the skin-specific 'high risk' HPV-8 and emphasize the potential regulatory role of sequences located downstream of the transcription start site.

摘要

人乳头瘤病毒8型(HPV-8)是一种严格意义上的皮肤致癌病毒,已知可在疣状表皮发育不良患者中诱发恶性皮肤病变。我们的研究表明,HPV-8癌基因E6转录起始位点周围的序列(核苷酸175 - 179)以及包含E6启动子P175可能的CCAAC和TATA框的序列含有一组四个基序,类似于多功能细胞转录因子阴阳1(YY1)的DNA识别位点。使用DNA酶I足迹法和凝胶阻滞试验可以证明,这些基序中的三个确实作为YY1结合位点起作用。为了测试它们对P175活性的功能相关性,在人角质形成细胞的瞬时表达试验中,在P175测试载体的背景下分析了工程化的YY1结合位点突变体。结果表明,YY1对HPV-8 E6启动子的活性具有正负两种影响;YY1与启动子帽位点上游的一个位点(BS1)结合激活转录,而下游位点(BS2)介导抑制作用。第二个下游YY1结合位点(BS3)似乎起辅助作用,增强了YY1 BS2的负效应。这些观察结果将YY1定义为参与控制皮肤特异性“高危”HPV-8的E6癌基因表达的重要细胞蛋白,并强调了转录起始位点下游序列的潜在调节作用。

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