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Transdominant mutants of I kappa B alpha block Tat-tumor necrosis factor synergistic activation of human immunodeficiency virus type 1 gene expression and virus multiplication.

机译：IκB alpha的转化突变体阻断了人类免疫缺陷病毒1型基因表达和病毒繁殖的Tat肿瘤坏死因子协同激活。

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The human immunodeficiency virus type 1 (HIV-1) long terminal repeat (LTR) contains two binding sites for the NF-kappa B/Rel family of transcription factors which are required for the transcriptional activation of viral genes by inflammatory cytokines such as tumor necrosis factor alpha (TNF-alpha) and interleukin-1. In the present study, we examined the effect of transdominant mutants of I kappa B alpha on the synergistic activation of the HIV-1 LTR by TNF-alpha and the HIV-1 transactivator, Tat, in Jurkat T cells. The synergistic induction of HIV-1 LTR-driven gene expression represented a 50- to 70-fold stimulation and required both an intact HIV-1 enhancer and Tat-TAR element interaction, since mutations in Tat protein (R52Q, R53Q) or in the bulge region of the TAR element that eliminated Tat binding to TAR were unable to stimulate LTR expression. Coexpression of I kappa B alpha inhibited Tat-TNF-alpha activation of HIV LTR in a dose-dependent manner. Transdominant forms of I kappa B alpha, mutated in critical serine or threonine residues required for inducer-mediated (S32A, S36A) and/or constitutive (S283A, T291A, T299A) phosphorylation of I kappa B alpha were tested for their capacity to block HIV-1 LTR transactivation. I kappa B alpha molecules mutated in the N-terminal sites were not degraded following inducer-mediated stimulation (t1/2, > 4 h) and were able to efficiently block HIV-1 LTR transactivation. Strikingly, the I kappa B alpha (S32A, S36A) transdominant mutant was at least five times as effective as wild-type I kappa B alpha in inhibiting synergistic induction of the HIV-1 LTR. This mutant also effectively inhibited HIV-1 multiplication in a single-cycle infection model in Cos-1 cells, as measured by Northern (RNA) blot analysis of viral mRNA species and viral protein production. These experiments suggest a strategy that may contribute to inhibition of HIV-1 gene expression by interfering with the NF-kappa B/Rel signaling pathway.

机译：1型人类免疫缺陷病毒（HIV-1）长末端重复序列（LTR）包含两个NF-κB/ Rel家族转录因子结合位点，这些结合位点是通过炎症性细胞因子（例如肿瘤坏死）激活病毒基因的转录所必需的α因子（TNF-alpha）和白介素-1。在本研究中，我们研究了Jukat T细胞中IκBalpha的突变型突变体对TNF-α和HIV-1反式激活物Tat协同激活HIV-1 LTR的作用。 HIV-1 LTR驱动基因表达的协同诱导代表50到70倍的刺激，并且需要完整的HIV-1增强剂和Tat-TAR元素相互作用，因为Tat蛋白（R52Q，R53Q）或消除Tat与TAR结合的TAR元件的凸起区域无法刺激LTR表达。 IκBα的共表达以剂量依赖性方式抑制HIV LTR的Tat-TNF-α活化。测试了诱导型介导的（S32A，S36A）和/或组成型（S283A，T291A，T299A）磷酸化IκBalpha所需的关键丝氨酸或苏氨酸残基中突变的IκBalpha的转化形式的阻断HIV的能力-1 LTR反式激活。在诱导剂介导的刺激下（t1 / 2，> 4 h），在N末端位点突变的IκBα分子未降解，并能够有效阻断HIV-1 LTR反式激活。令人惊讶的是，在抑制HIV-1 LTR的协同诱导中，IκB alpha（S32A，S36A）突变型突变体的有效性至少是野生型IκB alpha的五倍。该突变体还可以有效抑制Cos-1细胞在单周期感染模型中的HIV-1繁殖，这是通过病毒mRNA种类和病毒蛋白产生的Northern（RNA）印迹分析测得的。这些实验提出了可能通过干扰NF-κB/ Rel信号通路来抑制HIV-1基因表达的策略。

著录项

期刊名称 Journal of Virology
作者
P Beauparlant; H Kwon; M Clarke; R Lin; N Sonenberg; M Wainberg; J Hiscott;
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年(卷),期 1996(70),9
年度 1996
页码 5777–5785
总页数 9
原文格式 PDF
正文语种
中图分类人体病毒学（致病病毒）;病毒（滤过性病毒）;
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1. Quercetin synergistically reactivates human immunodeficiency virus type 1 latency by activating nuclear factor-kappa B [J] . Yang Xinyi, Zhu Xiaoli, Ji Haiyan, Molecular medicine reports . 2018,第2aPta1期

机译：槲皮素通过激活核因子-kappa b协同重新激活人类免疫缺陷病毒1型延迟
2. Elevated tumor necrosis factor-alpha activation of human immunodeficiency virus type 1 subtype C in Southern Africa is associated with an NF-kappaB enhancer gain-of-function. [J] . Montano MA, Nixon CP, Ndungu T, The Journal of Infectious Diseases . 2000,第1期

机译：在南部非洲，人类免疫缺陷病毒C型1亚型的肿瘤坏死因子α激活水平升高与NF-κB增强子的功能获得有关。
3. Proteins of 30 and 36 kilodaltons, membrane constituents of the Staphylococcus aureus L form, induce production of tumor necrosis factor alpha and activate the human immunodeficiency virus type 1 long terminal repeat. [J] . A Akashi, S Ono, K Kuwano, Infection and immunity . 1996,第8期

机译：30和36公里道尔顿的蛋白质（金黄色葡萄球菌L型的膜成分）诱导产生肿瘤坏死因子α，并激活人类免疫缺陷病毒1型长末端重复序列。
4. Brain-Derived Neurotrophic Factor Prevents Human Immunodeficiency Prevents Human Immunodeficiency Virus Type 1 Protein gp120 Neurotoxicityin the Rat Nigrostriatal System [C] . ITALO MOCCHETTI, RACHEL L. NOSHENY, GIANLUIGI TANDA, International Conference on Neuroprotective Agents: Clinical and Experimental Aspects . 2007

机译：脑衍生的神经营养因子可防止人类免疫缺陷可防止人类免疫缺陷病毒1型蛋白GP120神经毒性素大鼠核心瘤系统
5. Genetic analyses of human immunodeficiency virus type 1 integrase mutants. [D] . Lu, Richard W. 2005

机译：人类免疫缺陷病毒1型整合酶突变体的遗传分析。
6. Nuclear export of the human immunodeficiency virus type 1 nucleocytoplasmic shuttle protein Rev is mediated by its activation domain and is blocked by transdominant negative mutants. [O] . A M Szilvay, K A Brokstad, R Kopperud, 1995

机译：人类免疫缺陷病毒1型核质穿梭蛋白Rev的核输出由其激活结构域介导并被反显性负突变体阻断。
7. Tumor necrosis factor alpha activates human immunodeficiency virus type 1 through induction of nuclear factor binding to the NF-kappa B sites in the long terminal repeat. [O] . Duh, E J, Maury, W J, Folks, T M, 1989

机译：肿瘤坏死因子α通过诱导与长末端重复序列中的NF-κB位点结合的核因子而激活1型人类免疫缺陷病毒。
8. Hantaan Virus Nucleocapsid Protein Binds to Importin alpha Proteins and Inhibits Tumor Necrosis Factor Alpha-Induced Activation of Nuclear Factor Kappa B [R] . Taylor, S. L., Frias-Staheli, N., Garcia-Sastre, A., 2008

机译：汉坦病毒核衣壳蛋白与进口蛋白α蛋白结合并抑制肿瘤坏死因子α诱导的核因子κB活化

Transdominant mutants of I kappa B alpha block Tat-tumor necrosis factor synergistic activation of human immunodeficiency virus type 1 gene expression and virus multiplication.

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