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首页> 外文OA文献 >The NF-kappa B and Sp1 motifs of the human immunodeficiency virus type 1 long terminal repeat function as novel thyroid hormone response elements.
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The NF-kappa B and Sp1 motifs of the human immunodeficiency virus type 1 long terminal repeat function as novel thyroid hormone response elements.

机译:人类免疫缺陷病毒1型长末端重复序列的NF-κB和Sp1模体作为新型甲状腺激素反应元件发挥作用。

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We report that thyroid hormone (T3) receptor (T3R) can activate the human immunodeficiency virus type 1 (HIV-1) long terminal repeat (LTR). Purified chick T3R-alpha 1 (cT3R-alpha 1) binds as monomers and homodimers to a region in the LTR (nucleotides -104 to -75 [-104/-75]) which contains two tandem NF-kappa B binding sites and to a region (-80/-45) which contains three Sp1 binding sites. In contrast, human retinoic acid receptor alpha (RAR-alpha) and mouse retinoid X receptor beta (RXR-beta) do not bind to these elements. However, RXR-beta binds to these elements as heterodimers with cT3R-alpha 1 and to a lesser extent with RAR-alpha. Gel mobility shift assays also revealed that purified NF-kappa B p50/65 or p50/50 can bind to one but not both NF-kappa B sites simultaneously. Although the binding sites for p50/65, p50/50, and T3R, or Sp1 and T3R, overlap, their binding is mutually exclusive, and with the inclusion of RXR-beta, the major complex is the RXR-beta-cT3R-alpha 1 heterodimer. The NF-kappa B region of the LTR and the NF-kappa B elements from the kappa light chain enhancer both function as T3 response elements (TREs) when linked to a heterologous promoter. The TREs in the HIV-1 NF-kappa B sites appear to be organized as a direct repeat with an 8- or 10-bp gap between the half-sites. Mutations within the NF-kappa B motifs which eliminate binding of cT3R-alpha 1 also abolish stimulation by T3, indicating that cT3R-alpha 1 binding to the Sp1 region does not independently mediate activation by T3. The Sp1 region, however, is converted to a functionally strong TRE by the viral tat factor. These studies indicate that the HIV-1 LTR contains both tat-dependent and tat-independent TREs and reveal the potential for T3R to modulate other genes containing NF-kappa B- and Sp1-like elements. Furthermore, they indicate the importance of other transcription factors in determining whether certain T3R DNA binding sequences can function as an active TRE.
机译:我们报告甲状腺激素(T3)受体(T3R)可以激活人类免疫缺陷病毒1型(HIV-1)的长末端重复(LTR)。纯化的雏鸡T3R-alpha 1(cT3R-alpha 1)作为单体和同二聚体结合到LTR中的一个区域(核苷酸-104至-75 [-104 / -75]),该区域包含两个串联的NF-κB结合位点,一个包含三个Sp1结合位点的区域(-80 / -45)。相反,人视黄酸受体α(RAR-alpha)和小鼠视黄醇X受体beta(RXR-beta)不结合这些元素。但是,RXR-β与cT3R-alpha 1结合为这些二聚体,而与RAR-alpha结合的程度较小。凝胶迁移率迁移分析还显示,纯化的NF-κBp50 / 65或p50 / 50可以同时结合一个,但不能同时结合两个NF-κB位点。尽管p50 / 65,p50 / 50和T3R或Sp1和T3R的结合位点重叠,但它们的结合是互斥的,并且在包含RXR-beta的情况下,主要复合物是RXR-beta-cT3R-alpha 1个异二聚体。当与异源启动子连接时,LTR的NF-κB区和来自κ轻链增强子的NF-κB元件均充当T3反应元件(TRE)。 HIV-1NF-κB位点的TRE似乎是直接重复的,在两个位点之间有8或10 bp的间隔。消除cT3R-alpha 1结合的NF-κB基序内的突变也消除了T3的刺激,表明cT3R-alpha 1与Sp1区的结合并不独立介导T3的激活。但是,Sp1区被病毒tat因子转化为功能强大的TRE。这些研究表明,HIV-1 LTR既包含依赖于tat的TRE,也包含依赖于tat的TRE,并且揭示了T3R调节包含NF-κB和Sp1样元件的其他基因的潜力。此外,它们表明其他转录因子在确定某些T3R DNA结合序列是否可以充当活性TRE方面的重要性。

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