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Structural and functional features of a specific nucleosome containing a recognition element for the thyroid hormone receptor.

机译:含有甲状腺激素受体识别元件的特定核小体的结构和功能特征。

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摘要

The Xenopus thyroid hormone receptor betaA (TRbetaA) gene contains an important thyroid hormone response element (TRE) that is assembled into a positioned nucleosome. We determine the translational position of the nucleosome containing the TRE and the rotational positioning of the double helix with respect to the histone surface. Histone H1 is incorporated into the nucleosome leading to an asymmetric protection to micrococcal nuclease cleavage of linker DNA relative to the nucleosome core. Histone H1 association is without significant consequence for the binding of the heterodimer of thyroid hormone receptor and 9-cis retinoic acid receptor (TR/RXR) to nucleosomal DNA in vitro, or for the regulation of TRbetaA gene transcription following microinjection into the oocyte nucleus. Small alterations of 3 and 6 bp in the translational positioning of the TRE in chromatin are also without effect on the transcriptional activity of the TRbetaA gene, whereas a small change in the rotational position of the TRE (3 bp) relative to the histone surface significantly reduces the binding of TR/RXR to the nucleosome and decreases transcriptional activation directed by TR/RXR. Our results indicate that the specific architecture of the nucleosome containing the TRE may have regulatory significance for expression of the TRbetaA gene.
机译:爪蟾甲状腺激素受体betaA(TRbetaA)基因包含一个重要的甲状腺激素反应元件(TRE),该元件被组装成定位的核小体。我们确定包含TRE的核小体的翻译位置和相对于组蛋白表面的双螺旋的旋转位置。组蛋白H1被掺入到核小体中,导致相对于核小体核心对接头DNA的微球菌核酸酶切割不对称保护。组蛋白H1缔合对于甲状腺激素受体和9-顺式视黄酸受体(TR / RXR)的异二聚体在体外与核小体DNA的结合或显微注入卵母细胞核后调节TRbetaA基因转录没有显着影响。 TRE在染色质中翻译位置的3和6 bp的微小变化也不会影响TRbetaA基因的转录活性,而TRE的旋转位置(3 bp)相对于组蛋白表面的微小变化会明显降低TR / RXR与核小体的结合并降低TR / RXR指导的转录激活。我们的结果表明,含有TRE的核小体的特定结构可能对TRbetaA基因的表达具有调节意义。

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