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Structure of the full human RXR/VDR nuclear receptor heterodimer complex with its DR3 target DNA

机译:完整的人RXR / VDR核受体异二聚体复合物及其DR3靶DNA的结构

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摘要

Transcription regulation by steroid hormones and other metabolites is mediated by nuclear receptors (NRs) such as the vitamin D and retinoid X receptors (VDR and RXR). Here, we present the cryo electron microscopy (cryo-EM) structure of the heterodimeric complex of the liganded human RXR and VDR bound to a consensus DNA response element forming a direct repeat (DR3). The cryo-EM map of the 100-kDa complex allows positioning the individual crystal structures of ligand- and DNA-binding domains (LBDs and DBDs). The LBDs are arranged perpendicular to the DNA and are located asymmetrically at the DNA 5′-end of the response element. The structure reveals that the VDR N-terminal A/B domain is located close to the DNA. The hinges of both VDR and RXR are fully visible and hold the complex in an open conformation in which co-regulators can bind. The asymmetric topology of the complex provides the structural basis for RXR being an adaptive partner within NR heterodimers, while the specific helical structure of VDR's hinge connects the 3′-bound DBD with the 5′-bound LBD and thereby serves as a conserved linker of defined length sensitive to mutational deletion.
机译:类固醇激素和其他代谢产物的转录调控是由核受体(NRs)介导的,例如维生素D和类维生素X受体(VDR和RXR)。在这里,我们介绍了配体人类RXR和VDR的异源二聚体复合物的低温电子显微镜(cryo-EM)结构,该复合物与形成直接重复序列(DR3)的共有DNA反应元件结合。 100 kDa复合物的冷冻EM图谱可定位配体和DNA结合域(LBD和DBD)的单个晶体结构。 LBD垂直于DNA排列并且不对称地位于响应元件的DNA 5'末端。该结构揭示了VDR N端A / B结构域位于DNA附近。 VDR和RXR的铰链都是完全可见的,并将复合物保持在开放状态,共调节剂可以在其中结合。复合物的不对称拓扑为RXR作为NR异二聚体中的适应性伴侣提供了结构基础,而VDR铰链的特定螺旋结构将3'结合的DBD与5'结合的LBD连接起来,从而充当了RDR的保守连接子。定义的长度对突变缺失敏感。

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