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孤儿受体肝细胞核因子4的特异性同源二聚化定义了核受体的一个新亚类。

Exclusive homodimerization of the orphan receptor hepatocyte nuclear factor 4 defines a new subclass of nuclear receptors.

作者信息

Jiang G, Nepomuceno L, Hopkins K, Sladek F M

机构信息

Environmental Toxicology Graduate Program, University of California, Riverside 92521, USA.

出版信息

Mol Cell Biol. 1995 Sep;15(9):5131-43. doi: 10.1128/MCB.15.9.5131.

Abstract

Hepatocyte nuclear factor 4 (HNF-4), a highly conserved member of the steroid hormone receptor superfamily critical for development and liver-specific gene expression, is very similar to another superfamily member, retinoid X receptor alpha (RXR alpha), in overall amino acid sequence and DNA binding specificity. Since RXR alpha is known to heterodimerize with many other nuclear receptors, the formation of heterodimers between HNF-4 and RXR alpha was examined. With the electrophoretic mobility shift assay, coimmunoprecipitation, and transient transfection assays, it is shown that, unlike other nuclear receptors, HNF-4 does not form heterodimers with RXR alpha either in the presence or in the absence of DNA. We also show that in vitro-translated HNF-4 does not form heterodimeric complexes on DNA with a number of other receptors, including RXR beta, RXR gamma, retinoic acid receptor alpha, or thyroid hormone receptor alpha. To investigate the hypothesis that the lack of heterodimerization between HNF-4 and RXR alpha is due to a strong homodimerization activity of HNF-4, glycerol gradient sedimentation and kinetic analysis were used to show that HNF-4 is in fact a stable homodimer in solution. Finally, immunohistochemistry is used to show that the HNF-4 protein is found exclusively in the nuclei in both HepG2 cells, which express endogenous HNF-4, and transfected COS cells, which overexpress HNF-4. These findings lead us to propose that HNF-4 defines a new subclass of nuclear receptors which reside primarily in the nucleus and which bind DNA and regulate transcription as homodimers.

摘要

肝细胞核因子4(HNF-4)是类固醇激素受体超家族中高度保守的成员,对发育和肝脏特异性基因表达至关重要,在整体氨基酸序列和DNA结合特异性方面与另一个超家族成员视黄酸X受体α(RXRα)非常相似。由于已知RXRα可与许多其他核受体形成异二聚体,因此研究了HNF-4与RXRα之间异二聚体的形成。通过电泳迁移率变动分析、免疫共沉淀和瞬时转染分析表明,与其他核受体不同,无论有无DNA存在,HNF-4都不会与RXRα形成异二聚体。我们还表明,体外翻译的HNF-4不会与包括RXRβ、RXRγ、视黄酸受体α或甲状腺激素受体α在内的许多其他受体在DNA上形成异二聚体复合物。为了研究HNF-4与RXRα之间缺乏异二聚化是由于HNF-4强大的同二聚化活性这一假设,使用甘油梯度沉降和动力学分析表明,HNF-4实际上在溶液中是稳定的同二聚体。最后,免疫组织化学用于表明HNF-4蛋白仅在表达内源性HNF-4的HepG2细胞和过表达HNF-4的转染COS细胞的细胞核中被发现。这些发现使我们提出,HNF-4定义了一类新的核受体亚类,它们主要存在于细胞核中,以同二聚体形式结合DNA并调节转录。

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