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维甲酸X受体选择性激动剂及其合成方法。

Retinoid X Receptor Selective Agonists and their Synthetic Methods.

作者信息

Wagner Carl E, Jurutka Peter W, Marshall Pamela A, Heck Michael C

机构信息

School of Mathematical and Natural Sciences, Arizona State University, 4701 W Thunderbird Road, Glendale, AZ, United States.

出版信息

Curr Top Med Chem. 2017;17(6):742-767. doi: 10.2174/1568026616666160617091559.

DOI:10.2174/1568026616666160617091559
PMID:27320333
Abstract

Since the isolation and identification of the retinoid X receptor (RXR) as a member of the nuclear receptor (NR) superfamily in 1990, its analysis has ushered in a new understanding of physiological regulation by nuclear receptors, and novel methods to identify other unknown and orphan receptors. Expression of one or more of the three isoforms of RXR-α, β, and γ-can be found in every human cell type. Biologically, RXR plays a critical role through its ability to partner with other nuclear receptors. RXR is able to regulate nutrient metabolism by forming "permissive" heterodimers with peroxisome proliferator-activated receptor (PPAR), liver-X-receptor (LXR), farnesoid X receptor (FXR), pregnane X receptor (PXR) and constitutive androstane receptor (CAR), which function when ligands are bound to one or both of the heterodimer partners. Conversely, RXR is able to form "nonpermissive" heterodimers with vitamin D receptor (VDR), thyroid receptor (TR) and retinoic acid receptor (RAR), which function only in the presence of vitamin D, T3 and retinoic acid, respectively. Furthermore, RXR can form homodimers in the presence of a selective agonist, or rexinoid, to regulate gene expression and to either inhibit proliferation or induce apoptosis in human cancers. Thus, over the last 25 years there have been several reports on the design and synthesis of small molecule rexinoids. This review summarizes the synthetic methods for several of the most potent rexinoids thus far reported.

摘要

自1990年类视黄醇X受体(RXR)作为核受体(NR)超家族的一员被分离和鉴定以来,对其分析开启了对核受体生理调节的新认识,以及鉴定其他未知和孤儿受体的新方法。RXR-α、β和γ三种异构体中的一种或多种的表达可在每种人类细胞类型中找到。在生物学上,RXR通过与其他核受体结合的能力发挥关键作用。RXR能够通过与过氧化物酶体增殖物激活受体(PPAR)、肝脏X受体(LXR)、法尼醇X受体(FXR)、孕烷X受体(PXR)和组成型雄甾烷受体(CAR)形成“允许性”异二聚体来调节营养代谢,当配体与异二聚体的一个或两个伙伴结合时这些异二聚体发挥作用。相反,RXR能够与维生素D受体(VDR)、甲状腺受体(TR)和视黄酸受体(RAR)形成“非允许性”异二聚体,它们分别仅在维生素D、T3和视黄酸存在时发挥作用。此外,RXR可以在选择性激动剂或类视黄醇X受体激动剂存在的情况下形成同二聚体,以调节基因表达并抑制人类癌症中的增殖或诱导凋亡。因此,在过去25年里,有几篇关于小分子类视黄醇X受体激动剂设计和合成的报道。本综述总结了迄今为止报道的几种最有效的类视黄醇X受体激动剂的合成方法。

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