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一类对维甲酸X受体具有选择性活性的新型维甲酸增强HL-60细胞分化作用

Enhancement of HL-60 differentiation by a new class of retinoids with selective activity on retinoid X receptor.

作者信息

Apfel C M, Kamber M, Klaus M, Mohr P, Keidel S, LeMotte P K

机构信息

Department of Dermatology, F. Hoffmann-LaRoche, Basel, Switzerland.

出版信息

J Biol Chem. 1995 Dec 22;270(51):30765-72. doi: 10.1074/jbc.270.51.30765.

Abstract

Cellular responsiveness to retinoic acid and its metabolites is conferred through two distinct families of receptors: the retinoic acid receptors (RARs) and the retinoid X receptors (RXRs). Herein, we report on the identification and characterization of several conformationally restricted retinoids, which selectively bind and activate RX receptors. Under the influence of retinoids, HL-60 myelocytic leukemia cells differentiate into granulocytes. This effect is mediated by RAR alpha, as has been demonstrated through the use of a selective RAR alpha antagonist (Apfel, C., Bauer, F., Crettaz, M., Forni, L., Kamber, M., Kaufmann, F., LeMotte, P., Pirson, W., and Klaus, M. (1992) Proc. Natl. Acad. Sci. U.S.A. 89, 7129-7133). Here, we show that conformationally restricted RXR-specific retinoids, at doses that are per se inactive, are able to potentiate by up to one order of magnitude the pro-differentiating effects of all-trans retinoic acid and an RAR alpha-selective synthetic retinoid. We also present evidence that these RXR-selective ligands are able to bind to a DNA RXR.RAR heterodimer complex. This finding demonstrates that agonists for RARs and RXRs can synergistically promote HL-60 differentiation, which could be mediated through a heterodimer of these receptors.

摘要

细胞对维甲酸及其代谢产物的反应是通过两类不同的受体介导的

维甲酸受体(RARs)和类视黄醇X受体(RXRs)。在此,我们报告了几种构象受限类视黄醇的鉴定和特性,这些类视黄醇能选择性地结合并激活RX受体。在类视黄醇的影响下,HL-60髓性白血病细胞可分化为粒细胞。这种效应是由RARα介导的,这已通过使用选择性RARα拮抗剂得到证实(阿佩尔,C.,鲍尔,F.,克雷塔兹,M.,福尔尼,L.,坎贝尔,M.,考夫曼,F.,勒莫特,P.,皮尔森,W.,和克劳斯,M.(1992年)《美国国家科学院院刊》89,7129 - 7133)。在此,我们表明,构象受限的RXR特异性类视黄醇,在其本身无活性的剂量下,能够将全反式维甲酸和一种RARα选择性合成类视黄醇的促分化作用增强高达一个数量级。我们还提供证据表明,这些RXR选择性配体能够与DNA上的RXR·RAR异二聚体复合物结合。这一发现表明,RARs和RXRs的激动剂可协同促进HL-分化,这可能是通过这些受体的异二聚体介导的。

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