Effects on gene expression in rat liver after administration of RXR Agonists: UAB30, 4-Methyl-UAB30, and Targretin (Bexarotene)s

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Effects on gene expression in rat liver after administration of RXR Agonists: UAB30, 4-Methyl-UAB30, and Targretin (Bexarotene)s

机译：服用RXR激动剂后对大鼠肝脏中基因表达的影响：UAB30、4-甲基-UAB30和塔格列汀（Bexarotene）

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Examination of three retinoid X receptor (RXR) agonists [Targretin (TRG), UAB30, and 4-methyl-UAB30 (4-Me- UAB30)] showed that all inhibited mammary cancer in rodents and two (TRG and 4-Me-UAB30) strikingly increased serum triglyceride levels. Agents were administered in diets to female Sprague-Dawley rats. Liver RNA was isolated and microarrayed on the Affymetrix GeneChip Rat Exon 1.0 ST array. Statistical tests identified genes that exhibited differential expression and fell into groups, or modules, with differential expression among agonists. Genes in specific modules were changed by one, two, or all three agonists. An interactome analysis assessed the effects on genes that heterodimerize with known nuclear receptors. For proliferator-activated receptor a/RXR-activated genes, the strongest response was TRG . 4-Me-UAB30 . UAB30. Many liver X receptor/RXRrelated genes (e.g., Scd-1 and Srebf1, which are associated with increased triglycerides) were highly expressed in TRG and 4-Me-UAB30- but not UAB30-treated livers. Minimal expression changes were associated with retinoic acid receptor or vitamin D receptor heterodimers by any of the agonists. UAB30 unexpectedly and uniquely activated genes associated with the aryl hydrocarbon hydroxylase (Ah) receptor (Cyp1a1, Cyp1a2, Cyp1b1, and Nqo1). Based on the Ah receptor activation, UAB30 was tested for its ability to prevent dimethylbenzanthracene (DMBA)-induced mammary cancers, presumably by inhibiting DMBA activation, and was highly effective. Gene expression changes were determined by reverse transcriptasepolymerase chain reaction in rat livers treated with Targretin for 2.3, 7, and 21 days. These showed similar gene expression changes at all three time points, arguing some steady-state effect. Different patterns of gene expression among the agonists provided insight into molecular differences and allowed one to predict certain physiologic consequences of agonist treatment.

机译：对三种类维生素A X受体（RXR）激动剂[Tretretin（TRG），UAB30和4-甲基-UAB30（4-Me-UAB30）]的检查显示，它们均抑制了啮齿动物的乳癌，另外两种对TRK和4-Me-UAB30均具有抑制作用。）显着增加血清甘油三酯水平。在饮食中向雌性Sprague-Dawley大鼠施用药剂。分离肝RNA，并在Affymetrix GeneChip Rat Exon 1.0 ST阵列上进行微阵列。统计测试确定了表现出差异表达并落入激动剂之间差异表达的组或模块的基因。特定模块中的基因被一个，两个或所有三个激动剂改变。相互作用组分析评估了对与已知核受体异源二聚体基因的影响。对于增殖物激活的受体a / RXR激活的基因，最强的反应是TRG。 4-Me-UAB30。 UAB30。许多肝脏X受体/ RXR相关基因（例如，与甘油三酸酯含量增加相关的Scd-1和Srebf1）在TRG和4-Me-UAB30-处理的肝脏中高表达，而在UAB30处理的肝脏中未表达。通过任何激动剂，最小的表达变化都与视黄酸受体或维生素D受体异二聚体有关。 UAB30意外地且独特地激活了与芳烃羟化酶（Ah）受体（Cyp1a1，Cyp1a2，Cyp1b1和Nqo1）相关的基因。基于Ah受体激活，测试了UAB30预防二甲基苯并蒽（DMBA）诱导的乳腺癌的能力，推测是通过抑制DMBA激活来进行的，并且非常有效。通过逆转录酶聚合酶链反应在用Targretin处理2.3、7和21天的大鼠肝脏中确定基因表达的变化。这些在所有三个时间点都显示出相似的基因表达变化，这表明存在一定的稳态效应。激动剂之间基因表达的不同模式提供了对分子差异的深入了解，并使人们可以预测激动剂治疗的某些生理后果。

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《Molecular pharmacology.》 |2013年第3期|共11页
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机译：服用RXR激动剂后对大鼠肝脏中基因表达的影响：UAB30、4-甲基-UAB30和塔格列汀（Bexarotene）
2. The effects of coadministration of ghrelin agonist (GHRP-2) and GH on TNF-α, IL-6, and iNOS genes expression induced by LPS in mouse liver [J] . DepartmentofBiologyScienceandResearchBranch, DivisionofPhysiologyDepartmentofBasicSciences, DepartmentofBiologyQomBranch Comparative clinical pathology . 2014,第4期

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5. Effects of NMDA antagonists and GABA agonists on a multiple schedule of ethanol and saccharin self-administration in rats. [D] . Shelton, Keith Larry. 1995

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6. Effects on Gene Expression in Rat Liver after Administration of RXR Agonists: UAB30 4-Methyl-UAB30 and Targretin (Bexarotene) [O] . Peter T. Vedell, Yan Lu, Clinton J. Grubbs, -1

机译：服用RXR激动剂后对大鼠肝脏基因表达的影响：UAB30、4-甲基-UAB30和塔格列汀（Bexarotene）
7. A selective retinoid X receptor agonist bexarotene (LGD1069, targretin) inhibits angiogenesis and metastasis in solid tumours [O] . Yen, W-C, Prudente, R Y, Corpuz, M R, 2006

机译：选择性维甲酸X受体激动剂贝沙罗汀（LGD1069，targretin）抑制实体瘤中的血管生成和转移

Effects on gene expression in rat liver after administration of RXR Agonists: UAB30, 4-Methyl-UAB30, and Targretin (Bexarotene)s

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