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银杏叶提取物对人组成型雄烷受体的同种型选择性激活:SV23、SV24 和 SV25 剪接变异体的功能分析。

Isoform-selective activation of human constitutive androstane receptor by Ginkgo biloba extract: functional analysis of the SV23, SV24, and SV25 splice variants.

机构信息

Faculty of Pharmaceutical Sciences, The University of British Columbia, 2146 East Mall, Vancouver, British Columbia, V6T 1Z3, Canada.

出版信息

J Pharmacol Exp Ther. 2011 Nov;339(2):704-15. doi: 10.1124/jpet.111.186130. Epub 2011 Aug 23.

Abstract

Naturally occurring splice variants of human constitutive androstane receptor (hCAR) exist, including hCAR-SV23 (insertion of amino acids SPTV), hCAR-SV24 (APYLT), and hCAR-SV25 (SPTV and APYLT). An extract of Ginkgo biloba was reported to activate hCAR-SV24 and the wild type (hCAR-WT). However, it is not known whether it selectively affects hCAR splice variants, how it activates hCAR isoforms, and which chemical is responsible for the effects of the extract. Therefore, we evaluated the impact of G. biloba extract on the functionality of hCAR-SV23, hCAR-SV24, hCAR-SV25, and hCAR-WT and compared it with that of phenobarbital, di-(2-ethylhexyl)phthalate (DEHP), 6-(4-chlorophenyl)imidazo[2,1-b][1,3]thiazole-5-carbaldehyde O-(3,4-dichlorobenzyl)oxime (CITCO), and 1,4-bis-[2-(3,5-dichloropyridyloxy)]benzene (TCPOBOP) in cell-based reporter gene assays. Among the hCAR splice variants investigated, only hCAR-SV23 was activated by G. biloba extract, and this required cotransfection of a retinoid X receptor α (RXRα) expression plasmid. The extract activated hCAR-SV23 to a lesser extent than hCAR-WT, but ginkgolide A, ginkgolide B, ginkgolide C, ginkgolide J, and bilobalide were not responsible for the effects of the extract. CITCO activated hCAR-SV23, hCAR-SV24, and hCAR-WT. By comparison, phenobarbital activated hCAR-WT, whereas DEHP activated hCAR-SV23, hCAR-SV24 (with exogenous RXRα supplementation), and hCAR-WT. TCPOBOP did not affect the activity of any of the isoforms. G. biloba extract and phenobarbital did not bind or recruit coactivators to the ligand-binding domains of hCAR-WT and hCAR-SV23, whereas positive results were obtained with the controls (CITCO for hCAR-WT and DEHP for hCAR-SV23). In conclusion, G. biloba extract activates hCAR in an isoform-selective manner, and hCAR-SV23, hCAR-SV24, and hCAR-WT have overlapping, but distinct, sets of ligands.

摘要

天然存在的人组成型雄烷受体(hCAR)剪接变体,包括 hCAR-SV23(插入 SPTV 氨基酸)、hCAR-SV24(APYLT)和 hCAR-SV25(SPTV 和 APYLT)。银杏叶提取物被报道能激活 hCAR-SV24 和野生型(hCAR-WT)。然而,目前尚不清楚它是否选择性地影响 hCAR 剪接变体,它如何激活 hCAR 同工型,以及提取物中的哪种化学物质是其作用的原因。因此,我们评估了银杏叶提取物对 hCAR-SV23、hCAR-SV24、hCAR-SV25 和 hCAR-WT 功能的影响,并将其与苯巴比妥、邻苯二甲酸二(2-乙基己基)酯(DEHP)、6-(4-氯苯基)咪唑[2,1-b][1,3]噻唑-5-甲酰醛 O-(3,4-二氯苄基)肟(CITCO)和 1,4-双-[2-(3,5-二氯吡啶基氧基)]苯(TCPOBOP)进行了比较在基于细胞的报告基因检测中。在所研究的 hCAR 剪接变体中,只有 hCAR-SV23 被银杏叶提取物激活,并且这需要共转染视黄醇 X 受体α(RXRα)表达质粒。提取物对 hCAR-SV23 的激活作用小于 hCAR-WT,但银杏内酯 A、银杏内酯 B、银杏内酯 C、银杏内酯 J 和白果内酯不是提取物作用的原因。CITCO 激活 hCAR-SV23、hCAR-SV24 和 hCAR-WT。相比之下,苯巴比妥激活 hCAR-WT,而 DEHP 激活 hCAR-SV23、hCAR-SV24(外源性 RXRα 补充)和 hCAR-WT。TCPOBOP 对任何同工型的活性都没有影响。银杏叶提取物和苯巴比妥不能与 hCAR-WT 和 hCAR-SV23 的配体结合域结合或募集共激活因子,而对照(CITCO 用于 hCAR-WT 和 DEHP 用于 hCAR-SV23)则得到阳性结果。总之,银杏叶提取物以同工型选择性的方式激活 hCAR,hCAR-SV23、hCAR-SV24 和 hCAR-WT 具有重叠但不同的配体集。

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