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克隆和鉴定石磺视黄酸受体样蛋白。

Cloning and characterization of the retinoic acid receptor-like protein in the rock shell, Thais clavigera.

机构信息

Center for Environmental Risk Research, National Institute for Environmental Studies, 16-2 Onogawa, Tsukuba, Ibaraki 305-8506, Japan.

出版信息

Aquat Toxicol. 2013 Oct 15;142-143:403-13. doi: 10.1016/j.aquatox.2013.09.008. Epub 2013 Sep 16.

DOI:10.1016/j.aquatox.2013.09.008
PMID:24096236
Abstract

The organotin compounds have a high affinity for the retinoid X receptor (RXR), which is a transcriptional factor activated by retinoids that induce imposex in gastropods. However, the molecular mechanisms underlying the regulation of RXR and its related genes in gastropods remain unclear. We isolated a retinoic acid receptor (RAR)-like cDNA (TcRAR) in the rock shell, Thais clavigera, and examined the transcriptional activity of the TcRAR protein by using all-trans retinoic acid (ATRA). However, we did not observe any ligand-dependent transactivation by this protein. We also examined the transcriptional activity of the TcRAR-ligand binding domain fused with the GAL4-DNA binding domain by using retinoic acids, retinol, and organotins and again saw no noteworthy transcriptional induction by these chemicals. Use of a mammalian two-hybrid assay to assess the interaction of the TcRAR protein with the TcRXR isoforms suggested that TcRAR might form a heterodimer with the RXR isoforms. The transcriptional activity of domain-swapped TcRAR chimeric proteins (the A/B domain of TcRAR combined with the D-F domain of human RARα) was also examined and found to be ATRA-dependent. These results suggest that TcRAR is not activated by retinoic acids, but can form a heterodimer with TcRXR isoforms. These data contribute to our understanding of the mechanism by which RXR functions in gastropods.

摘要

有机锡化合物对维甲酸 X 受体 (RXR) 具有很高的亲和力,RXR 是一种被维甲酸激活的转录因子,能诱导腹足类动物出现雌雄同体现象。然而,腹足类动物中 RXR 及其相关基因的调控的分子机制尚不清楚。我们从石磺中分离出一种视黄酸受体 (RAR)-样 cDNA (TcRAR),并使用全反式视黄酸 (ATRA) 检测了 TcRAR 蛋白的转录活性。然而,我们没有观察到该蛋白的任何配体依赖性的反式激活。我们还使用视黄酸、视黄醇和有机锡检查了与 GAL4-DNA 结合域融合的 TcRAR 配体结合域的转录活性,这些化学物质也没有引起明显的转录诱导。使用哺乳动物双杂交测定法评估 TcRAR 蛋白与 TcRXR 同工型的相互作用表明,TcRAR 可能与 RXR 同工型形成异二聚体。还检查了域交换的 TcRAR 嵌合蛋白 (TcRAR 的 A/B 结构域与人类 RARα的 D-F 结构域) 的转录活性,发现其依赖于 ATRA。这些结果表明 TcRAR 不能被视黄酸激活,但可以与 TcRXR 同工型形成异二聚体。这些数据有助于我们理解 RXR 在腹足类动物中发挥作用的机制。

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