Lee Jin-Seon, Kim Eun-Young, Iwata Hisato, Tanabe Shinsuke
Center for Marine Environmental Studies (CMES), Ehime University, Bunkyo-cho 2-5, Matsuyama 790-8577, Ehime, Japan.
Comp Biochem Physiol C Toxicol Pharmacol. 2007 Apr;145(3):379-93. doi: 10.1016/j.cbpc.2007.01.007. Epub 2007 Jan 30.
High levels of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) and related planar halogenated aromatic hydrocarbons (PHAHs) are accumulated in fish-eating birds including common cormorant (Phalacrocorax carbo). Most of the biochemical and toxic effects of TCDD are mediated by a basic helix-loop-helix and a conserved region among Per, ARNT, and Sim (bHLH/PAS) proteins, aryl hydrocarbon receptor (AHR) and AHR nuclear translocator (ARNT). To study the molecular mechanism of TCDD toxicity in common cormorant as an avian model species, characterization of the AHR/ARNT signaling pathway in this species is necessary. The present study focuses on molecular characterization of ARNT from common cormorant (ccARNT). The cDNA of the ccARNT isoform, ccARNT1 obtained by the screening of hepatic cDNA library contains a 2424-bp open reading frame that encodes 807 amino acids, exhibiting high identities (92%) with chicken ARNT. This isoform contains a unique 22 amino acid residue in 3' end of PAS A domain as is also recognized in chicken ARNT. The ccARNT2 cDNA isolated from brain tissue has a 2151-bp open reading frame. The deduced amino acid sequence of ccARNT2 protein (716 aa) shows a conservation of bHLH and PAS motif in its N-terminal region with high similarities (96% and 78%, respectively) to that of ccARNT1. Using quantitative RT-PCR methods, the tissue distribution profiles of ccARNT1 and ccARNT2 were unveiled. Both ccARNT1 and ccARNT2 mRNAs were ubiquitously expressed in all examined tissues including liver. The expression profile of ccARNT1 was comparable with that of rodent ARNT1, but ccARNT2 was not with rodent ARNT2, implying different roles of ARNT2 between the two species. There was a significant positive correlation between ARNT1 and ARNT2 mRNA expression levels in the liver of wild cormorant population, indicating that their expressions may be enforced by similar transcriptional regulation mechanism. Novel variants of ccARNT1 and ccARNT2 isoforms that were supposed to arise from their splicing process were also identified and their hepatic expression profiles were determined. These results indicate that ccARNT1, ccARNT2 and their splice variants may more intricately regulate the AHR/ARNT signaling pathway and consequently may be responsible for the species diversity of toxic effects and susceptibility to PHAHs.
高浓度的2,3,7,8 - 四氯二苯并 - 对 - 二噁英(TCDD)及相关平面卤代芳烃(PHAHs)在以鱼类为食的鸟类(包括普通鸬鹚(Phalacrocorax carbo))体内蓄积。TCDD的大多数生化和毒性作用是由Per、ARNT和Sim(bHLH/PAS)蛋白、芳烃受体(AHR)和AHR核转运体(ARNT)中的一个碱性螺旋 - 环 - 螺旋和一个保守区域介导的。为了研究作为鸟类模式物种的普通鸬鹚中TCDD毒性的分子机制,有必要对该物种中的AHR/ARNT信号通路进行表征。本研究聚焦于普通鸬鹚ARNT(ccARNT)的分子表征。通过筛选肝脏cDNA文库获得的ccARNT亚型ccARNT1的cDNA包含一个2424 bp的开放阅读框,编码807个氨基酸,与鸡ARNT具有高度同源性(92%)。该亚型在PAS A结构域的3'端含有一个独特的22个氨基酸残基,鸡ARNT中也有此特征。从脑组织中分离出的ccARNT2 cDNA有一个2151 bp的开放阅读框。推导的ccARNT2蛋白氨基酸序列(716个氨基酸)在其N端区域显示出bHLH和PAS基序的保守性,与ccARNT1的相似性较高(分别为96%和78%)。使用定量RT - PCR方法,揭示了ccARNT1和ccARNT2的组织分布情况。ccARNT1和ccARNT2的mRNA在包括肝脏在内的所有检测组织中均有广泛表达。ccARNT1的表达谱与啮齿动物ARNT1的相似,但ccARNT2与啮齿动物ARNT2不同,这意味着ARNT2在这两个物种中发挥不同作用。野生鸬鹚种群肝脏中ARNT1和ARNT2 mRNA表达水平之间存在显著正相关,表明它们的表达可能受相似的转录调控机制影响。还鉴定了推测由剪接过程产生的ccARNT1和ccARNT2亚型的新变体,并确定了它们在肝脏中的表达谱。这些结果表明,ccARNT1、ccARNT2及其剪接变体可能更复杂地调节AHR/ARNT信号通路,因此可能是毒性效应物种多样性和对PHAHs易感性的原因。
