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首页> 外文期刊>The Biochemical Journal >Co-planar 3,3',4,4',5-pentachlorinated biphenyl and non-co-planar 2,2',4,6,6'-pentachlorinated biphenyl differentially induce recruitment of oestrogen receptor alpha to aryl hydrocarbon receptor target genes.

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Co-planar 3,3',4,4',5-pentachlorinated biphenyl and non-co-planar 2,2',4,6,6'-pentachlorinated biphenyl differentially induce recruitment of oestrogen receptor alpha to aryl hydrocarbon receptor target genes.

机译：共平面3,3'，4,4'，5-五氯联苯和非共平面2,2'，4,6,6'-五氯联苯差异诱导雌激素受体α募集至芳烃受体靶基因。

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In the present study we examined the ability of 3,3',4,4',5-pentachlorinated biphenyl [PCB126 (polychlorinated biphenyl 126)], a prototypical AHR (aryl hydrocarbon receptor) agonist, and 2,2',4,6,6'-PCB (PCB104), which does not activate AHR, to induce the recruitment of ERalpha (oestrogen receptor alpha) to CYP1A1 (cytochrome P4501A1 gene) and CYP1B1 promoters in T-47D human breast cancer cells and other cell lines. PCB126 treatment strongly induced CYP1A1 and CYP1B1 mRNA expression that was unaffected by co-treatment with E2 (17beta-oestradiol). PCB104 failed to induce changes in either CYP1A1 or CYP1B1 expression levels. ChIP (chromatin immunoprecipitation) assays show that PCB126, but not PCB104, increased the promoter occupancy by ERalpha to CYP1A1 and CYP1B1 promoters. Co-treatment with PCB126+E2 significantly enhanced the promoter occupancy of ERalpha at CYP1A1, whereas co-treatment with PCB126+4-hydroxytamoxifen or ICI182,780 did not. Competitive binding studies revealed that neither PCB126 nor PCB104 bound to ERalpha. HEK-293 cells (human embryonic kidney-293 cells) stably transfected with ERalpha showed significantly higher PCB126-induced CYP1A1 expression compared with empty vector controls, whereas no increase was observed in cells stably transfected with ERalpha lacking its N-terminal AF1 (activation function-1) domain (ERalphaDeltaAF1). Despite no increase in AHR-mediated gene expression, ChIP assays revealed that ERalphaDeltaAF1 was present at CYP1A1 and CYP1B1 promoters. HC11 mouse mammary cells stably expressing shRNA (small-hairpin RNA) against ERalpha showed an 8-fold reduction in PCB126-dependent Cyp1a1 expression. Our results provide further evidence that AHR agonists induce ERalpha promoter occupancy at AHR target genes through indirect activation of ERalpha, and support a role for ERalpha in AHR transactivation.

机译：在本研究中，我们研究了原型AHR（芳烃受体）激动剂3,3'，4,4'，5-五氯联苯[PCB126（polychlorinated biphenyl 126）]和2,2'，4的能力， 6,6'-PCB（PCB104）不会激活AHR，从而诱导ERalpha（雌激素受体α）募集到T-47D人乳腺癌细胞和其他细胞系中的CYP1A1（细胞色素P4501A1基因）和CYP1B1启动子。 PCB126处理强烈诱导CYP1A1和CYP1B1 mRNA表达，而与E2（17β-雌二醇）共同处理不受影响。 PCB104无法诱导CYP1A1或CYP1B1表达水平的变化。 ChIP（染色质免疫沉淀）测定法显示，PCB126，而不是PCB104，增加了ERalpha对CYP1A1和CYP1B1启动子的启动子占有率。与PCB126 + E2共同处理可显着增强ERalpha在CYP1A1的启动子占有率，而与PCB126 + 4-羟基他莫昔芬或ICI182,780共同处理则不会。竞争性结合研究表明，PCB126和PCB104均未结合ERalpha。稳定转染ERalpha的HEK-293细胞（人胚肾293细胞）与空载体对照相比显示出明显更高的PCB126诱导的CYP1A1表达，而在缺少N末端AF1的ERalpha稳定转染的细胞中未观察到增加（激活功能-1）域（ERalphaDeltaAF1）。尽管AHR介导的基因表达没有增加，但ChIP分析显示ERalphaDeltaAF1存在于CYP1A1和CYP1B1启动子上。稳定表达针对ERalpha的shRNA（小发夹RNA）的HC11小鼠乳腺细胞显示PCB126依赖性Cyp1a1表达降低了8倍。我们的结果提供了进一步的证据，表明AHR激动剂通过间接激活ERalpha来诱导AHR目标基因上的ERalpha启动子占据，并支持ERalpha在AHR反式激活中的作用。

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来源
《The Biochemical Journal》 |2007年第2期|共11页
作者
Matthews J; Wihlen B; Heldring N; MacPherson L; Helguero L; Treuter E; Haldosen LA; Gustafsson JA;
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正文语种 eng
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关键词
Estrogen Receptor alpha; Polychlorinated Biphenyls; Receptors; Aryl Hydrocarbon; 多氯联苯化合物; 受体; 芳基烃;

机译：Estrogen Receptor alpha;Polychlorinated Biphenyls;Receptors;Aryl Hydrocarbon;多氯联苯化合物;受体;芳基烃;

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1. Co-planar 3,3',4,4',5-pentachlorinated biphenyl and non-co-planar 2,2',4,6,6'-pentachlorinated biphenyl differentially induce recruitment of oestrogen receptor alpha to aryl hydrocarbon receptor target genes. [J] . Matthews J, Wihlen B, Heldring N, The Biochemical Journal . 2007,第2期

机译：共平面3,3'，4,4'，5-五氯联苯和非共平面2,2'，4,6,6'-五氯联苯差异诱导雌激素受体α募集至芳烃受体靶基因。
2. 2,2',3,3',4,4'-Hexahydroxy-1,1'-biphenyl-6,6'-dimethanol dimethyl ether (HBDDE)-induced neuronal apoptosis independent of classical protein kinase C alpha or gamma inhibition. [J] . Mathur A, Vallano ML Biochemical Pharmacology . 2000,第6期

机译：2,2'，3,3'，4,4'-己羟基-1,1'-联苯-6,6'-二甲醇二甲醚（HBDDE）诱导的神经元凋亡，独立于经典的蛋白激酶Cα或γ抑制。
3. The aryl hydrocarbon receptor agonist 3,3',4,4',5-pentachlorobiphenyl induces distinct patterns of gene expression between hepatoma and glioma cells: chromatin remodeling as a mechanism for selective effects. [J] . Maier MS, Legare ME, Hanneman WH Neurotoxicology . 2007,第3期

机译：芳基烃受体激动剂3,3'，4,4'，5-五氯联苯诱导肝癌和神经胶质瘤细胞之间基因表达的不同模式：染色质重塑作为选择性作用的机制。
4. New insights into the 3-methylcholanthrene-induced chromatin binding profiles of aryl hydrocarbon and estrogen receptor alpha. [D] . Pansoy, Andrea Josephine. 2009

机译：对3-甲基胆甾醇诱导的芳烃和雌激素受体α的染色质结合谱的新见解。
5. Co-planar 33′44′5-pentachlorinated biphenyl and non-co-planar 22′466′-pentachlorinated biphenyl differentially induce recruitment of oestrogen receptor α to aryl hydrocarbon receptor target genes [O] . Jason Matthews, Björn Wihlén, Nina Heldring, 2007

机译：共平面33445-五氯联苯和非共平面22466-五氯联苯差异诱导雌激素受体α募集至芳烃受体靶基因
6. Co-planar 3,3′,4,4′,5-pentachlorinated biphenyl and non-co-planar 2,2′,4,6,6′-pentachlorinated biphenyl differentially induce recruitment of oestrogen receptor α to aryl hydrocarbon receptor target genes [O] . Matthews, Jason, Wihlén, Björn, Heldring, Nina, 2007

机译：共平面3,3'，4,4'，5-五氯联苯和非共平面2,2'，4,6,6'-五氯联苯差异诱导雌激素受体α募集至芳烃受体靶基因

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