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多氯联苯126刺激人肾上腺皮质H295R细胞的基础和诱导性醛固酮生物合成。

Polychlorinated biphenyl 126 stimulates basal and inducible aldosterone biosynthesis of human adrenocortical H295R cells.

作者信息

Li Lih-Ann, Wang Pei-Wen, Chang Louis W

机构信息

Division of Environmental Health and Occupational Medicine, National Health Research Institutes, Kao-hsiung 807, Taiwan, ROC.

出版信息

Toxicol Appl Pharmacol. 2004 Feb 15;195(1):92-102. doi: 10.1016/j.taap.2003.11.007.

Abstract

To understand the effects of polychlorinated biphenyls (PCBs) on adrenal aldosterone biosynthesis, we have performed a systematical study to characterize the corresponding steroidogenic response of human adrenocortical cell line H295R to PCB126 exposure. We found that PCB126 at high concentrations stimulated basal and inducible aldosterone production. The aldosterone induction occurred concomitantly with activation of the CYP11B2 gene. Despite the fact that PCB126 acted in synergy with both potassium and angiotensin II (Ang II) in activation of aldosterone synthesis, PCB126 only modestly increased CYP11B2 mRNA expression in the presence of Ang II contrary to the synergistic transcriptional induction elicited by PCB126 and potassium. This implicated that PCB126 had differential interactions with the potassium and Ang II signaling systems in the regulation of aldosterone biosynthesis. In addition, high concentrations of PCB126 elevated transcriptional expression of the type I Ang II receptor (AT(1)) and might thus sensitize the cellular Ang II responsiveness in both basal and inducible aldosterone biosynthesis. SF-1 was not involved in the PCB126-induced transcriptional regulation despite its importance in steroidogenic gene activation.

摘要

为了解多氯联苯(PCBs)对肾上腺醛固酮生物合成的影响,我们进行了一项系统性研究,以表征人肾上腺皮质细胞系H295R对PCB126暴露的相应类固醇生成反应。我们发现,高浓度的PCB126刺激了基础和诱导性醛固酮的产生。醛固酮的诱导与CYP11B2基因的激活同时发生。尽管PCB126在醛固酮合成激活过程中与钾和血管紧张素II(Ang II)协同作用,但与PCB126和钾引发的协同转录诱导相反,在存在Ang II的情况下,PCB126仅适度增加CYP11B2 mRNA表达。这表明PCB126在醛固酮生物合成调节中与钾和Ang II信号系统存在不同的相互作用。此外,高浓度的PCB126提高了I型Ang II受体(AT(1))的转录表达,因此可能在基础和诱导性醛固酮生物合成中使细胞对Ang II的反应性敏感。尽管SF-1在类固醇生成基因激活中很重要,但它不参与PCB126诱导的转录调节。

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