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雌激素对大鼠神经胶质细胞中类固醇代谢的介导调节;通过调控细胞色素P450 7B1介导的催化作用对神经甾体水平的影响。

Estrogen-mediated regulation of steroid metabolism in rat glial cells; effects on neurosteroid levels via regulation of CYP7B1-mediated catalysis.

作者信息

Wicher Grzegorz, Norlin Maria

机构信息

Department of Pharmaceutical Biosciences, Uppsala University, Sweden.

Department of Pharmaceutical Biosciences, Uppsala University, Sweden.

出版信息

J Steroid Biochem Mol Biol. 2015 Jan;145:21-7. doi: 10.1016/j.jsbmb.2014.09.022. Epub 2014 Sep 26.

Abstract

Many neuroactive steroids, including dehydroepiandrosterone (DHEA), pregnenolone, 27-hydroxycholesterol and 17β-estradiol, are known to affect development and function of the brain and nervous system. These and other steroids can undergo tissue and/or cell-specific enzymatic conversions into steroid metabolites. Carefully regulated production of steroids with various physiological effects is important for cells of the nervous system. Astrocytes express many steroidogenic enzymes and are considered important producers of brain steroids. The quantitative roles of different pathways for steroid metabolism in rat astrocytes are not clear. In the current study we examined effects of estrogens on steroid metabolism catalyzed by CYP7B1 and other enzymes in primary cultures of rat astrocytes. The CYP7B1 enzyme, which has been linked to neurodegenerative disease, is involved in the metabolism of several important neurosteroids. In the present study, we found that 7α-hydroxylation, performed by CYP7B1, is the quantitatively most important pathway for DHEA metabolism in rat astrocytes. In addition, our present experiments on catalytic steroid conversions revealed that estrogens significantly suppress the CYP7B1-catalyzed metabolism of not only DHEA but also of pregnenolone and 27-hydroxycholesterol in rat astrocytes. These novel findings point to a regulatory mechanism for control of the cellular levels of these neurosteroids via CYP7B1. Our hypothesis that estrogens can regulate neurosteroid levels via this enzymatic reaction was supported by experiments using ELISA to assay levels of DHEA and pregnenolone in the presence or absence of estrogen. Furthermore, the present results show that estrogen suppresses CYP7B1-catalyzed 7α-hydroxylation also in primary cultures of rat Schwann cells, indicating that regulation by estrogen via this enzyme may be of relevance in both the CNS and the PNS.

摘要

许多神经活性甾体,包括脱氢表雄酮(DHEA)、孕烯醇酮、27-羟基胆固醇和17β-雌二醇,已知会影响大脑和神经系统的发育与功能。这些以及其他甾体可在组织和/或细胞特异性酶的作用下转化为甾体代谢产物。对具有各种生理效应的甾体进行严格调控的生成过程,对神经系统细胞而言至关重要。星形胶质细胞表达多种甾体生成酶,被认为是脑甾体的重要生成者。大鼠星形胶质细胞中不同甾体代谢途径的定量作用尚不清楚。在本研究中,我们检测了雌激素对大鼠星形胶质细胞原代培养物中由CYP7B1和其他酶催化的甾体代谢的影响。CYP7B1酶与神经退行性疾病有关,参与几种重要神经甾体的代谢。在本研究中,我们发现由CYP7B1进行的7α-羟基化是大鼠星形胶质细胞中DHEA代谢的定量上最重要的途径。此外,我们目前关于催化甾体转化的实验表明,雌激素显著抑制大鼠星形胶质细胞中CYP7B1催化的不仅是DHEA,还有孕烯醇酮和27-羟基胆固醇的代谢。这些新发现指出了一种通过CYP7B1控制这些神经甾体细胞水平的调节机制。我们关于雌激素可通过这种酶促反应调节神经甾体水平的假设,通过使用ELISA测定有无雌激素时DHEA和孕烯醇酮水平的实验得到了支持。此外,目前的结果表明,雌激素在大鼠雪旺细胞原代培养物中也抑制CYP7B1催化的7α-羟基化,这表明雌激素通过该酶的调节在中枢神经系统和外周神经系统中可能都具有相关性。

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