Transcriptional regulation of human hydroxysteroid sulfotransferase SULT2A1 by LXR&#945;.

Ou, Zhimin; Jiang, Mengxi; Hu, Bingfang; Huang, Yixian; Xu, Meishu; Ren, Songrong; Li, Song; Liu, Suhuan; Xie, Wen; Huang, Min

Transcriptional regulation of human hydroxysteroid sulfotransferase SULT2A1 by LXRα.

Ou, Zhimin; Jiang, Mengxi; Hu, Bingfang; Huang, Yixian; Xu, Meishu; Ren, Songrong; Li, Song; Liu, Suhuan; Xie, Wen; Huang, Min.

Affiliation

Ou Z; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Jiang M; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Hu B; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Huang Y; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Xu M; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Ren S; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Li S; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Liu S; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Xie W; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg
Huang M; Institute of Clinical Pharmacology, Sun Yat-Sen University, Guangzhou, China (Z.O., B.H., M.H.); Center for Pharmacogenetics and Department of Pharmaceutical Sciences (Z.O., M.J., B.H., Y.H., M.X., S.R., So.L., W.X.) and Department of Pharmacology and Chemical Biology (W.X.), University of Pittsburg

Drug Metab Dispos ; 42(10): 1684-9, 2014 Oct.

Article in En | MEDLINE | ID: mdl-25028566

ABSTRACT

ABSTRACT

The nuclear receptor liver X receptor (LXR) plays an important role in the metabolism and homeostasis of cholesterol, lipids, bile acids, and steroid hormones. In this study, we uncovered a function of LXRα (NR1H3) in regulating the human hydroxysteroid sulfotransferase SULT2A1, a phase II conjugating enzyme known to sulfonate bile acids, hydroxysteroid dehydroepiandrosterone, and related androgens. We showed that activation of LXR induced the expression of SULT2A1 at mRNA, protein, and enzymatic levels. A combination of promoter reporter gene and chromatin immunoprecipitation assays showed that LXRα transactivated the SULT2A1 gene promoter through its specific binding to the -500- to -258-base pair region of the SULT2A1 gene promoter. LXR small interfering RNA knockdown experiments suggested that LXRα, but not LXRß, played a dominant role in regulating SULT2A1. In primary human hepatocytes, we found a positive correlation between the expression of SULT2A1 and LXRα, which further supported the regulation of SULT2A1 by LXRα. In summary, our results established human SULT2A1 as a novel LXRα target gene. The expression of LXRα is a potential predictor for the expression of SULT2A1 in human liver.

Subject(s)

Gene Expression Regulation; Orphan Nuclear Receptors/metabolism; Sulfotransferases/genetics; Transcription, Genetic; Cells, Cultured; Gene Expression Regulation/drug effects; Hepatocytes/metabolism; Humans; Liver X Receptors; Promoter Regions, Genetic/genetics; Protein Isoforms/metabolism; RNA, Small Interfering/pharmacology; Transcription, Genetic/drug effects

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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Transcription, Genetic / Sulfotransferases / Gene Expression Regulation / Orphan Nuclear Receptors Limits: Humans Language: En Journal: Drug Metab Dispos Year: 2014 Document type: Article

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