Genomic characterization and regulation of CYP3a13: role of xenobiotics and nuclear receptors

被引:28
作者
Anakk, S
Kalsotra, A
Shen, Q
Vu, MT
Staudinger, JL
Davies, PJA
Strobel, HW
机构
[1] Univ Texas, Sch Med, Dept Biochem & Mol Biol, Houston, TX 77225 USA
[2] Univ Texas, Sch Med, Dept Integrat Biol, Houston, TX 77225 USA
[3] Univ Kansas, Med Ctr, Dept Pharmacol & Toxicol, Lawrence, KS 66045 USA
关键词
cytochrome P4503A; drug metabolism; sexual dimorphism; nuclear receptors;
D O I
10.1096/fj.02-1004fje
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
We report that CYP3a13 gene, located on mouse chromosome 5, spans 27.5 Kb and contains 13 exons. The transcription start site is 35 bp upstream of the coding region and results in a 109 bp 5' untranslated region. CYP3a13 promoter shows putative binding sites for retinoid X receptor, pregnane X receptor, and estrogen receptor. CYP3a13 shows a broad tissue distribution with predominant expression in liver. Although CYP3a13 shares 92% nucleotide identity with the female-specific rat CYP3A9, its expression does not exhibit sexual dimorphism. Ligand activation of peroxisomal proliferator-activated receptor-gamma and retinoid X receptor inhibit expression of CYP3a13 at the transcription level in a tissue-specific manner. Another novel finding is hepatic induction of CYP3a13 by dexamethasone occurring only in pregnane X receptor null mice. We also report that pregnane X receptor is essential to maintain robust in vivo basal levels of CYP3a13 in contrast to CYP3a11. CYP3a13 protein expressed in vitro can metabolize clinically active drugs ethylmorphine and erythromycin, as well as benzphetamine. We conclude that CYP3a13 is regulated differentially by various nuclear receptors. In humans this may lead to altered drug metabolism, as many of the newly synthesized ligands/drugs targeted toward these nuclear receptors could influence CYP3A gene expression.
引用
收藏
页码:1736 / +
页数:23
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