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CYP3A4 mRNA 转录本具有缩短的 3'-非翻译区在肝细分化、肝脏发育和药物诱导反应中的作用。

The role of CYP3A4 mRNA transcript with shortened 3'-untranslated region in hepatocyte differentiation, liver development, and response to drug induction.

机构信息

Department of Pharmacology, Toxicology, and Therapeutics, University of Kansas Medical Center, Kansas City, Kansas 66160, USA.

出版信息

Mol Pharmacol. 2012 Jan;81(1):86-96. doi: 10.1124/mol.111.074393. Epub 2011 Oct 13.

Abstract

Cytochrome P450 3A4 (CYP3A4) metabolizes more than 50% of prescribed drugs. The expression of CYP3A4 changes during liver development and may be affected by the administration of some drugs. Alternative mRNA transcripts occur in more than 90% of human genes and are frequently observed in cells responding to developmental and environmental signals. Different mRNA transcripts may encode functionally distinct proteins or contribute to variability of mRNA stability or protein translation efficiency. The purpose of this study was to examine expression of alternative CYP3A4 mRNA transcripts in hepatocytes in response to developmental signals and drugs. cDNA cloning and RNA sequencing (RNA-Seq) were used to identify CYP3A4 mRNA transcripts. Three transcripts were found in HepaRG cells and liver tissues: one represented a canonical mRNA with full-length 3'-untranslated region (UTR), one had a shorter 3'-UTR, and one contained partial intron-6 retention. The alternative mRNA transcripts were validated by either rapid amplification of cDNA 3'-end or endpoint polymerase chain reaction (PCR). Quantification of the transcripts by RNA-Seq and real time quantitative PCR revealed that the CYP3A4 transcript with shorter 3'-UTR was preferentially expressed in developed livers, differentiated hepatocytes, and in rifampicin- and phenobarbital-induced hepatocytes. The CYP3A4 transcript with shorter 3'-UTR was more stable and produced more protein compared with the CYP3A4 transcript with canonical 3'-UTR. We conclude that the 3'-end processing of CYP3A4 contributes to the quantitative regulation of CYP3A4 gene expression through alternative polyadenylation, which may serve as a regulatory mechanism explaining changes of CYP3A4 expression and activity during hepatocyte differentiation and liver development and in response to drug induction.

摘要

细胞色素 P450 3A4(CYP3A4)代谢超过 50%的处方药。CYP3A4 的表达在肝发育过程中发生变化,并且可能受某些药物的给药影响。替代 mRNA 转录本存在于超过 90%的人类基因中,并且在响应发育和环境信号的细胞中经常观察到。不同的 mRNA 转录本可能编码功能上不同的蛋白质,或者有助于 mRNA 稳定性或蛋白质翻译效率的变异性。本研究的目的是研究替代 CYP3A4 mRNA 转录本在肝细胞中对发育信号和药物的反应。cDNA 克隆和 RNA 测序(RNA-Seq)用于鉴定 CYP3A4 mRNA 转录本。在 HepaRG 细胞和肝组织中发现了三种转录本:一种代表具有全长 3'-非翻译区(UTR)的典型 mRNA,一种具有较短的 3'-UTR,一种含有部分内含子-6 保留。通过快速扩增 cDNA 3'-末端或终点聚合酶链反应(PCR)验证替代 mRNA 转录本。通过 RNA-Seq 和实时定量 PCR 对转录本进行定量,发现具有较短 3'-UTR 的 CYP3A4 转录本在发育中的肝脏、分化的肝细胞以及利福平诱导的和苯巴比妥诱导的肝细胞中优先表达。与具有典型 3'-UTR 的 CYP3A4 转录本相比,具有较短 3'-UTR 的 CYP3A4 转录本更稳定且产生更多的蛋白质。我们得出结论,CYP3A4 的 3'-末端加工通过可变多聚腺苷酸化有助于 CYP3A4 基因表达的定量调节,这可能是解释 CYP3A4 表达和活性在肝细胞分化和肝发育过程中以及在药物诱导时变化的调节机制。

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