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Alterations in Hepatic mRNA Expression of Phase II Enzymes and Xenobiotic Transporters after Targeted Disruption of Hepatocyte Nuclear Factor 4 Alpha

机译:靶向破坏肝细胞核因子4α后,II期酶和异源生物转运蛋白肝mRNA表达的变化。

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摘要

Hepatocyte nuclear factor 4 alpha (HNF4a) is a liver-enriched master regulator of liver function. HNF4a is important in regulating hepatic expression of certain cytochrome P450s. The purpose of this study was to use mice lacking HNF4a expression in liver (HNF4a-HNull) to elucidate the role of HNF4a in regulating hepatic expression of phase II enzymes and transporters in mice. Compared with male wild-type mice, HNF4a-HNull male mouse livers had (1) markedly lower messenger RNAs (mRNAs) encoding the uptake transporters sodium taurocholate cotransporting polypeptide, organic anion transporting polypeptide (Oatp) 1a1, Oatp2b1, organic anion transporter 2, sodium phosphate cotransporter type 1, sulfate anion transporter 1, sodium-dependent vitamin C transporter 1, the phase II enzymes Uridine 5′-diphospho (UDP)-glucuronosyltransferase (Ugt) 2a3, Ugt2b1, Ugt3a1, Ugt3a2, sulfotransferase (Sult) 1a1, Sult1b1, Sult5a1, the efflux transporters multidrug resistance–associated protein (Mrp) 6, and multidrug and toxin extrusion 1; (2) moderately lower mRNAs encoding Oatp1b2, organic cation transporter (Oct) 1, Ugt1a5, Ugt1a9, glutathione S-transferase (Gst) m4, Gstm6, and breast cancer resistance protein; but (3) higher mRNAs encoding Oatp1a4, Octn2, Ugt1a1, Sult1e1, Sult2a2, Gsta4, Gstm1-m3, multidrug resistance protein (Mdr) 1a, Mrp3, and Mrp4. Hepatic signaling of nuclear factor E2–related factor 2 and pregnane X receptor appear to be activated in HNF4a-HNull mice. In conclusion, HNF4a deficiency markedly alters hepatic mRNA expression of a large number of phase II enzymes and transporters, probably because of the loss of HNF4a, which is a transactivator and a determinant of gender-specific expression and/or adaptive activation of signaling pathways important in hepatic regulation of these phase II enzymes and transporters.
机译:肝细胞核因子4α(HNF4a)是肝脏功能丰富的肝脏主要调节剂。 HNF4a在调节某些细胞色素P450的肝表达中很重要。这项研究的目的是使用在肝脏中缺乏HNF4a表达的小鼠(HNF4a-HNull)来阐明HNF4a在调节小鼠II期酶和转运蛋白的肝表达中的作用。与雄性野生型小鼠相比,HNF4a-HNull雄性小鼠肝脏具有(1)较低的信使RNA(mRNA),其编码摄取转运蛋白牛磺胆酸钠共转运多肽,有机阴离子转运多肽(Oatp)1a1,Oatp2b1,有机阴离子转运蛋白2,磷酸钠共转运蛋白1,硫酸盐阴离子转运蛋白1,钠依赖性维生素C转运蛋白1,II期酶尿苷5'-二磷酸(UDP)-葡萄糖醛酸转移酶(Ugt)2a3,Ugt2b1,Ugt3a1,Ugt3a2,磺基转移酶(Sult)1a1, Sult1b1,Sult5a1,外排转运蛋白多药耐药相关蛋白(Mrp)6,多药和毒素挤出1; (2)编码Oatp1b2,有机阳离子转运蛋白(Oct)1,Ugt1a5,Ugt1a9,谷胱甘肽S-转移酶(Gst)m4,Gstm6和乳腺癌抗性蛋白的mRNA较低;但是(3)编码Oatp1a4,Octn2,Ugt1a1,Sult1e1,Sult2a2,Gsta4,Gstm1-m3,多药耐药蛋白(Mdr)1a,Mrp3和Mrp4的更高mRNA。 HNF4a-HNull小鼠似乎激活了核因子E2相关因子2和孕烷X受体的肝信号。总之,HNF4a缺乏症会明显改变大量II期酶和转运蛋白的肝mRNA表达,这可能是由于HNF4a的丢失引起的,HNF4a是一种反式激活因子,是性别特异性表达和/或信号通路适应性激活的决定因素。这些II期酶和转运蛋白的肝调节作用。

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