Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon beta in Toll-Like Receptor 3-and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes

Shah Pranav; Omoluabi Ozozoma; Moorthy Bhagavatula; Ghose Romi

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Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon beta in Toll-Like Receptor 3-and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes

机译：衔接子蛋白类似收费的白介素域包含适配器诱导干扰素β在收费象受体3和4介导的肝药物代谢酶和转运蛋白调控中的作用

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The expressions and activities of hepatic drug-metabolizing enzymes and transporters (DMETs) are altered during infection and inflammation. Inflammatory responses in the liver are mediated primarily by Toll-like receptor (TLR)-signaling, which involves recruitment of Toll/interleukin (IL)-1 receptor (TIR) domain containing adaptor protein (TIRAP) and TIR domain containing adaptor inducing interferon (IFN)-beta (TRIF) that eventually leads to induction of proinflammatory cytokines and mitogen-activated protein kinases (MAPKs). Lipopolysaccharide (LPS) activates the Gram-negative bacterial receptor TLR4 and polyinosinic: polycytidylic acid (polyI:C) activates the viral receptor TLR3. TLR4 signaling involves TIRAP and TRIF, whereas TRIF is the only adaptor protein involved in the TLR3 pathway. We have shown previously that LPS-mediated downregulation of DMETs is independent of TIRAP. To determine the role of TRIF, we treated TRIF+/+ and TRIF-/- mice with LPS or polyI: C. LPS downregulated (similar to 40%-60%) Cyp3a11, Cyp2a4, Ugt1a1, Mrp2 mRNA levels, whereas polyI: C downregulated (similar to 30%-60%) Cyp3a11, Cyp2a4, Cyp1a2, Cyp2b10, Ugt1a1, Mrp2, and Mrp3 mRNA levels in TRIF+/+ mice. This downregulation was not attenuated in TRIF-/- mice. Induction of cytokines by LPS was observed in both TRIF+/+ and TRIF-/- mice. Cytokine induction was delayed in polyI: C-treated TRIF-/- mice, indicating that multiple mechanisms mediating polyI: C signaling exist. To assess the role of MAPKs, primary hepatocytes were pretreated with specific inhibitors before treatment with LPS/polyI: C. We found that only the c-jun-N-terminal kinase (JNK) inhibitor attenuated the down-regulation of DMETs. These results show that TRIF-independent pathways can be involved in the downregulation of DMETs through TLR4 and 3. JNK-dependent mechanisms likely mediate this downregulation.

机译：肝药物代谢酶和转运蛋白（DMET）的表达和活性在感染和炎症过程中发生改变。肝脏中的炎症反应主要由Toll样受体（TLR）信号介导，这涉及募集含有Toll /白介素（IL）-1受体（TIR）的衔接子蛋白（TIRAP）和包含TIR的介导衔接子的干扰素（ IFN）-beta（TRIF）最终导致促炎性细胞因子和促分裂原活化蛋白激酶（MAPK）的诱导。脂多糖（LPS）激活革兰氏阴性细菌受体TLR4，而多肌苷酸：聚胞苷酸（polyI：C）激活病毒受体TLR3。 TLR4信号传导涉及TIRAP和TRIF，而TRIF是唯一参与TLR3途径的衔接子蛋白。先前我们已经表明，LPS介导的DMETs下调独立于TIRAP。为了确定TRIF的作用，我们用LPS或polyI：C处理了TRIF + / +和TRIF-/-小鼠。LPS下调（相似于40％-60％）Cyp3a11，Cyp2a4，Ugt1a1，Mrp2 mRNA水平，而polyI：C下调TRIF + / +小鼠的Cyp3a11，Cyp2a4，Cyp1a2，Cyp2b10，Ugt1a1，Mrp2和Mrp3 mRNA水平（类似于30％-60％）。在TRIF-/-小鼠中这种下调没有减弱。在TRIF + / +和TRIF-/-小鼠中均观察到LPS诱导的细胞因子。在polyI：C处理的TRIF-/-小鼠中，细胞因子的诱导被延迟，表明存在多种介导polyI：C信号传导的机制。为了评估MAPK的作用，在用LPS / polyI：C处理之前，先用特异性抑制剂预处理原代肝细胞。我们发现只有c-jun-N-末端激酶（JNK）抑制剂可减弱DMETs的下调。这些结果表明，不依赖TRIF的途径可通过TLR4和3参与DMET的下调。JNK依赖的机制可能介导此下调。

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《Drug Metabolism and Disposition: The Biological Fate of Chemicals》 |2016年第1期|共7页
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Shah Pranav; Omoluabi Ozozoma; Moorthy Bhagavatula; Ghose Romi;
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1. Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon beta in Toll-Like Receptor 3-and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes [J] . Shah Pranav, Omoluabi Ozozoma, Moorthy Bhagavatula, Drug Metabolism and Disposition: The Biological Fate of Chemicals . 2016,第1期

机译：衔接子蛋白类似收费的白介素域包含适配器诱导干扰素β在收费象受体3和4介导的肝药物代谢酶和转运蛋白调控中的作用
2. Regulation of hepatic drug-metabolizing enzyme genes by Toll-like receptor 4 signaling is independent of Toll-interleukin 1 receptor domain-containing adaptor protein. [J] . Ghose R, White D, Guo T, Drug Metabolism and Disposition: The Biological Fate of Chemicals . 2008,第1期

机译：Toll样受体4信号传导对肝药物代谢酶基因的调节独立于包含Toll-白介素1受体域的衔接蛋白。
3. Phosphatidylinositol 4-Phosphate 5-Kinase α Facilitates Toll-like Receptor 4-mediated Microglial Inflammation through Regulation of the Toll/Interleukin-1 Receptor Domain-containing Adaptor Protein (TIRAP) Location [J] . Tu Thi Ngoc Nguyen, Yong Min Kim, T. Doohun Kim, The Journal of biological chemistry . 2013,第8期

机译：磷脂酰肌醇4-磷酸5-激酶α通过调节含量/白细胞介素-1受体结构域（TIRAP）位置，促进损伤的受体4介导的微胶质炎症
4. Porphyromonas gingivalis major and minor fimbria-induced interleukin-8 production by human aortic endothelial cells: The role of Toll-like receptors (TLR)2 and TLR4. [D] . Davey, Michael Thomas. 2007

机译：人主动脉内皮细胞牙龈卟啉单胞菌主要和次要的菌毛诱导白细胞介素8的产生：Toll样受体（TLR）2和TLR4的作用。
5. Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon β in Toll-Like Receptor 3- and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes [O] . Pranav Shah, Ozozoma Omoluabi, Bhagavatula Moorthy, -1

机译：包含衔接子蛋白的类似介素介素结构域的区域在介导的类似Toll受体3和4介导的肝药物代谢酶和转运蛋白的调控中包含介导干扰素β的作用。
6. Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon in Toll-Like Receptor 3- and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes [O] . P. Shah, O. Omoluabi, B. Moorthy, 2015

机译：适配器蛋白收缩蛋白蛋白含有衔接子在肝脏药物代谢酶和转运蛋白基因的肝脏药物代谢酶的3-和4介导的调节中的作用

Role of Adaptor Protein Toll-Like Interleukin Domain Containing Adaptor Inducing Interferon beta in Toll-Like Receptor 3-and 4-Mediated Regulation of Hepatic Drug Metabolizing Enzyme and Transporter Genes

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