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首页> 外文期刊>Drug Metabolism and Disposition: The Biological Fate of Chemicals >Differential role of Toll-interleukin 1 receptor domain-containing adaptor protein in Toll-like receptor 2-mediated regulation of gene expression of hepatic cytokines and drug-metabolizing enzymes.
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Differential role of Toll-interleukin 1 receptor domain-containing adaptor protein in Toll-like receptor 2-mediated regulation of gene expression of hepatic cytokines and drug-metabolizing enzymes.

机译:Toll-白介素1受体域的适配器蛋白在Toll样受体2介导的肝细胞因子和药物代谢酶基因表达的调节中的差异作用。

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Pharmacological activities of drugs are impaired during inflammation because of reduced expression of hepatic drug-metabolizing enzyme genes (DMEs) and their regulatory nuclear receptors (NRs): pregnane X receptor (PXR), constitutive androstane receptor (CAR), and retinoid X receptor (RXRalpha). We have shown that a component of Gram-positive bacteria, lipoteichoic acid (LTA) induces proinflammatory cytokines and reduces gene expression of hepatic DMEs and NRs. LTA is a Toll-like receptor 2 (TLR2) ligand, which initiates signaling by recruitment of Toll-interleukin 1 receptor domain-containing adaptor protein (TIRAP) to the cytoplasmic TIR domain of TLR2. To determine the role of TIRAP in TLR2-mediated regulation of DME genes, TLR2(+/+), TLR2(-/-), TIRAP(+/+), and TIRAP(-/-) mice were given LTA injections. RNA levels of the DMEs (Cyp3a11, Cyp2b10, and sulfoaminotransferase), xenobiotic NRs (PXR and CAR), and nuclear protein levels of the central NR RXRalpha were reduced approximately 50 to 60% in LTA-treated TLR2(+/+) but not in TLR2(-/-) mice. Induction of hepatic cytokines (interleukin-1beta, tumor necrosis factor-alpha, and interleukin-6), c-Jun NH(2)-terminal kinase, and nuclear factor-kappaBeta was blocked in TLR2(-/-) mice. As expected, expression of hepatic DMEs and NRs was reduced by LTA in TIRAP(+/+) but not in TIRAP(-/-) mice. Of interest, cytokine RNA levels were induced in the livers of both the TIRAP(+/+) and TIRAP(-/-) mice, whereas LTA-mediated induction of serum cytokines was attenuated in TIRAP(-/-) mice. LTA-mediated down-regulation of DME genes was attenuated in hepatocytes from TLR2(-/-) or TIRAP(-/-) mice and in small interfering RNA-treated hepatocytes. Thus, the effect of TLR2 on DME genes in hepatocytes was mediated by TIRAP, whereas TIRAP was not involved in mediating the effects of TLR2 on cytokine expression in the liver.
机译:在炎症过程中,由于肝药物代谢酶基因(DME)及其调节性核受体(NRs)的表达降低,导致药物的药理活性受到损害:孕烷X受体(PXR),组成型雄烷烃受体(CAR)和类维生素A X受体( RXRalpha)。我们已经表明,革兰氏阳性细菌的一部分,脂磷壁酸(LTA)会诱导促炎细胞因子并减少肝DME和NRs的基因表达。 LTA是Toll样受体2(TLR2)配体,它通过将包含Toll-白介素1受体域的衔接蛋白(TIRAP)募集到TLR2的细胞质TIR域来启动信号传导。为了确定TIRAP在TLR2介导的DME基因调控中的作用,给LTA注射了TLR2(+ / +),TLR2(-/-),TIRAP(+ / +)和TIRAP(-/-)小鼠。在经LTA处理的TLR2(+ / +)中,DME的RNA水平(Cyp3a11,Cyp2b10和磺胺基转移酶),异种生物NRs(PXR和CAR)和中央NR RXRalpha的核蛋白水平降低了约50%至60%,但没有降低在TLR2(-/-)小鼠中。在TLR2(-/-)小鼠中,肝细胞因子(白介素-1β,肿瘤坏死因子-α和白介素-6),c-Jun NH(2)-末端激酶和核因子-kappaBeta的诱导被阻断。如预期的那样,在TIRAP(+ / +)小鼠中LTA降低了肝DME和NRs的表达,但在TIRAP(-/-)小鼠中却没有。有趣的是,在TIRAP(+ / +)和TIRAP(-/-)小鼠的肝脏中均诱导了细胞因子RNA水平,而在TIRAP(-/-)小鼠中LTA介导的血清细胞因子诱导被减弱。 LTA介导的DME基因下调在来自TLR2(-/-)或TIRAP(-/-)小鼠的肝细胞中以及在小干扰RNA处理的肝细胞中得以减弱。因此,TLR2对肝细胞中DME基因的影响是由TIRAP介导的,而TIRAP不参与介导TLR2对肝脏中细胞因子表达的影响。

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