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首页> 外文期刊>Drug Design, Development and Therapy >Paclitaxel alleviated sepsis-induced acute lung injury by activating MUC1 and suppressing TLR-4/NF-κB pathway
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Paclitaxel alleviated sepsis-induced acute lung injury by activating MUC1 and suppressing TLR-4/NF-κB pathway

机译:紫杉醇通过激活MUC1和抑制TLR-4 /NF-κB途径减轻败血症引起的急性肺损伤

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Purpose: It has been reported that approximately 40% of ALI (acute lung injury) incidence resulted from sepsis. Paclitaxel, as a classic anti-cancer drug, plays an important role in the regulation of inflammation. However, we do not know whether it has a protective effect against CLP (cecal ligation and puncture)-induced septic ALI. Our study aims to illuminate the mitigative effects of paclitaxel on sepsis-induced ALI and its relevant mechanisms. Materials and methods: The survival rates and organ injuries were used to evaluate the effects of paclitaxel on CLP mice. The levels of inflammatory cytokines were tested by ELISA. MUC1 siRNA pre-treatment was used to knockdown MUC1 expression in vitro. GO203 was used to inhibit the homodimerization of MUC1-C in vivo. The expression levels of MUC1, TLR 4 and p-NF-κB/p65 were detected by Western blot. Results: Our results showed that paclitaxel improved the survival rates and ameliorated organ injuries especially lung injury in CLP-induced septic mice. These were accompanied by reduced inflammatory cytokines in sera and BALF (bronchoalveolar lavage fluid). We also found paclitaxel could attenuate TLR 4-NF-κB/p65 activation both in lung tissues of septic mice and LPS-stimulated lung type II epithelial cell line A549. At the upstream level, paclitaxel-upregulated expression levels of MUC1 in both in vivo and in vitro experiments. The inhibitory effects of paclitaxel on TLR 4-NF-κB/p65 activation were reversed in lung tissues of septic mice pre-treated with MUC1 inhibitor and in MUC1-knockdown A549 cells. Protection of paclitaxel on sepsis-induced ALI and decrease of inflammatory cytokines were also abolished by inhibition of MUC1. Conclusion: Collectively, these results indicated paclitaxel could significantly alleviate acute lung injury in CLP-induced septic mice and LPS-stimulated lung type II epithelial cell line A549 by activating MUC1 and suppressing TLR-4/NF-κB pathway.
机译:目的:据报道,约40%的ALI(急性肺损伤)发生率是由败血症引起的。紫杉醇作为一种经典的抗癌药,在炎症调节中起着重要作用。但是,我们不知道它是否对CLP(盲肠结扎和穿刺)诱导的败血症ALI具有保护作用。我们的研究旨在阐明紫杉醇对败血症诱导的ALI的缓解作用及其相关机制。材料和方法:使用存活率和器官损伤评估紫杉醇对CLP小鼠的影响。通过ELISA测试炎性细胞因子的水平。使用MUC1 siRNA预处理在体外敲低MUC1的表达。 GO203用于体内抑制MUC1-C的同型二聚化。 Western blot检测MUC1,TLR 4和p-NF-κB/ p65的表达水平。结果:我们的结果表明,紫杉醇可改善CLP诱导的败血症小鼠的存活率并改善器官损伤,尤其是肺损伤。这些伴有血清和BALF(支气管肺泡灌洗液)中炎性细胞因子的减少。我们还发现紫杉醇可以减弱脓毒症小鼠肺组织和LPS刺激的II型肺上皮细胞系A549中TLR4-NF-κB/ p65的活化。在上游水平,紫杉醇在体内和体外实验中均上调了MUC1的表达水平。紫杉醇对经MUC1抑制剂预处理的脓毒症小鼠的肺组织和MUC1抑制型A549细胞的TLR4-NF-κB/ p65激活的抑制作用被逆转。紫杉醇对败血症诱导的ALI的保护作用和炎症细胞因子的减少也被MUC1抑制所取消。结论:总体而言,这些结果表明紫杉醇可以通过激活MUC1并抑制TLR-4 /NF-κB途径,显着减轻CLP诱导的败血症小鼠和LPS刺激的II型肺上皮细胞系A549的急性肺损伤。

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