首页> 美国卫生研究院文献>Evidence-based Complementary and Alternative Medicine : eCAM >Gene Expression Profiles Underlying Selective T-Cell-Mediated Immunity Activity of a Chinese Medicine Granule on Mice Infected with Influenza Virus H1N1
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Gene Expression Profiles Underlying Selective T-Cell-Mediated Immunity Activity of a Chinese Medicine Granule on Mice Infected with Influenza Virus H1N1

机译:选择性T细胞介导的中药颗粒对H1N1流感病毒感染小鼠的免疫活性的基因表达谱

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摘要

A Chinese medicine granule, Shu-Feng-Xuan-Fei (SFXF), is critical for viral clearance in early phase of influenza virus infection. In this study, 72 ICR mice were randomly divided into six groups: normal control group, virus control group, Oseltamivir group, low-dose SFXF, medium-dose SFXF, and high-dose SFXF. Mice were anesthetized and inoculated with 4LD50 of influenza virus A (H1N1) except normal control group. Oseltamivir group received 11.375 mg·kg−1 ·d−1 Oseltamivir Phosphate. SFXF 3.76, 1.88 and 0.94 g·kg−1 ·d−1 were administrated to mice in all SFXF groups. Each group was in equal dose of 0.2ml daily for 4 consecutive days. Mice were sacrificed and then total RNA was extracted in lung tissue. Some genes involved in T-cell-mediated immunity were selected by DNA microarray. These candidate genes were verified by Real-Time PCR and western immunoblotting. Compared with virus control group, in Toll-like receptor signaling pathway, 12 virus-altered genes were significantly reduced following medium-dose SFXF treatment. Eighteen antigen processing presentation-associated genes were upregulated by medium-dose SFXF. In the process of T cell receptor signaling pathway, 19 genes were downregulated by medium-dose SFXF treatment. On exploration into effector T cells activation and cytokines, all of altered genes in virus control group were reversed by medium-dose SFXF. Real-time PCR and western immunoblotting showed that the regulation of medium-dose SFXF in IL-4, IFN-γ, TNF-α, IL-1β, TLR7, MyD88, p38, and JNK was superior to Oseltamivir and high-dose SFXF group. Therefore, SFXF granules could reduce influenza infected cells and activation of T cells.
机译:中药颗粒舒风玄飞(SFXF)对于流感病毒感染早期的病毒清除至关重要。在这项研究中,将72只ICR小鼠随机分为六组:正常对照组,病毒对照组,奥瑟他韦组,低剂量SFXF,中剂量SFXF和高剂量SFXF。除正常对照组外,将小鼠麻醉并接种4LD50的甲型流感病毒(H1N1)。 Oseltamivir组接受11.375 mg·kg -1 ·d -1 磷酸Oseltamivir。将SFXF 3.76、1.88和0.94 g·kg -1 ·d -1 施用于所有SFXF组的小鼠。每组连续4天每天服用等量0.2ml。处死小鼠,然后在肺组织中提取总RNA。通过DNA微阵列选择一些参与T细胞介导的免疫的基因。这些候选基因通过实时PCR和Western免疫印迹验证。与病毒对照组相比,在中剂量SFXF处理后,Toll样受体信号通路中12个病毒改变的基因明显减少。中等剂量的SFXF上调了18个与抗原加工呈递相关的基因。在T细胞受体信号通路中,中剂量SFXF处理下调了19个基因。在探索效应T细胞的活化和细胞因子时,用中剂量的SFXF逆转了病毒对照组中所有改变的基因。实时荧光定量PCR和Western免疫印迹结果表明,中等剂量SFXF对IL-4,IFN-γ,TNF-α,IL-1β,TLR7,MyD88,p38和JNK的调节优于Oseltamivir和大剂量SFXF组。因此,SFXF颗粒可以减少流感病毒感染的细胞和T细胞的活化。

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