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首页> 外文期刊>Colloids and Surfaces, B. Biointerfaces >Dual function of interleukin-23 Aptamer to suppress brain inflammation via attachment to macrophage stimulating 1 kinase and interleukin-23
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Dual function of interleukin-23 Aptamer to suppress brain inflammation via attachment to macrophage stimulating 1 kinase and interleukin-23

机译:白细胞介素-33适体的双重功能通过附着到巨噬细胞刺激1激酶和白细胞介素-23的巨噬细胞抑制脑炎症

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摘要

In the present study, the dual function of interleukin-23 (IL-23) Aptamer to suppress brain inflammation via attachment to macrophage stimulating 1 (MST1) kinase and IL-23, was introduced. Also, the anti-inflammatory property of IL-23 Aptamer has been investigated. This study showed that IL-23 Aptamer could reduce the clinical development of brain inflammation induced by Parathion, as an important organophosphate toxin. Both immunostaining and H&E staining indicated that the total inflammatory infiltration foci were remarkably decreased in IL-23 Aptamer-treated mice. Moreover, this study showed that IL-23 Aptamer reduced both absolute and relative numbers of MST1 + CD4 + Th1 cells and IL-23-producing cells. Analysis of the Hippo signaling genes showed a sharp decrease of MST1 kinase compared with other genes (P < 0.001). Moreover, computer-assisted molecular docking demonstrated that both MST1 kinase and IL-23 could tightly attach to IL-23 Aptamer, and maybe block it. Taken together, IL-23 Aptamer coud decrease brain inflammation via suppressing MST1 kinase and IL-23.
机译:在本研究中,引入了白细胞介素-33(IL-23)适体通过附着到巨噬细胞刺激1(MST1)激酶和IL-23的脑炎抑制脑炎的双重功能。此外,已经研究了IL-23适体的抗炎性能。本研究表明,IL-23适体可以降低通过解性诱导的脑炎症的临床发展,作为重要的有机磷酸毒素。免疫染色和H&E染色表明,IL-23适体处理的小鼠中总炎性渗透灶极性降低。此外,该研究表明,IL-23适体减少了MST1 + CD4 + TH1细胞和IL-23产生细胞的绝对和相对数。与其他基因相比,河马信号基因的分析显示MST1激酶的急剧下降(P <0.001)。此外,计算机辅助分子对接证明了MST1激酶和IL-23可以紧密地连接到IL-23适体,并且可以阻挡它。通过抑制MST1激酶和IL-23,将IL-23 Aptamer Coud降低脑炎症。

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