首页> 外文期刊>BMC Complementary and Alternative Medicine >Experimental validation and computational modeling of anti-influenza effects of quercetin-3-O-α-L-rhamnopyranoside from indigenous south African medicinal plant Rapanea melanophloeos
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Experimental validation and computational modeling of anti-influenza effects of quercetin-3-O-α-L-rhamnopyranoside from indigenous south African medicinal plant Rapanea melanophloeos

机译:土着南非药用植物Rapanea melanophloeos槲皮素-3-O-α-L-鼠霉酐抗流感作用的实验验证和计算模拟

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BACKGROUND:Influenza A virus (IAV) is still a major health threat. The clinical manifestations of this infection are related to immune dysregulation, which causes morbidity and mortality. The usage of traditional medication with immunomodulatory properties against influenza infection has been increased recently. Our previous study showed antiviral activity of quercetin-3-O-α-L-rhamnopyranoside (Q3R) isolated from Rapanea melanophloeos (RM) (L.) Mez (family Myrsinaceae) against H1N1 (A/PR/8/34) infection. This study aimed to confirm the wider range of immunomodulatory effect of Q3R on selective pro- and anti-inflammatory cytokines against IAV in vitro, to evaluate the effect of Q3R on apoptosis pathway in combination with H1N1, also to assess the physical interaction of Q3R with virus glycoproteins and RhoA protein using computational docking.METHODS:MDCK cells were exposed to Q3R and 100CCID50/100?μl of H1N1 in combined treatments (co-, pre- and post-penetration treatments). The treatments were tested for the cytokines evaluation at RNA and protein levels by qPCR and ELISA, respectively. In another set of treatment, apoptosis was examined by detecting RhoA GTPase protein and caspase-3 activity. Molecular docking was used as a tool for evaluation of the potential anti-influenza activity of Q3R.RESULTS:The expressions of cytokines in both genome and protein levels were significantly affected by Q3R treatment. It was shown that Q3R was much more effective against influenza when it was applied in co-penetration treatment. Q3R in combination with H1N1 increased caspase-3 activity while decreasing RhoA activation. The molecular docking results showed strong binding ability of Q3R with M2 transmembrane, Neuraminidase of 2009 pandemic H1N1, N1 and H1 of PR/8/1934 and Human RhoA proteins, with docking energy of -?10.81, -?10.47, -?9.52, -?9.24 and?-?8.78 Kcal/mol, respectively.CONCLUSIONS:Quercetin-3-O-α-L-rhamnopyranoside from RM was significantly effective against influenza infection by immunomodulatory properties, affecting the apoptosis pathway and binding ability to viral receptors M2 transmembrane and Neuraminidase of 2009 pandemic H1N1 and human RhoA cellular protein. Further research will focus on detecting the detailed specific mechanism of Q3R in virus-host interactions.
机译:背景:流感病毒(IAV)仍然是一个重大的健康威胁。这种感染的临床表现与免疫失调有关,导致发病率和死亡率。最近增加了对免疫调节性能免疫调节性能的传统药物的用法已增加。我们以前的研究表明,从Rapanea melanophloeos(RM)(L.)Mez(Family myrsinaceae)对H1N1(A / PR / 8/34)感染分离的槲皮素-3-O-α-L- rhamnyAlyside(Q3R)的抗病毒活性。本研究旨在确认Q3R的更广泛的免疫调节作用对Q3R对IAV的选择性促炎和抗炎细胞因子的免疫调节作用,评价Q3R与H1N1的凋亡途径的影响,也评估Q3R的物理相互作用病毒糖蛋白和rhoA蛋白使用计算码头。方法:将MDCK细胞暴露于组合处理中的Q3R和100ccid50 / 100?μlH1N1(共渗透和后渗透后处理)。通过QPCR和ELISA对RNA和蛋白水平进行细胞因子评估的治疗方法。在另一组治疗中,通过检测RhOA GTPAse蛋白和Caspase-3活性来检查细胞凋亡。将分子对接用作评估Q3R的潜在抗流感活性的工具。结果:基因组和蛋白质水平的细胞因子的表达受到Q3R处理的显着影响。结果表明,当其在共渗透处理时,Q3R对流感更有效。 Q3R与H1N1组合增加了Caspase-3活性,同时降低了RhoA激活。分子对接结果表明,Q3R的Q3R与M2跨膜,2009年大流行H1N1,N1和H1的QUR,N1和H1和人RhOO蛋白的Qu,N1和H1,具有对接能量的Q3R, - Δ10.81, - ?10.47, - ?9.52, - ?9.52, - ? - ? - ? - ? - ? - α-克隆/摩尔,分别:来自RM的槲皮素-3-O-α-L-鼠李酮苷对免疫调节性质的流感感染显着有效,影响凋亡途径和病毒受体的结合能力M2 2009年大流行H1N1和人rhOA细胞蛋白的跨膜和神经氨酸酶。进一步的研究将重点是检测病毒 - 宿主交互中Q3R的详细特定机制。

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