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新型三唑衍生物的不对称合成及其体外抗病毒活性与作用机制

Asymmetric synthesis of novel triazole derivatives and their in vitro antiviral activity and mechanism of action.

作者信息

Cao Xiufang, Wang Wenda, Wang Shuangshuang, Bao Longzhu

机构信息

College of Science, Huazhong Agricultural University, Wuhan 430070, People's Republic of China.

College of Science, Huazhong Agricultural University, Wuhan 430070, People's Republic of China.

出版信息

Eur J Med Chem. 2017 Oct 20;139:718-725. doi: 10.1016/j.ejmech.2017.08.057. Epub 2017 Aug 26.

Abstract

In this study, forty-four chiral triazole derivatives have been prepared via asymmetric synthesis, and which has been successfully characterized by typical spectroscopic techniques including H NMR, C NMR, EI-MS, elemental analysis and optical rotations. Their in vitro antiviral activities against EV71 and CVB3 were fully investigated in cell-based assays. It was observed that 13 synthetic triazole derivatives inhibited the CPE of EV71 on RD cells, with EC in the 5.3-15.9 μg/ml range and corresponding SIs of 4.0-27.6, while 17 triazole derivatives showed antiviral activities against CVB3, with EC in the 4.7-15.1 μg/ml range and the corresponding SIs of 3.7-14.5. In addition, in some cases, the respective enantiomers showed significantly selective inhibitory effect against EV71, most notably for the enantiomers 9(R) and 10(S), 42(R) and 43(S), which presented an obvious activity difference. The most potential molecules are the compounds 10 and 43 with S-configuration, and which exhibit good SI values compared with the control Ribavirin.

摘要

在本研究中,通过不对称合成制备了44种手性三唑衍生物,并通过包括¹H NMR、¹³C NMR、EI-MS、元素分析和旋光在内的典型光谱技术成功对其进行了表征。在基于细胞的试验中全面研究了它们对EV71和CVB3的体外抗病毒活性。观察到13种合成三唑衍生物抑制了RD细胞上EV71的细胞病变效应,EC在5.3 - 15.9μg/ml范围内,相应的SI为4.0 - 27.6,而17种三唑衍生物对CVB3显示出抗病毒活性,EC在4.7 - 15.1μg/ml范围内,相应的SI为3.7 - 14.5。此外,在某些情况下,各自的对映体对EV71表现出显著的选择性抑制作用,最明显的是对映体9(R)和10(S)、42(R)和43(S),它们表现出明显的活性差异。最具潜力的分子是具有S构型的化合物10和43,与对照利巴韦林相比,它们表现出良好的SI值。

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