College of Chemistry and Pharmaceutical Engineering, Huanghuai University, Zhumadian 463000, China.
School of Life Sciences, Chinese University of Hong Kong, Shatin, N.T, Hong Kong SAR 999077, China.
Bioorg Chem. 2020 Sep;102:104106. doi: 10.1016/j.bioorg.2020.104106. Epub 2020 Jul 17.
Parasitic characteristics, mutations and resistance of influenza A virus make it difficult for current influenza antiviral drugs to maintain long-term effectiveness. Currently, to design non-adamantane compounds targeting the S31N mutant of M2 proton channel is a promising direction for the development of novel anti-influenza drugs. In our previous research, a pinanamine-based antiviral M090 was discovered to target hemagglutinin instead of M2, with its structure being highly similar to reported M2-S31N inhibitors. Herein, a series of pinane oxime derivatives were designed from scratch and evaluated for anti-influenza activity and their cytotoxicity in vitro. Utilizing a combination of structure-activity relationship analysis, electrophysiological assay and molecular docking, the most potent compound 11h, as a M2-S31N blocker, exhibited excellent activity with EC value at the low micromolar level against both H3N2 and H1N1. No significant toxicity of 11h was observed. In addition, compound 11h was located tightly in the pore of the drug-binding site with the thiophene moiety facing down toward the C-terminus, and did not adopt a similar position and orientation as the reference inhibitor.
流感病毒的寄生特性、突变和耐药性使得当前的流感抗病毒药物难以长期保持有效。目前,针对 M2 质子通道 S31N 突变设计非金刚烷类化合物是开发新型抗流感药物的有前途的方向。在我们之前的研究中,发现了一种基于金刚烷胺的抗病毒药物 M090,它的作用靶点是血凝素而不是 M2,其结构与报道的 M2-S31N 抑制剂高度相似。在此,我们从头开始设计了一系列金刚烷肟衍生物,并在体外评估了它们的抗流感活性和细胞毒性。通过结构-活性关系分析、电生理测定和分子对接的结合,最有效的化合物 11h 作为 M2-S31N 阻断剂,对 H3N2 和 H1N1 均表现出优异的活性,EC 值在低微摩尔水平。同时,化合物 11h 没有明显的毒性。此外,化合物 11h 紧密地位于药物结合位点的孔内,噻吩部分朝向 C 末端向下,并且没有采用与参考抑制剂相似的位置和取向。
