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首页> 外文期刊>ACS medicinal chemistry letters >Toward the Target: Tilorone, Quinacrine, and Pyronaridine Bind to Ebola Virus Glycoprotein
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Toward the Target: Tilorone, Quinacrine, and Pyronaridine Bind to Ebola Virus Glycoprotein

机译:朝向目标:椴树,喹吖啶和Pyronaridine与埃博拉病毒糖蛋白结合

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摘要

Pyronaridine, tilorone, and quinacrine were recently identified by a machine learning model and demonstrated in vitro and in vivo activity against Ebola virus (EBOV) and represent viable candidates for drug repurposing. The target for these molecules was previously unknown. These drugs have now been docked into the crystal structure of the ebola glycoprotein and then experimentally validated in vitro using microscale thermophoresis to generate K-d values for tilorone (0.73 mu M), pyronaridine (7.34 mu M), and quinacrine (7.55 mu M). These molecules were shown to bind with a higher affinity than the previously reported toremifene (16 mu M). These three structures provide more insight into the structural diversity of ebola glycoprotein inhibitors which can be utilized in the discovery and design of additional inhibitors.
机译:最近通过机器学习模型识别吡喃胆碱,潮罗酮和喹吖啶,并对埃博拉病毒(EBOV)的体外和体内活动进行了证明,代表了用于药物重估的可行候选者。 这些分子的靶标先前未知。 这些药物现在已经停靠在埃博拉糖蛋白的晶体结构中,然后使用微尺寸热孔进行实验验证,以产生潮罗酮(0.73μm),吡喃啶(7.34μm)和喹吖啶(7.55μm)的K-D值。 显示这些分子与先前报道的Toremifene(16μm)含有更高的亲和力。 这三种结构提供了更有洞察力的埃博拉糖蛋白抑制剂结构多样性,其可用于发现和设计附加抑制剂。

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