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Antiviral therapies against Ebola and other emerging viral diseases using existing medicines that block virus entry

机译:使用阻止病毒进入的现有药物抗埃博拉病毒和其他新兴病毒性疾病的抗病毒疗法

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摘要

Emerging viral diseases pose a threat to the global population as intervention strategies are mainly limited to basic containment due to the lack of efficacious and approved vaccines and antiviral drugs. The former was the only available intervention when the current unprecedented Ebolavirus (EBOV) outbreak in West Africa began. Prior to this, the development of EBOV vaccines and anti-viral therapies required time and resources that were not available. Therefore, focus has turned to re-purposing of existing, licenced medicines that may limit the morbidity and mortality rates of EBOV and could be used immediately. Here we test three such medicines and measure their ability to inhibit pseudotype viruses (PVs) of two EBOV species, Marburg virus (MARV) and avian influenza H5 (FLU-H5). We confirm the ability of chloroquine (CQ) to inhibit viral entry in a pH specific manner. The commonly used proton pump inhibitors, Omeprazole and Esomeprazole were also able to inhibit entry of all PVs tested but at higher drug concentrations than may be achieved in vivo. We propose CQ as a priority candidate to consider for treatment of EBOV.
机译:新兴的病毒性疾病对全球人口构成威胁,因为由于缺乏有效的,经过批准的疫苗和抗病毒药物,干预策略主要限于基本控制。前者是当前西非史无前例的埃博拉病毒(EBOV)爆发时唯一可用的干预措施。在此之前,EBOV疫苗和抗病毒疗法的开发需要时间和资源。因此,焦点已转向重新使用现有的许可药物,这些药物可能会限制EBOV的发病率和死亡率,并可以立即使用。在这里,我们测试了这三种药物,并测量了它们抑制两种EBOV物种的伪型病毒(PVs)的能力,即马尔堡病毒(MARV)和禽流感H5(FLU-H5)。我们证实了氯喹(CQ)以特定于pH的方式抑制病毒进入的能力。常用的质子泵抑制剂奥美拉唑和埃索美拉唑也能够抑制所有受测PV的进入,但药物浓度高于体内可能达到的浓度。我们建议将CQ作为考虑治疗EBOV的优先考虑对象。

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