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Statins Suppress Ebola Virus Infectivity by Interfering with Glycoprotein Processing

机译:他汀类药物通过干扰糖蛋白加工抑制埃博拉病毒的感染性。

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ABSTRACT Ebola virus (EBOV) infection is a major public health concern due to high fatality rates and limited effective treatments. Statins, widely used cholesterol-lowering drugs, have pleiotropic mechanisms of action and were suggested as potential adjunct therapy for Ebola virus disease (EVD) during the 2013–2016 outbreak in West Africa. Here, we evaluated the antiviral effects of statin (lovastatin) on EBOV infection in vitro . Statin treatment decreased infectious EBOV production in primary human monocyte-derived macrophages and in the hepatic cell line Huh7. Statin treatment did not interfere with viral entry, but the viral particles released from treated cells showed reduced infectivity due to inhibition of viral glycoprotein processing, as evidenced by decreased ratios of the mature glycoprotein form to precursor form. Statin-induced inhibition of infectious virus production and glycoprotein processing was reversed by exogenous mevalonate, the rate-limiting product of the cholesterol biosynthesis pathway, but not by low-density lipoprotein. Finally, statin-treated cells produced EBOV particles devoid of the surface glycoproteins required for virus infectivity. Our findings demonstrate that statin treatment inhibits EBOV infection and suggest that the efficacy of statin treatment should be evaluated in appropriate animal models of EVD. IMPORTANCE Treatments targeting Ebola virus disease (EVD) are experimental, expensive, and scarce. Statins are inexpensive generic drugs that have been used for many years for the treatment of hypercholesterolemia and have a favorable safety profile. Here, we show the antiviral effects of statins on infectious Ebola virus (EBOV) production. Our study reveals a novel molecular mechanism in which statin regulates EBOV particle infectivity by preventing glycoprotein processing and incorporation into virus particles. Additionally, statins have anti-inflammatory and immunomodulatory effects. Since inflammation and dysregulation of the immune system are characteristic features of EVD, statins could be explored as part of EVD therapeutics.
机译:摘要由于高死亡率和有限的有效治疗方法,埃博拉病毒(EBOV)感染是主要的公共卫生问题。他汀类药物是广泛使用的降低胆固醇的药物,具有多效性作用机制,被认为是2013-2016年西非爆发埃博拉病毒病(EVD)的潜在辅助疗法。在这里,我们评估了他汀类药物(洛伐他汀)在体外对EBOV感染的抗病毒作用。他汀类药物治疗减少了人类原代单核细胞衍生的巨噬细胞和肝细胞系Huh7的传染性EBOV产生。抑制素处理不干扰病毒进入,但是从处理细胞释放的病毒颗粒由于抑制了病毒糖蛋白加工而显示出降低的感染力,这由成熟糖蛋白形式与前体形式的比率降低所证明。他汀类药物对感染性病毒产生和糖蛋白加工的抑制作用被胆固醇生物合成途径的限速产物外源性甲羟戊酸逆转,但低密度脂蛋白却不能逆转。最后,用他汀类药物处理的细胞产生的EBOV颗粒缺少病毒感染所需的表面糖蛋白。我们的发现表明,他汀类药物治疗可抑制EBOV感染,并建议应在适当的EVD动物模型中评估他汀类药物的治疗效果。重要针对埃博拉病毒病(EVD)的治疗是实验性,昂贵且稀缺的。他汀类药物是廉价的非专利药物,已用于治疗高胆固醇血症多年,并具有良好的安全性。在这里,我们显示了他汀类药物对传染性埃博拉病毒(EBOV)生产的抗病毒作用。我们的研究揭示了一种新的分子机制,其中他汀类药物通过阻止糖蛋白加工和掺入病毒颗粒来调节EBOV颗粒的感染性。另外,他汀类药物具有抗炎和免疫调节作用。由于免疫系统的炎症和调节异常是EVD的特征,因此他汀类药物可作为EVD治疗药物的一部分进行探索。

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