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Bafilomycin A1 and U18666A Efficiently Impair ZIKV Infection

机译:Bafilomycin A1和U18666A有效损害ZIKV感染

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摘要

Zika virus (ZIKV) is a highly transmissive virus that belongs to the Flaviviridae family, which comprises several other pathogens that threaten human health. This re-emerging virus gained attention during the outbreak in Brazil in 2016, where a considerable number of microcephaly cases in newborns was associated with ZIKV infection during pregnancy. Lacking a preventive vaccine or antiviral drugs, efforts have been made to better understand the viral life cycle. In light of this, the relevance of the endosomal–lysosomal compartment for the ZIKV life cycle was investigated. A549 and SH-SY5Y cells were infected with either the African strain (associated with mild symptoms) or the French Polynesia strain (associated with neurological complications). For both strains, the V-ATPase inhibitor, bafilomycin A1, efficiently inhibited ZIKV entry and prevented the spread of the infection by interfering with viral maturation. Additionally, affecting cholesterol metabolism and transport with the drug U18666A, which inactivates late endosomes and lysosomes, impairs the viral life cycle. The data presented show a clear antiviral effect of two compounds that target the same compartments in different ways. This highlights the relevance of the endosomal–lysosomal compartment for the viral life cycle that should be considered as a target for antivirals.
机译:寨卡病毒(ZIKV)是高传播病毒,属于黄病毒科,其中包括威胁人类健康的其他几种病原体。这种重新出现的病毒在2016年的巴西爆发中引起了人们的关注,在新生儿中,相当数量的新生儿小头畸形病例与孕期ZIKV感染有关。由于缺乏预防性疫苗或抗病毒药物,人们已做出努力,以更好地了解病毒的生命周期。有鉴于此,研究了内体-溶酶体区室与ZIKV生命周期的相关性。 A549和SH-SY5Y细胞感染了非洲毒株(伴有轻度症状)或法属波利尼西亚毒株(伴有神经系统并发症)。对于这两种菌株,V-ATPase抑制剂bafilomycin A1有效地抑制ZIKV进入并通过干扰病毒成熟来防止感染的传播。此外,使用药物U18666A影响胆固醇的代谢和运输,该药物可使晚期的内体和溶酶体失活,从而损害病毒的生命周期。所提供的数据表明,两种以不同方式靶向同一区室的化合物具有明显的抗病毒作用。这突出了内体-溶酶体区室与病毒生命周期的相关性,应将其视为抗病毒药物的靶标。

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