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Prophylactic, therapeutic and neutralizing effects of zinc oxide tetrapod structures against herpes simplex virus type-2 infection

机译:氧化锌四足体结构对单纯疱疹病毒2型感染的预防,治疗和中和作用

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The attachment of Herpes simplex virus type-2 (HSV-2) to a target cell requires ionic interactions between negatively charged cell surface co-receptor heparan sulfate (HS) and positively charged residues on viral envelop glycoproteins, gB and gC. Effective blocking of this first step of HSV-2 pathogenesis demonstrates significant prophylactic effects against the viral disease; any in vitro therapeutic effects of blocking this interaction, however, are not clear. Here, we provide new evidence that zinc oxide tetrapod micro-nanostructures synthesized by flame transport approach significantly block HSV-2 entry into target cells and, in addition, demonstrate the potential to stop the spread of the virus among already infected cells. The zinc oxide tetrapods (ZnOTs) also exhibit the ability to neutralize HSV-2 virions. Natural target cells such as human vaginal epithelial and HeLa cells showed highly reduced infectivity when infected with HSV-2 virions that were pre-incubated with the ZnOTs. The mechanism behind the ability of ZnOTs to prevent, neutralize or reduce HSV-2 infection relies on their ability to bind the HSV-2 virions. We used fluorescently labeled ZnOTs and GFP-expressing HSV-2 virions to demonstrate the binding of the ZnOTs with HSV-2. We also show that the binding and hence, the antiviral effects of ZnOTs can be enhanced by illuminating the ZnOTs with UV light. Our results provide new insights into the anti-HSV-2 effects of ZnOT and rationalize their development as a HSV-2 trapping agent for the prevention and/or treatment of infection. The observed results also demonstrate that blocking HSV-2 attachment can have prophylactic as well as therapeutic applications.
机译:2型单纯疱疹病毒(HSV-2)与靶细胞的附着需要带负电荷的细胞表面共受体硫酸乙酰肝素(HS)与病毒包膜糖蛋白,gB和gC上带正电荷的残基之间的离子相互作用。有效阻断HSV-2发病机理的这一第一步表明,它对病毒性疾病具有明显的预防作用。但是,尚不清楚阻断这种相互作用的任何体外治疗作用。在这里,我们提供了新的证据,表明通过火焰传输方法合成的氧化锌四足体微纳米结构显着阻止了HSV-2进入靶细胞,此外,还证明了阻止病毒在已经感染的细胞中传播的潜力。氧化锌四足动物(ZnOTs)还具有中和HSV-2病毒体的能力。当用预先与ZnOTs孵育的HSV-2病毒体感染时,诸如人类阴道上皮和HeLa细胞之类的天然靶细胞显示出极低的感染力。 ZnOTs预防,中和或减少HSV-2感染的能力背后的机制取决于它们结合HSV-2病毒粒子的能力。我们使用荧光标记的ZnOTs和表达GFP的HSV-2病毒粒子来证明ZnOTs与HSV-2的结合。我们还表明,可以通过用紫外线照射ZnOTs来增强ZnOTs的结合以及因此的抗病毒作用。我们的结果为ZnOT的抗HSV-2效应提供了新的见解,并使它们合理发展为HSV-2捕获剂以预防和/或治疗感染。观察到的结果还表明,阻断HSV-2的附着可具有预防和治疗应用。

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