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Inhibition of poxvirus growth by Terameprocol, a methylated derivative of nordihydroguaiaretic acid.

机译:Terameprocol,一种去甲氢愈创木酸的甲基化衍生物,可抑制痘病毒的生长。

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Terameprocol (TMP) is a methylated derivative of nordihydroguaiaretic acid, a phenolic antioxidant originally derived from creosote bush extracts. TMP has previously been shown to have antiviral and anti-inflammatory activities, and has been proven safe in phase I clinical trials conducted to evaluate TMP as both a topical and parenteral therapeutic. In the current study, we examined the ability of TMP to inhibit poxvirus growth in vitro, and found that TMP potently inhibited the growth of both cowpox virus and vaccinia virus in a variety of cell lines. TMP treatment was highly effective at reducing infectious virus yield in multi-step virus growth assays, but it did not substantially inhibit the synthesis of infectious progeny viruses in individual infected cells. These contrasting results showed that TMP inhibits poxvirus growth in vitro by preventing the efficient spread of virus particles from cell to cell. The canonical mechanism of poxvirus cell-to-cell spread requires morphogenesis of cell-associated, enveloped virions. The virions then trigger the formation of actin tails to project them from the cell surface. The number of actin tails present at the surface of poxvirus-infected cells was reduced dramatically by treatment with TMP. Whether TMP inhibits poxvirus morphogenesis, or subsequent events required for actin tail formation, remains to be determined. The results of this study, together with the clinical safety record of TMP, support further evaluation of TMP as a poxvirus therapeutic.
机译:Terameprocol(TMP)是去甲二氢愈创木酸的甲基化衍生物,去甲二氢愈创木酸是一种酚抗氧化剂,最初是从杂酚丛灌木提取物中提取的。 TMP先前已被证明具有抗病毒和抗炎活性,并已在进行TMP作为局部和肠胃外治疗药物评估的I期临床试验中被证明是安全的。在当前的研究中,我们检查了TMP在体外抑制痘病毒生长的能力,发现TMP在多种细胞系中均能有效抑制牛痘病毒和牛痘病毒的生长。在多步病毒生长测定中,TMP处理在降低传染性病毒产量方面非常有效,但是它并没有实质性地抑制单个感染细胞中传染性子代病毒的合成。这些相反的结果表明,TMP通过阻止病毒颗粒从细胞到细胞的有效传播而在体外抑制痘病毒的生长。痘病毒细胞间传播的典型机制需要细胞相关的包膜病毒粒子的形态发生。病毒体然后触发肌动蛋白尾巴的形成,将它们从细胞表面投射出来。通过TMP处理,痘病毒感染细胞表面存在的肌动蛋白尾巴数量大大减少。 TMP是否抑制痘病毒形态发生或肌动蛋白尾巴形成所需的后续事件仍有待确定。这项研究的结果以及TMP的临床安全性记录,支持进一步评估TMP作为痘病毒治疗剂。

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