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微管抑制剂足叶草毒素可抑制人巨细胞病毒的早期进入步骤。

The Microtubule Inhibitor Podofilox Inhibits an Early Entry Step of Human Cytomegalovirus.

作者信息

Cohen Tobias, Schwarz Toni M, Vigant Frederic, Gardner Thomas J, Hernandez Rosmel E, Lee Benhur, Tortorella Domenico

机构信息

Department of Microbiology, Icahn School of Medicine at Mount Sinai, New York, NY 10029, USA.

出版信息

Viruses. 2016 Oct 24;8(10):295. doi: 10.3390/v8100295.

Abstract

Human cytomegalovirus is a ubiquitous β-herpesvirus that infects many different cell types through an initial binding to cell surface receptors followed by a fusion event at the cell membrane or endocytic vesicle. A recent high-throughput screen to identify compounds that block a step prior to viral gene expression identified podofilox as a potent and nontoxic inhibitor. Time-of-addition studies in combination with quantitative-PCR analysis demonstrated that podofilox limits an early step of virus entry at the cell surface. Podofilox was also able to drastically reduce infection by herpes simplex 1, an α-herpesvirus with a very similar entry process to CMV. Podofilox caused a reduced maximal plateau inhibition of infection by viruses with single step binding processes prior to fusion-like Newcastle disease virus, Sendai virus, and influenza A virus or viruses that enter via endocytosis like vesicular stomatitis virus and a clinical-like strain of CMV. These results indicate that microtubules appear to be participating in the post-binding step of virus entry including the pre- and post-penetration events. Modulation of the plasma membrane is required to promote virus entry for herpesviruses, and that podofilox, unlike colchicine or nocodazole, is able to preferentially target microtubule networks at the plasma membrane.

摘要

人巨细胞病毒是一种普遍存在的β疱疹病毒,它通过最初与细胞表面受体结合,随后在细胞膜或内吞小泡处发生融合事件,感染多种不同的细胞类型。最近一项旨在鉴定能阻断病毒基因表达之前步骤的化合物的高通量筛选,确定了足叶草毒素是一种有效且无毒的抑制剂。添加时间研究与定量PCR分析相结合表明,足叶草毒素在细胞表面限制了病毒进入的早期步骤。足叶草毒素还能够大幅降低单纯疱疹病毒1的感染,单纯疱疹病毒1是一种α疱疹病毒,其进入过程与巨细胞病毒非常相似。足叶草毒素对具有类似于新城疫病毒、仙台病毒和甲型流感病毒等融合前单步结合过程的病毒,或通过内吞作用进入的病毒(如水泡性口炎病毒和一种临床样巨细胞病毒株)的感染,引起的最大平台期抑制降低。这些结果表明,微管似乎参与了病毒进入的结合后步骤,包括穿透前和穿透后事件。对于疱疹病毒而言,质膜的调节是促进病毒进入所必需的,并且与秋水仙碱或诺考达唑不同,足叶草毒素能够优先靶向质膜处的微管网络。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae75/5086627/f43aec9316f9/viruses-08-00295-g001.jpg

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