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Pentagalloylglucose downregulates cofilin1 and inhibits HSV-1 infection.

机译:戊铝酰葡萄糖可下调cofilin1并抑制HSV-1感染。

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To investigate the anti-herpesvirus mechanism of pentagalloylglucose (PGG), we compared the proteomic changes between herpes simplex virus type 1 (HSV-1) infected MRC-5 cells with or without PGG-treatment, and between non-infected MRC-5 cells with or without PGG-treatment by 2-DE and MS-based analysis. Differentially expressed cellular proteins were mainly involved with actin cytoskeleton regulation. Significantly, PGG can down-regulate cofilin1, a key regulator of actin cytoskeleton dynamics. PGG can inhibit HSV-1-induced rearrangements of actin cytoskeleton which is important for infectivity. Furthermore, cofilin1 knockdown by siRNA also inhibited the HSV-1-induced actin-skeleton rearrangements. Both PGG-treatment and cofilin1 knockdown can reduce HSV-1 DNA, mRNA, protein synthesis and virus yields. Altogether, the results suggested that down-regulating cofilin1 plays a role in PGG inhibiting HSV-1 infection. PGG may be a promising anti-herpesvirus agent for drug development.
机译:为了研究五甲基戊二糖(PGG)的抗疱疹病毒机制,我们比较了使用或不使用PGG治疗的单纯疱疹病毒1型(HSV-1)感染的MRC-5细胞和未感染的MRC-5细胞之间的蛋白质组学变化通过2-DE和基于MS的分析可对PGG进行处理或不进行PGG处理。差异表达的细胞蛋白主要参与肌动蛋白的细胞骨架调控。重要的是,PGG可以下调cofilin1,cofilin1是肌动蛋白细胞骨架动力学的关键调节剂。 PGG可以抑制HSV-1诱导的肌动蛋白细胞骨架重排,这对感染性很重要。此外,siRNA对cofilin1的抑制还抑制了HSV-1诱导的肌动蛋白骨架重排。 PGG处理和cofilin1组合均可降低HSV-1 DNA,mRNA,蛋白质合成和病毒产量。总之,结果表明下调cofilin1在PGG抑制HSV-1感染中起作用。 PGG可能是用于药物开发的有希望的抗疱疹病毒药物。

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