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芜菁花叶病毒基因组连接蛋白(VPg)对 pokeweed 抗病毒蛋白(PAP)的抑制作用。

Inhibition of pokeweed antiviral protein (PAP) by turnip mosaic virus genome-linked protein (VPg).

机构信息

Department of Chemistry, Hunter College and the Graduate Center of the City University of New York, New York, NY 10065, USA.

出版信息

J Biol Chem. 2012 Aug 24;287(35):29729-38. doi: 10.1074/jbc.M112.367581. Epub 2012 Jul 6.

Abstract

Pokeweed antiviral protein (PAP) from Phytolacca americana is a ribosome-inactivating protein (RIP) and an RNA N-glycosidase that removes specific purine residues from the sarcin/ricin loop of large rRNA, arresting protein synthesis at the translocation step. PAP is also a cap-binding protein and is a potent antiviral agent against many plant, animal, and human viruses. To elucidate the mechanism of RNA depurination, and to understand how PAP recognizes and targets various RNAs, the interactions between PAP and turnip mosaic virus genome-linked protein (VPg) were investigated. VPg can function as a cap analog in cap-independent translation and potentially target PAP to uncapped IRES-containing RNA. In this work, fluorescence spectroscopy and HPLC techniques were used to quantitatively describe PAP depurination activity and PAP-VPg interactions. PAP binds to VPg with high affinity (29.5 nm); the reaction is enthalpically driven and entropically favored. Further, VPg is a potent inhibitor of PAP depurination of RNA in wheat germ lysate and competes with structured RNA derived from tobacco etch virus for PAP binding. VPg may confer an evolutionary advantage by suppressing one of the plant defense mechanisms and also suggests the possible use of this protein against the cytotoxic activity of ribosome-inactivating proteins.

摘要

美洲商陆抗病毒蛋白(PAP)是一种核糖体失活蛋白(RIP)和 RNA N-糖苷酶,它从大 rRNA 的 Sarcin/ricin 环中去除特定的嘌呤残基,在易位步骤中止蛋白质合成。PAP 也是一种帽结合蛋白,是一种针对许多植物、动物和人类病毒的有效抗病毒剂。为了阐明 RNA 脱嘌呤的机制,并了解 PAP 如何识别和靶向各种 RNA,研究了 PAP 与芜菁花叶病毒基因组连接蛋白(VPg)之间的相互作用。VPg 可以在无帽依赖翻译中充当帽类似物,并可能将 PAP 靶向含有非帽 IRES 的 RNA。在这项工作中,荧光光谱和 HPLC 技术被用于定量描述 PAP 脱嘌呤活性和 PAP-VPg 相互作用。PAP 与 VPg 具有高亲和力结合(29.5nm);反应是焓驱动的,有利于熵。此外,VPg 是 PAP 对麦胚裂解物中 RNA 脱嘌呤作用的有效抑制剂,并与来自烟草蚀纹病毒的结构 RNA 竞争 PAP 结合。VPg 可能通过抑制植物防御机制之一而获得进化优势,这也表明可能利用这种蛋白来对抗核糖体失活蛋白的细胞毒性活性。

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