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硫代尿嘧啶交联质谱法:一种基于细胞的方法,用于鉴定参与病毒扩增的宿主因子。

Thiouracil cross-linking mass spectrometry: a cell-based method to identify host factors involved in viral amplification.

机构信息

Department of Microbiology, University of Alabama at Birmingham, Birmingham, Alabama, USA.

出版信息

J Virol. 2013 Aug;87(15):8697-712. doi: 10.1128/JVI.00950-13. Epub 2013 Jun 5.

Abstract

Eukaryotic RNA viruses are known to utilize host factors; however, the identity of these factors and their role in the virus life cycle remain largely undefined. Here, we report a method to identify proteins bound to the viral RNA during amplification in cell culture: thiouracil cross-linking mass spectrometry (TUX-MS). TUX-MS relies on incorporation of a zero-distance cross-linker into the viral RNA during infection. Proteins bound to viral RNA are cross-linked prior to cell lysis, purified, and identified using mass spectrometry. Using the TUX-MS method, an unbiased screen for poliovirus (PV) host factors was conducted. All host and viral proteins that are known to interact with the poliovirus RNA were identified. In addition, TUX-MS identified an additional 66 host proteins that have not been previously described in poliovirus amplification. From these candidates, eight were selected and validated. Furthermore, we demonstrate that small interfering RNA (siRNA)-mediated knockdown of two of these uncharacterized host factors results in either a decrease in copy number of positive-stranded RNA or a decrease in PV translation. These data demonstrate that TUX-MS is a robust, unbiased method to identify previously unknown host cell factors that influence virus growth. This method is broadly applicable to a range of RNA viruses, such as flaviviruses, alphaviruses, picornaviruses, bunyaviruses, and coronaviruses.

摘要

真核 RNA 病毒已知利用宿主因子;然而,这些因子的身份及其在病毒生命周期中的作用在很大程度上仍未确定。在这里,我们报告了一种在细胞培养中鉴定与病毒 RNA 结合的蛋白质的方法:硫代尿嘧啶交联质谱(TUX-MS)。TUX-MS 依赖于在感染过程中将零距离交联剂掺入病毒 RNA 中。在细胞裂解之前,将与病毒 RNA 结合的蛋白质交联,然后使用质谱进行纯化和鉴定。使用 TUX-MS 方法,对脊髓灰质炎病毒(PV)宿主因子进行了无偏筛选。鉴定出了所有已知与脊髓灰质炎病毒 RNA 相互作用的宿主和病毒蛋白。此外,TUX-MS 还鉴定出了另外 66 种以前未在脊髓灰质炎病毒扩增中描述过的宿主蛋白。从这些候选物中,选择并验证了八个。此外,我们证明,两种这些未表征的宿主因子的小干扰 RNA(siRNA)介导的敲低导致正链 RNA 的拷贝数减少或 PV 翻译减少。这些数据表明,TUX-MS 是一种强大的、无偏的方法,可以鉴定以前未知的影响病毒生长的宿主细胞因子。该方法广泛适用于一系列 RNA 病毒,如黄病毒、甲病毒、小 RNA 病毒、布尼亚病毒和冠状病毒。

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