Martínez-Sobrido Luis, Zúñiga Elina I, Rosario Debralee, García-Sastre Adolfo, de la Torre Juan Carlos
Molecular Integrative Neuroscience Department (MIND), The Scripps Research Institute, IMM-6, 10550 N. Torrey Pines Road, La Jolla, CA 92037, USA.
J Virol. 2006 Sep;80(18):9192-9. doi: 10.1128/JVI.00555-06.
The prototypic arenavirus lymphocytic choriomeningitis virus (LCMV) is a formidable battle horse for the study of viral immunology, as well as viral persistence and associated diseases. Investigations with LCMV have uncovered basic mechanisms by which viruses avoid elimination by the host adaptive immune response. In this study we show that LCMV also disables the host innate defense by interfering with beta interferon (IFN-beta) production in response to different stimuli, including infection with Sendai virus and liposome-mediated DNA transfection. Inhibition of IFN production in LCMV-infected cells was caused by an early block in the IFN regulatory factor 3 (IRF-3) activation pathway. This defect was restored in cells cured of LCMV, indicating that one or more LCMV products are responsible for the inhibition of IRF-3 activation. Using expression plasmids encoding individual LCMV proteins, we found that expression of the LCMV nucleoprotein (NP) was sufficient to inhibit both IFN production and nuclear translocation of IRF-3. To our knowledge, this is the first evidence of an IFN-counteracting viral protein in the Arenaviridae family. Inhibition of IFN production by the arenavirus NP is likely to be a determinant of virulence in vivo.
原型沙粒病毒淋巴细胞性脉络丛脑膜炎病毒(LCMV)是病毒免疫学、病毒持续性感染及相关疾病研究中的一个重要对象。对LCMV的研究揭示了病毒逃避宿主适应性免疫反应清除的基本机制。在本研究中,我们发现LCMV还通过干扰β干扰素(IFN-β)对不同刺激(包括仙台病毒感染和脂质体介导的DNA转染)的产生来破坏宿主的固有防御。LCMV感染细胞中IFN产生的抑制是由IFN调节因子3(IRF-3)激活途径的早期阻断引起的。在清除LCMV的细胞中,这一缺陷得以恢复,表明一种或多种LCMV产物是IRF-3激活抑制的原因。使用编码单个LCMV蛋白的表达质粒,我们发现LCMV核蛋白(NP)的表达足以抑制IFN产生和IRF-3的核转位。据我们所知,这是沙粒病毒科中一种IFN拮抗病毒蛋白的首个证据。沙粒病毒NP对IFN产生的抑制可能是体内毒力的一个决定因素。
