Cornu T I, de la Torre J C
Division of Virology, Department of Neuropharmacology, The Scripps Research Institute, La Jolla, California 92037, USA.
J Virol. 2001 Oct;75(19):9415-26. doi: 10.1128/JVI.75.19.9415-9426.2001.
Arenaviruses have a bisegmented negative-strand RNA genome whose proteomic capability is limited to only four polypeptides, namely, nucleoprotein (NP), surface glycoprotein (GP) that is proteolytically processed into GP1+GP2, polymerase (L), and a small (11-kDa) RING finger protein (Z). The role of Z during the Lymphocytic choriomeningitis virus (LCMV) life cycle is poorly understood. We investigated the function of Z in virus transcription and replication by using a reverse genetic system for the prototypic arenavirus LCMV. This system involves an LCMV minigenome and the minimal viral trans-acting factors (NP and L), expressed from separated cotransfected plasmids. Cotransfection of the Z cDNA strongly inhibited LCMV minigenome expression. The effect required synthesis of Z protein; its magnitude was dose dependent and occurred with levels of Z protein substantially lower than those observed in LCMV-infected cells. Coexpression of Z did not prevent the encapsidation of plasmid supplied minigenome, but it affected both transcription and RNA replication similarly. Mutations in Z that unfolded its RING finger domain eliminated its inhibitory activity, but RING proteins not related to Z did not affect LCMV minigenome expression. Consistent with the minigenome results, cells transiently expressing Z exhibited decreased susceptibility to infection with LCMV.
沙粒病毒具有双节段负链RNA基因组,其蛋白质组能力仅限于四种多肽,即核蛋白(NP)、经蛋白水解加工成GP1+GP2的表面糖蛋白(GP)、聚合酶(L)和一种小的(11 kDa)泛素连接酶E3(Z)。Z在淋巴细胞性脉络丛脑膜炎病毒(LCMV)生命周期中的作用尚不清楚。我们通过使用原型沙粒病毒LCMV的反向遗传系统研究了Z在病毒转录和复制中的功能。该系统涉及一个LCMV微型基因组和从单独共转染质粒表达的最小病毒反式作用因子(NP和L)。Z cDNA的共转染强烈抑制LCMV微型基因组的表达。这种作用需要合成Z蛋白;其强度呈剂量依赖性,并且在Z蛋白水平远低于LCMV感染细胞中观察到的水平时就会出现。Z的共表达并不阻止质粒提供的微型基因组的衣壳化,但它对转录和RNA复制的影响类似。Z中使其泛素连接酶E3结构域展开的突变消除了其抑制活性,但与Z无关的泛素连接酶E3不影响LCMV微型基因组的表达。与微型基因组结果一致,瞬时表达Z的细胞对LCMV感染的敏感性降低。
