Sen Adrish, Sen Nandini, Mackow Erich R
Department of Medicine, SUNY at Stony Brook, Stony Brook, NY 11794, USA.
J Virol. 2007 Nov;81(21):11758-67. doi: 10.1128/JVI.01124-07. Epub 2007 Aug 15.
The rotavirus NSP5 protein directs the formation of viroplasm-like structures (VLS) and is required for viroplasm formation within infected cells. In this report, we have defined signals within the C-terminal 21 amino acids of NSP5 that are required for VLS formation and that direct the insolubility and hyperphosphorylation of NSP5. Deleting C-terminal residues of NSP5 dramatically increased the solubility of N-terminally tagged NSP5 and prevented NSP5 hyperphosphorylation. Computer modeling and analysis of the NSP5 C terminus revealed the presence of an amphipathic alpha-helix spanning 21 C-terminal residues that is conserved among rotaviruses. Proline-scanning mutagenesis of the predicted helix revealed that single-amino-acid substitutions abolish NSP5 insolubility and hyperphosphorylation. Helix-disrupting NSP5 mutations also abolished localization of green fluorescent protein (GFP)-NSP5 fusions into VLS and directly correlate VLS formation with NSP5 insolubility. All mutations introduced into the hydrophobic face of the predicted NSP5 alpha-helix disrupted VLS formation, NSP5 insolubility, and the accumulation of hyperphosphorylated NSP5 isoforms. Some NSP5 mutants were highly soluble but still were hyperphosphorylated, indicating that NSP5 insolubility was not required for hyperphosphorylation. Expression of GFP containing the last 68 residues of NSP5 at its C terminus resulted in the formation of punctate VLS within cells. Interestingly, GFP-NSP5-C68 was diffusely dispersed in the cytoplasm when calcium was depleted from the medium, and after calcium resupplementation GFP-NSP5-C68 rapidly accumulated into punctate VLS. A potential calcium switch, formed by two tandem pseudo-EF-hand motifs (DxDxD), is present just upstream of the predicted alpha-helix. Mutagenesis of either DxDxD motif abolished the regulatory effect of calcium on VLS formation and resulted in the constitutive assembly of GFP-NSP5-C68 into punctate VLS. These results reveal specific residues within the NSP5 C-terminal domain that direct NSP5 hyperphosphorylation, insolubility, and VLS formation in addition to defining residues that constitute a calcium-dependent trigger of VLS formation. These studies identify functional determinants within the C terminus of NSP5 that regulate VLS formation and provide a target for inhibiting NSP5-directed VLS functions during rotavirus replication.
轮状病毒NSP5蛋白指导类病毒质体结构(VLS)的形成,是感染细胞内病毒质体形成所必需的。在本报告中,我们确定了NSP5 C末端21个氨基酸内的信号,这些信号是VLS形成所必需的,并且指导NSP5的不溶性和过度磷酸化。删除NSP5的C末端残基显著增加了N末端标记的NSP5的溶解度,并阻止了NSP5的过度磷酸化。对NSP5 C末端的计算机建模和分析揭示了存在一个跨越21个C末端残基的两亲性α螺旋,该螺旋在轮状病毒中保守。对预测螺旋的脯氨酸扫描诱变表明,单氨基酸取代消除了NSP5的不溶性和过度磷酸化。破坏螺旋的NSP5突变也消除了绿色荧光蛋白(GFP)-NSP5融合蛋白在VLS中的定位,并直接将VLS形成与NSP5的不溶性相关联。引入预测的NSP5α螺旋疏水面上的所有突变都破坏了VLS形成、NSP5不溶性和过度磷酸化的NSP5异构体的积累。一些NSP5突变体高度可溶,但仍过度磷酸化,表明过度磷酸化不需要NSP5不溶性。在其C末端表达含有NSP5最后6个残基的GFP导致细胞内点状VLS的形成。有趣的是,当培养基中钙耗尽时,GFP-NSP5-C68在细胞质中扩散分布,补充钙后,GFP-NSP5-C68迅速积累成点状VLS。在预测的α螺旋上游刚好存在一个由两个串联的假EF手基序(DxDxD)形成的潜在钙开关。对任一DxDxD基序的诱变消除了钙对VLS形成的调节作用,并导致GFP-NSP5-C68组成型组装成点状VLS。这些结果揭示了NSP5 C末端结构域内除了定义构成VLS形成的钙依赖性触发因素的残基外,还指导NSP5过度磷酸化、不溶性和VLS形成的特定残基。这些研究确定了NSP5 C末端内调节VLS形成的功能决定因素,并为在轮状病毒复制过程中抑制NSP5指导的VLS功能提供了一个靶点。
