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禽呼肠孤病毒L2基因组片段序列以及所编码的依赖RNA的RNA聚合酶蛋白的预测结构/功能

Avian reovirus L2 genome segment sequences and predicted structure/function of the encoded RNA-dependent RNA polymerase protein.

作者信息

Xu Wanhong, Coombs Kevin M

机构信息

Department of Medical Microbiology and Infectious Diseases, University of Manitoba, Manitoba, Canada.

出版信息

Virol J. 2008 Dec 17;5:153. doi: 10.1186/1743-422X-5-153.

Abstract

BACKGROUND

The orthoreoviruses are infectious agents that possess a genome comprised of 10 double-stranded RNA segments encased in two concentric protein capsids. Like virtually all RNA viruses, an RNA-dependent RNA polymerase (RdRp) enzyme is required for viral propagation. RdRp sequences have been determined for the prototype mammalian orthoreoviruses and for several other closely-related reoviruses, including aquareoviruses, but have not yet been reported for any avian orthoreoviruses.

RESULTS

We determined the L2 genome segment nucleotide sequences, which encode the RdRp proteins, of two different avian reoviruses, strains ARV138 and ARV176 in order to define conserved and variable regions within reovirus RdRp proteins and to better delineate structure/function of this important enzyme. The ARV138 L2 genome segment was 3829 base pairs long, whereas the ARV176 L2 segment was 3830 nucleotides long. Both segments were predicted to encode lambdaB RdRp proteins 1259 amino acids in length. Alignments of these newly-determined ARV genome segments, and their corresponding proteins, were performed with all currently available homologous mammalian reovirus (MRV) and aquareovirus (AqRV) genome segment and protein sequences. There was approximately 55% amino acid identity between ARV lambdaB and MRV lambda3 proteins, making the RdRp protein the most highly conserved of currently known orthoreovirus proteins, and there was approximately 28% identity between ARV lambdaB and homologous MRV and AqRV RdRp proteins. Predictive structure/function mapping of identical and conserved residues within the known MRV lambda3 atomic structure indicated most identical amino acids and conservative substitutions were located near and within predicted catalytic domains and lining RdRp channels, whereas non-identical amino acids were generally located on the molecule's surfaces.

CONCLUSION

The ARV lambdaB and MRV lambda3 proteins showed the highest ARV:MRV identity values (approximately 55%) amongst all currently known ARV and MRV proteins. This implies significant evolutionary constraints are placed on dsRNA RdRp molecules, particularly in regions comprising the canonical polymerase motifs and residues thought to interact directly with template and nascent mRNA. This may point the way to improved design of anti-viral agents specifically targeting this enzyme.

摘要

背景

正呼肠孤病毒是一种感染性因子,其基因组由10个双链RNA片段组成,包裹在两个同心蛋白质衣壳中。与几乎所有RNA病毒一样,病毒繁殖需要一种依赖RNA的RNA聚合酶(RdRp)。已确定了原型哺乳动物正呼肠孤病毒以及包括水生呼肠孤病毒在内的其他几种密切相关呼肠孤病毒的RdRp序列,但尚未有任何禽正呼肠孤病毒的相关报道。

结果

我们测定了两种不同禽呼肠孤病毒ARV138和ARV176编码RdRp蛋白的L2基因组片段核苷酸序列,以确定呼肠孤病毒RdRp蛋白内的保守和可变区域,并更好地描绘这种重要酶的结构/功能。ARV138的L2基因组片段长3829个碱基对,而ARV176的L2片段长3830个核苷酸。两个片段预计都编码长度为1259个氨基酸的λB RdRp蛋白。将这些新确定的禽呼肠孤病毒基因组片段及其相应蛋白与所有目前可用的同源哺乳动物呼肠孤病毒(MRV)和水生呼肠孤病毒(AqRV)基因组片段及蛋白序列进行比对。禽呼肠孤病毒λB与哺乳动物呼肠孤病毒λ3蛋白之间的氨基酸同一性约为55%,这使得RdRp蛋白成为目前已知正呼肠孤病毒蛋白中保守性最高的蛋白,禽呼肠孤病毒λB与同源的哺乳动物呼肠孤病毒和水生呼肠孤病毒RdRp蛋白之间的同一性约为28%。在已知的哺乳动物呼肠孤病毒λ3原子结构内对相同和保守残基进行预测性结构/功能图谱分析表明,大多数相同氨基酸和保守取代位于预测的催化结构域附近和内部以及RdRp通道内,而非相同氨基酸通常位于分子表面。

结论

在所有目前已知的禽呼肠孤病毒和哺乳动物呼肠孤病毒蛋白中,禽呼肠孤病毒λB和哺乳动物呼肠孤病毒λ3蛋白显示出最高的禽呼肠孤病毒与哺乳动物呼肠孤病毒同一性值(约55%)。这意味着双链RNA RdRp分子受到显著的进化限制,特别是在包含规范聚合酶基序和被认为直接与模板及新生mRNA相互作用的残基的区域。这可能为专门针对该酶的抗病毒药物的改进设计指明方向。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bc31/2615760/ff29fff4c2b6/1743-422X-5-153-1.jpg

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