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水疱性口炎病毒(新泽西株)(奥格登株)的5'-末端序列:NS蛋白与负责异型干扰活性的NS结合位点之间的相互作用是怎样的?

The 5'-terminal sequence of VSV(NJ) (Ogden): is the interaction of the NS protein with the NS binding site responsible for heterotypic interference activity?

作者信息

Rud E W, Kang C Y

机构信息

Department of Microbiology and Immunology, University of Ottawa, Faculty of Health Sciences, Ontario, Canada.

出版信息

Virology. 1988 Jun;164(2):551-5. doi: 10.1016/0042-6822(88)90572-7.

Abstract

The 5'-terminal sequence of VSV(NJ) (Ogden) and VSV(NJ) (Hazelhurst) was compared in an attempt to understand why the defective interfering particle, DI-LT, heterotypically interferes with VSV(NJ) (Ogden) but not with VSV(NJ) (Hazelhurst). The 5'-terminal sequence of VSV(NJ) (Ogden) genomic RNA was determined by direct RNA sequencing and by DNA sequencing of cDNA clones of the 3'-terminal sequence of VSV(NJ) (Ogden) DI particle genome. Primer extension analysis of the 5'-terminus of VSV(NJ) (Ogden) standard genomic RNA confirmed these data. Within the last 47 nucleotides, equivalent to the negative-strand leader RNA, the only nucleotide changes between VSV(NJ) (Ogden) and VSV(NJ) (Hazelhurst) occur between nucleotides 19 and 26, representing part of the putative NS binding region described by Isaac and Keene (J. Virol. 43, 241-249 (1982] for VSV(IND) DI particles. The spacer (S) region, located between the polyadenylation signal of the L gene and the 47th nucleotide of the leader RNA, contains more differences. The polyadenylation signal of the L gene is fully conserved, but the remainder of the L gene region (177 nucleotides) has highly diverged between VSV(NJ) (Ogden) and VSV(NJ) (Hazelhurst). The changes in the NS binding region of the negative-strand leader RNA provide further evidence for the divergent evolution of VSV(NJ) (Ogden) and VSV(NJ) (Hazelhurst). The NS binding region has been implicated as a crucial site for the initiation of RNA transcription and replication. The interaction of the NS protein with this site may determine the ability of DI particles to interfere heterotypically.

摘要

比较了水疱性口炎病毒(新泽西株)(奥格登)和水疱性口炎病毒(新泽西株)(黑兹尔赫斯特)的5'末端序列,以试图理解为什么缺陷干扰颗粒DI-LT能异型干扰水疱性口炎病毒(新泽西株)(奥格登),却不能干扰水疱性口炎病毒(新泽西株)(黑兹尔赫斯特)。通过直接RNA测序以及对水疱性口炎病毒(新泽西株)(奥格登)DI颗粒基因组3'末端序列的cDNA克隆进行DNA测序,确定了水疱性口炎病毒(新泽西株)(奥格登)基因组RNA的5'末端序列。对水疱性口炎病毒(新泽西株)(奥格登)标准基因组RNA的5'末端进行引物延伸分析证实了这些数据。在相当于负链前导RNA的最后47个核苷酸内,水疱性口炎病毒(新泽西株)(奥格登)和水疱性口炎病毒(新泽西株)(黑兹尔赫斯特)之间唯一的核苷酸变化发生在第19至26个核苷酸之间,这代表了艾萨克和基恩(《病毒学杂志》43卷,241 - 249页[1982年])所描述的水疱性口炎病毒(印第安纳株)DI颗粒假定的NS结合区域的一部分。位于L基因聚腺苷酸化信号与前导RNA第47个核苷酸之间的间隔(S)区域差异更多。L基因的聚腺苷酸化信号完全保守,但L基因区域的其余部分(177个核苷酸)在水疱性口炎病毒(新泽西株)(奥格登)和水疱性口炎病毒(新泽西株)(黑兹尔赫斯特)之间有很大差异。负链前导RNA的NS结合区域的变化为水疱性口炎病毒(新泽西株)(奥格登)和水疱性口炎病毒(新泽西株)(黑兹尔赫斯特)的趋异进化提供了进一步证据。NS结合区域被认为是RNA转录和复制起始的关键位点。NS蛋白与该位点的相互作用可能决定DI颗粒异型干扰的能力。

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