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Potyviridae 家族多聚蛋白切割位点的概述与分析。

Overview and analysis of the polyprotein cleavage sites in the family Potyviridae.

机构信息

Plant-Pathogen Interactions Division, Rothamsted Research, Harpenden, Herts. AL5 2JQ, UK.

出版信息

Mol Plant Pathol. 2005 Jul 1;6(4):471-87. doi: 10.1111/j.1364-3703.2005.00296.x.

DOI:10.1111/j.1364-3703.2005.00296.x
PMID:20565672
Abstract

SUMMARY The genomes of plant viruses in the family Potyviridae encode large polyproteins that are cut by virus-encoded proteases into ten mature proteins. Three different types of protease have been identified, each of which cuts at sites with a distinctive sequence pattern. The experimental evidence for this specificity is reviewed and the cleavage site patterns are compiled for all sequenced species within the family. Seven of the nine cleavage sites in each species are cut by the viral NIa-Pro and patterns around these sites are related where possible to the active site-substrate interactions recently deduced following the resolution of the crystal structure of Tobacco etch virus (TEV) NIa-Pro (Phan et al., 2002. J. Biol. Chem. 277, 50564-50572). In particular, a revised series of cleavage sites for Sweet potato mild mottle virus (genus Ipomovirus) is proposed with a conserved His at the P1 position. This is supported by homology modelling studies using the TEV structure as a template. The data also provide a standard to correct the annotation of some other published sequences and to help predict these sites in further virus sequences as they become available. Comprehensive data for all sequences of each virus in the family, together with some summaries, have been made available at http://www.rothamsted.bbsrc.ac.uk/ppi/links/pplinks/potycleavage/index.html.

摘要

摘要

在马铃薯 Y 病毒科中,病毒基因组编码的多聚蛋白由病毒编码的蛋白酶切割成 10 个成熟蛋白。现已鉴定出 3 种不同类型的蛋白酶,它们在具有独特序列模式的位点进行切割。本文回顾了这些特异性的实验证据,并为该科中所有测序的病毒物种编译了切割位点模式。在每个物种中,有 7 个 9 个切割位点由病毒的 NIa-Pro 切割,并且尽可能地将这些位点周围的模式与最近根据烟草蚀纹病毒(TEV)NIa-Pro 的晶体结构解析得出的活性部位-底物相互作用的结论相关联(Phan 等人,2002 年。J. Biol. Chem. 277,50564-50572)。特别是,建议对甘薯轻斑驳病毒(属 Ipomovirus)的一系列新的切割位点进行保守性分析,其中 P1 位有一个保守的组氨酸。这一观点得到了使用 TEV 结构作为模板的同源建模研究的支持。该数据还为校正其他一些已发表序列的注释提供了标准,并有助于预测这些位点在进一步病毒序列中的可用性。该家族中每种病毒的所有序列的综合数据,以及一些摘要,都可以在 http://www.rothamsted.bbsrc.ac.uk/ppi/links/pplinks/potycleavage/index.html 上获得。

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