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别具一格的抗原变异——疏螺旋体的故事

Antigenic variation with a twist--the Borrelia story.

作者信息

Norris Steven J

机构信息

Department of Pathology. University of Texas Medical School at Houston, PO Box 20708, Houston, TX 77225-0708, USA.

出版信息

Mol Microbiol. 2006 Jun;60(6):1319-22. doi: 10.1111/j.1365-2958.2006.05204.x.

Abstract

A common mechanism of immune evasion in pathogenic bacteria and protozoa is antigenic variation, in which genetic or epigenetic changes result in rapid, sequential shifts in a surface-exposed antigen. In this issue of Molecular Microbiology, Dai et al. provide the most complete description to date of the vlp/vsp antigenic variation system of the relapsing fever spirochaete, Borrelia hermsii. This elaborate, plasmid-encoded system involves an expression site that can acquire either variable large protein (vlp) or variable small protein (vsp) surface lipoprotein genes from 59 different archival copies. The archival vlp and vsp genes are arranged in clusters on at least five different plasmids. Gene conversion occurs through recombination events at upstream homology sequences (UHS) found in each gene copy, and at downstream homology sequences (DHS) found periodically among the vlp/vsp archival genes. Previous studies have shown that antigenic variation in relapsing fever Borrelia not only permits the evasion of host antibody responses, but can also result in changes in neurotropism and other pathogenic properties. The vlsE antigenic variation locus of Lyme disease spirochaetes, although similar in sequence to the relapsing fever vlp genes, has evolved a completely different antigenic variation mechanism involving segmental recombination from a contiguous array of vls silent cassettes. These two systems thus appear to represent divergence from a common precursor followed by functional convergence to create two distinct antigenic variation processes.

摘要

病原菌和原生动物中一种常见的免疫逃避机制是抗原变异,即基因或表观遗传变化导致表面暴露抗原快速、连续地转变。在本期《分子微生物学》中,戴等人提供了迄今为止对复发性发热螺旋体赫氏疏螺旋体的vlp/vsp抗原变异系统最完整的描述。这个复杂的、由质粒编码的系统涉及一个表达位点,该位点可以从59个不同的存档拷贝中获取可变大蛋白(vlp)或可变小蛋白(vsp)表面脂蛋白基因。存档的vlp和vsp基因在至少五个不同的质粒上成簇排列。基因转换通过每个基因拷贝中发现的上游同源序列(UHS)以及vlp/vsp存档基因中周期性出现的下游同源序列(DHS)处的重组事件发生。先前的研究表明,复发性发热疏螺旋体中的抗原变异不仅能使病原体逃避宿主抗体反应,还可能导致嗜神经性和其他致病特性的改变。莱姆病螺旋体的vlsE抗原变异位点虽然在序列上与复发性发热的vlp基因相似,但已经进化出一种完全不同的抗原变异机制,涉及从一系列连续的vls沉默盒中进行片段重组。因此,这两个系统似乎代表了从一个共同前体分化出来,随后功能趋同,从而产生了两个不同的抗原变异过程。

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