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Molecular basis of Mycoplasma surface antigenic variation: a novel set of divergent genes undergo spontaneous mutation of periodic coding regions and 5 regulatory sequences.

机译:支原体表面抗原变异的分子基础:一组新的趋异基因经历周期性编码区和5调控序列的自发突变。

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摘要

Antigenic diversity is generated in the wall-less pathogen Mycoplasma hyorhinis by combinatorial expression and phase variation of multiple, size-variant membrane surface lipoproteins (Vlps). The unusual structural basis for Vlp variation was revealed in a cluster of related but divergent vlp genes, vlpA, vlpB and vlpC, which occur as single chromosomal copies. These encode conserved N-terminal domains for membrane insertion and lipoprotein processing, but divergent external domains undergoing size variation by loss or gain of repetitive intragenic coding sequences while retaining a motif with distinctive charge distribution. Genetic analysis of phenotypically switched isogenic lineages representing ON or OFF expression states of Vlp products ruled out chromosomal rearrangement or frameshift mutations as mechanisms for Vlp phase variation. However, highly conserved vlp promoter regions contain a tract of contiguous A residues immediately upstream of the -10 box which is subject to frequent mutations altering its length in exact correspondence with the ON and OFF phase states of specific genes. This suggests a mechanism of transcriptional control regulating high frequency phase variation and random combinatorial expression of Vlps. The multiple levels of diversity embodied in the vlp gene cluster represents a novel adaptive capability particularly suited for this class of wall-less microbe.
机译:通过多种大小变化的膜表面脂蛋白(Vlps)的组合表达和相变,在无壁病原体支原体支原体中产生了抗原多样性。 Vlp变异的异常结构基础在一组相关但彼此不同的vlp基因vlpA,vlpB和vlpC中揭示,它们以单个染色体拷贝的形式出现。它们编码用于膜插入和脂蛋白加工的保守的N-末端结构域,但是通过重复的基因内编码序列的丢失或获得而经历尺寸变化的发散的外部结构域,同时保留具有独特电荷分布的基序。代表Vlp产物ON或OFF表达状态的表型转换同基因谱系的遗传分析排除了染色体重排或移码突变作为Vlp相变的机制。但是,高度保守的vlp启动子区域在-10框的上游立即包含大量连续的A残基,该残基经常发生突变,其长度发生变化,与特定基因的ON和OFF相态完全一致。这表明转录控制调节高频相位变化和Vlps的随机组合表达的机制。 vlp基因簇中体现的多样性的多重水平代表了一种新的适应能力,特别适合此类无壁微生物。

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