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Molecular basis of size and antigenic variation of a Mycoplasma hominis adhesin encoded by divergent vaa genes.

机译:由不同的vaa基因编码的人支原体黏附素的大小和抗原变异的分子基础。

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摘要

The molecular basis for the size and antigenic diversity of the variable adherence-associated (Vaa) antigen, a major surface protein and a putative adhesin (of Mycoplasma hominis, is described. Size-variant alleles of the single-copy vaa gene encode abundant surface lipoproteins containing one to four nearly identical, tandem repetitive units of 121 amino acids in the central region of the mature Vaa product. Gain or loss of central repeats in vaa genes gives rise to distinct size-variant Vaa antigens in clonal populations of this organism. The N-terminal and repeat regions of Vaa contain highly conserved sequences, while the C-terminal region, implicated as the adherence-mediating module, is highly variable and divergent among different strains of this pathogen. Sequence variation in this region may underlie the strain-dependent binding of some monoclonal antibodies to Vaa products. The Vaa antigen is expressed in vivo during chronic, active arthritis associated with M. hominis infection and is highly immunogenic in the human host. Size variation and C-terminal antigenic divergence of Vaa could affect the adherence of M. hominis and evasion of antibody-mediated immunity, thereby contributing to the organism's adaptive capability in the human host. Variation in vaa genes reveals a distinct pattern of mutations generating mycoplasma surface variation.
机译:描述了可变黏附相关(Vaa)抗原,主要表面蛋白和假定黏附素(人支原体)的大小和抗原多样性的分子基础。单拷贝vaa基因的大小可变等位基因编码丰富的表面脂蛋白在成熟Vaa产物的中央区域含有1-4个几乎相同的串联重复单元,共121个氨基酸,vaa基因的中央重复序列的获得或缺失会在该生物的克隆种群中产生不同的大小可变的Vaa抗原。 Vaa的N末端和重复区域包含高度保守的序列,而C末端区域(作为粘附介导模块)则是高度可变的,并且在该病原体的不同菌株之间存在差异。单克隆抗体与Vaa产物的依赖结合Vaa抗原在与人型支原体感染相关的慢性活动性关节炎过程中在体内表达离子,在人类宿主中具有高度免疫原性。 Vaa的大小变化和C端抗原性差异可能会影响人型分枝杆菌的粘附以及抗体介导的免疫力的逃逸,从而有助于生物体在人类宿主中的适应能力。 vaa基因的变异揭示了产生支原体表面变异的独特变异模式。

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