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Sequence variation and immunologic cross-reactivity among Babesia bovis merozoite surface antigen 1 proteins from vaccine strains and vaccine breakthrough isolates

机译:来自疫苗株和疫苗突破分离株的牛杆状裂殖子裂殖子表面抗原1蛋白之间的序列变异和免疫交叉反应

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摘要

The Babesia bovis merozoite surface antigen 1 (MSA-1) is an immunodominant membrane glycoprotein that is the target of invasion-blocking antibodies. While antigenic variation has been demonstrated in MSA-1 among strains from distinct geographical areas, the extent of sequence variation within a region where it is endemic and the effect of variation on immunologic cross-reactivity have not been assessed. In this study, sequencing of MSA-1 from two Australian B. bovis vaccine strains and 14 breakthrough isolates from vaccinated animals demonstrated low sequence identity in the extracellular region of the molecule, ranging from 19.8 to 46.7% between the T vaccine strain and eight T vaccine breakthrough isolates, and from 18.7 to 99% between the K vaccine strain and six K vaccine breakthrough isolates. Although MSA-1 amino acid sequence varied substantially among strains, overall predicted regions of hydrophilicity and hydrophobicity in the extracellular domain were conserved in all strains examined, suggesting a conserved functional role for MSA-1 despite sequence polymorphism. Importantly, the antigenic variation created by sequence differences resulted in a lack of immunologic cross-reactivity among outbreak strains using sera from animals infected with the B. bovis vaccine strains. Additionally, sera from cattle hyperinfected with the Mexico strain of B. bovis and shown to be clinically immune did not cross-react with MSA-1 from any other isolate tested. The results indicate that isolates of B. bovis capable of evading vaccine-induced immunity contain an msa-1 gene that is significantly different from the msa-1 of the vaccine strain, and that the difference can result in a complete lack of cross-reactivity between MSA-1 from vaccine and breakthrough strains in immunized animals.
机译:牛巴贝斯虫裂殖子表面抗原1(MSA-1)是一种免疫显性膜糖蛋白,是入侵阻断抗体的靶标。尽管在来自不同地理区域的菌株中已在MSA-1中证明了抗原变异,但尚未评估其流行区域内序列变异的程度以及变异对免疫交叉反应性的影响。在这项研究中,对来自两个澳大利亚牛双歧杆菌疫苗株的MSA-1的测序和来自疫苗接种的动物的14个突破性分离株的测序表明,该分子的细胞外区域具有较低的序列同一性,在T疫苗株和八个T株之间介于19.8%至46.7%之间疫苗突破分离株,以及K疫苗株和6个K疫苗突破分离株之间的比率为18.7%至99%。尽管菌株之间的MSA-1氨基酸序列有很大不同,但是在所有检测的菌株中,细胞外域中亲水性和疏水性的总体预测区域均保守,这表明尽管序列多态性,MSA-1的功能仍保守。重要的是,由序列差异产生的抗原变异导致爆发菌株之间缺乏免疫交叉反应性,使用来自牛双歧杆菌疫苗菌株感染的动物的血清。此外,用牛双歧杆菌墨西哥感染高感染牛的血清,并显示出临床免疫力,它与来自任何其他测试分离株的MSA-1没有交叉反应。结果表明,能够逃避疫苗诱导的免疫力的牛双歧杆菌分离株包含与疫苗株的msa-1显着不同的msa-1基因,这种差异可能导致完全缺乏交叉反应性疫苗中的MSA-1与免疫动物中的突破菌株之间的差异。

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