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Plasmodium vivax

机译:疟原虫vivax.

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摘要

Plasmodium vivax Cysteine-Rich Protective Antigen (CyRPA) is a merozoite protein participating in the parasite invasion of human reticulocytes. During natural P. vivax infection, antibody responses against PvCyRPA have been detected. In children, low anti-CyRPA antibody titers correlated with clinical protection, which suggests this protein as a potential vaccine candidate. This work analyzed the genetic and amino acid diversity of pvcyrpa in Mexican and global parasites. Consensus coding sequences of pvcyrpa were obtained from seven isolates. Other sequences were extracted from a repository. Maximum likelihood phylogenetic trees, genetic diversity parameters, linkage disequilibrium (LD), and neutrality tests were analyzed, and the potential amino acid polymorphism participation in B-cell epitopes was investigated. In 22 sequences from Southern Mexico, two synonymous and 21 nonsynonymous mutations defined nine private haplotypes. These parasites had the highest LD-R2 index and the lowest nucleotide diversity compared to isolates from South America or Asia. The nucleotide diversity and Tajima’s D values varied across the coding gene. The exon-1 sequence had greater diversity and Rm values than those of exon-2. Exon-1 had significant positive values for Tajima’s D, β-α values, and for the Z (HA: dN > dS) and MK tests. These patterns were similar for parasites of different origin. The polymorphic amino acid residues at PvCyRPA resembled the conformational B-cell peptides reported in PfCyRPA. Diversity at pvcyrpa exon-1 is caused by mutation and recombination. This seems to be maintained by balancing selection, likely due to selective immune pressure, all of which merit further study.
机译:富含疟原虫半胱氨酸的保护性抗原(Cyrpa)是参与寄生虫侵袭人网状细胞的Merozoite蛋白质。在天然p.Vivax感染期间,已经检测到针对pvcyrpa的抗体反应。在儿童中,低抗核糖抗体滴度与临床保护相关,这表明该蛋白质作为潜在的疫苗候选者。这项工作分析了墨西哥和全球寄生虫Pvcyrpa的遗传和氨基酸多样性。 PVCyrPA的共有编码序列是从七分离物中获得的。从储存库中提取其他序列。分析了最大似然性系统,遗传多样性参数,连接不平衡(LD)和中性试验,研究了潜在的氨基酸多态性参与B细胞表位。在墨西哥南部的22个序列中,两个同义词和21个非正式突变定义了九个私人单倍型。与南美洲或亚洲的分离物相比,这些寄生虫具有最高的LD-R2指数和最低的核苷酸多样性。核苷酸多样性和Tajima的D值在编码基因上变化。外显子-1序列具有比外部2-2更大的多样性和RM值。 Exon-1对Tajima的D,β-α值以及Z(HA:DN> DS)和MK测试具有显着的正值。这些模式类似于不同源的寄生虫。 Pvcyrpa的多态性氨基酸残基类似于Pfcyrpa中报道的构象B细胞肽。 Pvcyrpa Exon-1的多样性是由突变和重组引起的。这似乎通过平衡选择,可能是由于选择性免疫压力,所有这些都是进一步的研究。

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