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Extent of polymorphism and selection pressure on the Trypanosoma cruzi vaccine candidate antigen Tc24

机译:多态性和选择压力的程度,曲妥肌瘤患者候选抗原TC24

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摘要

Abstract Introduction Chagas disease, caused by the protozoan parasite Trypanosoma cruzi, is a major public health problem in the Americas, and existing drugs have severe limitations. In this context, a vaccine would be an attractive alternative for disease control. One of the difficulties in developing an effective vaccine lies in the high genetic diversity of T. cruzi. In this study, we evaluated the level of sequence diversity of the leading vaccine candidate Tc24 in multiple parasite strains. Methods and Results We quantified its level of polymorphism within and between T. cruzi discrete typing units (DTUs) and how this potential polymorphism is structured by different selective pressures. We observed a low level of polymorphism of Tc24 protein, weakly associated with parasite DTUs, but not with the geographic origin of the strains. In particular, Tc24 was under strong purifying selection pressure and predicted CD8+ T‐cell epitopes were mostly conserved. Tc24 strong conservation may be associated with structural/functional constrains to preserve EF hand domains and their calcium‐binding loops, and Tc24 is likely important for the parasite fitness. Discussion Together, these results show that a vaccine based on Tc24 is likely to be effective against a wide diversity of parasite strains across the American continent, and further development of this vaccine candidate should be a high priority.
机译:摘要介绍恰加斯病,引起的原生动物寄生虫克氏锥虫,是在美洲的主要公共卫生问题,和现有的药物有严重的局限性。在这种情况下,疫苗将是控制疾病的有吸引力的选择。一个在开发有效的疫苗就在于克氏锥虫的高遗传多样性的困难。在这项研究中,我们评估了领先的候选疫苗TC24多种寄生虫株的序列多样性的水平。方法和结果我们内和克氏锥虫离散打字单位(DTU的),以及如何这个潜在的多态性是由不同的选择压力,结构之间的定量其多态性水平。我们观察到TC24蛋白质,弱寄生虫的DTU相关的多态性的较低水平,但与菌株的地理来源。特别是,TC24是在强净化选择压力和预测的CD8 + T细胞表位大多是保守的。 TC24强大的保护可以与结构/功能约束相关联,以保持EF手域和它们的钙结合环,和TC24是寄生虫健身可能很重要。讨论总之,这些结果表明,基于TC24的疫苗可能是有效对抗横跨美洲大陆的寄生虫株,而这种候选疫苗的进一步发展的巨大差异应该是一个高优先级。

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