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Probing the Rhipicephalus bursa Sialomes in Potential Anti-Tick Vaccine Candidates: A Reverse Vaccinology Approach

机译:在潜在的抗蜱疫苗候选中探究雷氏素苔藓氏鳞粉:反向疫苗学方法

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摘要

In the wake of the ‘omics’ explosion of data, reverse vaccinology approaches are being applied more readily as an alternative for the discovery of candidates for next generation diagnostics and vaccines. Promising protective antigens for the control of ticks and tick-borne diseases can be discovered by mining available omics data for immunogenic epitopes. The present study aims to explore the previously obtained Rhipicephalus bursa sialotranscriptome during both feeding and Babesia infection, to select antigenic targets that are either membrane-associated or a secreted protein, as well as unique to the ectoparasite and not present in the mammalian host. Further, they should be capable of stimulating T and B cells for a potential robust immune response, and be non-allergenic or toxic to the host. From the R. bursa transcriptome, 5706 and 3025 proteins were identified as belonging to the surfaceome and secretome, respectively. Following a reverse genetics immunoinformatics pipeline, nine preferred candidates, consisting of one transmembrane-related and eight secreted proteins, were identified. These candidates showed a higher predicted antigenicity than the Bm86 antigen, with no homology to mammalian hosts and exposed regions. Only four were functionally annotated and selected for further in silico analysis, which examined their protein structure, surface accessibility, flexibility, hydrophobicity, and putative linear B and T-cell epitopes. Regions with overlapping coincident epitopes groups (CEGs) were evaluated to select peptides that were further analyzed for their physicochemical characteristics, potential allergenicity, toxicity, solubility, and potential propensity for crystallization. Following these procedures, a set of three peptides from the three R. bursa proteins were selected. In silico results indicate that the designed epitopes could stimulate a protective and long-lasting immune response against those tick proteins, reflecting its potential as anti-tick vaccines. The immunogenicity of these peptides was evaluated in a pilot immunization study followed by tick feeding to evaluate its impact on tick behavior and pathogen transmission. Combining in silico methods with in vivo immunogenicity evaluation enabled the screening of vaccine candidates prior to expensive infestation studies on the definitive ovine host animals.
机译:在“OMICS的数据爆炸之后,逆向疫过程方法被更容易地应用于发现下一代诊断和疫苗的候选者的替代方案。可以通过用于免疫原性表位的可用OMICS数据来发现用于控制蜱和蜱传疾病的有前途的保护性抗原。本研究旨在探讨先前获得的Rapicephalus Bursa SialotorcareMome,以选择抗原靶,所述抗原靶点是膜相关的或分泌蛋白质,以及异醛酸盐的独特,而不是哺乳动物宿主。此外,它们应该能够刺激T和B细胞以进行潜在的鲁棒免疫应答,对宿主具有非过敏性或毒性。从R.Bursa转录组,5706和3025蛋白分别被鉴定为属于表面和沉淀物。在逆向遗传免疫信息管道之后,鉴定了由一种跨膜相关和8个分泌蛋白组成的九个优选的候选物。这些候选者显示出比BM86抗原更高的预测抗原,没有对哺乳动物宿主和暴露区域的同源性。只有四种在硅分析中进一步在功能上注释并选择,该分析检查了它们的蛋白质结构,表面可接近性,柔韧性,疏水性和推定的线性B和T细胞表位。评价具有重叠重合表位群(CEG)的区域以选择进一步分析其物理化学特性,潜在过敏性,毒性,溶解度和结晶潜在倾向的肽。在这些程序之后,选择了来自三种R. Bursa蛋白的一组三种肽。在Silico结果中,表明所设计的表位可以刺激对那些蜱蛋白的保护和长期的免疫应答,反映其作为抗蜱疫苗的潜力。在先导免疫研究中评价这些肽的免疫原性,然后评估滴定送料以评估其对蜱行为和病原体传递的影响。在体内免疫原性评价中结合硅方法,使得在昂贵的胚胎宿主动物的昂贵侵扰研究之前使疫苗候选患者筛选。

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