首页> 美国卫生研究院文献>Journal of Parasitic Diseases: Official Organ of the Indian Society for Parasitology >Bioinformatics analysis of single and multi-hybrid epitopes of GRA-1 GRA-4 GRA-6 and GRA-7 proteins to improve DNA vaccine design against Toxoplasma gondii
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Bioinformatics analysis of single and multi-hybrid epitopes of GRA-1 GRA-4 GRA-6 and GRA-7 proteins to improve DNA vaccine design against Toxoplasma gondii

机译:GRA-1GRA-4GRA-6和GRA-7蛋白的单和多杂交表位的生物信息学分析以改善针对弓形虫的DNA疫苗设计

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摘要

Toxoplasma gondii, is a causative agent of morbidity and mortality in immunocompromised and congenitally-infected individuals. Attempts to construct DNA vaccines against T. gondii using surface proteins are increasing. The dense granule antigens are highly expressed in the acute and chronic phases of T. gondii infection and considered as suitable DNA vaccine candidates to control toxoplasmosis. In the present study, bioinformatics tools and online software were used to predict, analyze and compare the structural, physical and chemical characters and immunogenicity of the GRA-1, GRA-4, GRA-6 and GRA-7 proteins. Sequence alignment results indicated that the GRA-1, GRA-4, GRA-6 and GRA-7 proteins had low similarity. The secondary structure prediction demonstrated that among the four proteins, GRA-1 and GRA-6 had similar secondary structure except for a little discrepancy. Hydrophilicity/hydrophobicity analysis showed multiple hydrophilic regions and some classical high hydrophilic domains for each protein sequence. Immunogenic epitope prediction results demonstrated that the GRA-1 and GRA-4 epitopes were stable and GRA-4 showed the highest degree of antigenicity. Although the GRA-7 epitope had the highest score of immunogenicity, this epitope was instable and had the lowest degree of antigenicity and half-time in eukaryotic cell. Also, the results indicated that GRA4–GRA7 epitope and GRA6–GRA7 had the highest degree of antigenicity and immunogenicity among multi-hybrid epitopes, respectively. Totally, in the present study, single epitopes showed the highest degree of antigenicity compared with multi-hybrid epitopes. Given the results, it can be concluded that GRA-4 and GRA-7 can be powerful DNA vaccine candidates against T. gondii.
机译:弓形虫是免疫功能低下和先天感染个体中发病和死亡的病因。使用表面蛋白构建针对弓形虫的DNA疫苗的尝试正在增加。致密颗粒抗原在弓形虫感染的急性和慢性阶段高度表达,被认为是控制弓形虫病的合适DNA候选疫苗。在本研究中,使用生物信息学工具和在线软件来预测,分析和比较GRA-1,GRA-4,GRA-6和GRA-7蛋白的结构,理化特性和免疫原性。序列比对结果表明,GRA-1,GRA-4,GRA-6和GRA-7蛋白具有较低的相似性。二级结构预测表明,在四种蛋白质中,GRA-1和GRA-6具有相似的二级结构,只是差异很小。亲水性/疏水性分析显示每个蛋白序列有多个亲水性区域和一些经典的高亲水性结构域。免疫原性表位预测结果表明,GRA-1和GRA-4表位稳定,而GRA-4显示出最高的抗原性。尽管GRA-7表位具有最高的免疫原性评分,但该表位不稳定,在真核细胞中的抗原性和半衰期最低。同样,结果表明,在多杂交表位中,GRA4–GRA7表位和GRA6–GRA7分别具有最高的抗原性和免疫原性。总的来说,在本研究中,与多杂交表位相比,单个表位显示出最高的抗原性。根据结果​​,可以得出结论,GRA-4和GRA-7可能是抗弓形虫的强大DNA疫苗候选者。

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