In silico study to predict promiscuous peptides for immunodiagnosis of cystic echinococcosis.

Q3 Medicine
Tropical Parasitology Pub Date : 2023-01-01 Epub Date: 2023-05-19 DOI:10.4103/tp.tp_70_22
Varun Chauhan, Azhar Khan, Umar Farooq
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引用次数: 0

Abstract

Background: Cystic echinococcosis (CE), caused by Echinococcus granulosus, is a major zoonotic disease that causes significant human morbidity and mortality. This cosmopolitan disease is difficult to diagnose, treat, and control. So far, crude extracts of hydatid cyst fluid containing antigen B or antigen 5 have been used as the primary antigenic source for its immunodiagnosis. The main issue is that it reacts with sera from people infected with other helminths. There is currently no standard, specific, or sensitive test for disease diagnosis, and no human vaccine has been reported.

Aims and objectives: Considering the need for efficient immunization and/or immunodiagnosis, six E. granulosus antigens, antigen 5, antigen B, heat shock proteins such as Hsp-8 and Hsp-90, phosphoenolpyruvate carboxykinase, and tetraspanin-1, were chosen.

Materials and methods: Using various in silico tools, T cell and B cell epitopes (promiscuous peptides) were predicted by targeting antigen 5, antigen B, heat shock proteins such as Hsp-8 and Hsp-90, phosphoenolpyruvate carboxykinase, and tetraspanin-1.

Results: There are twelve promiscuous peptides with overlapping human leukocyte antigen (HLA) class-I, class-II, and conformational B cell epitopes. Such immunodominant peptides could be useful as subunit vaccines. Furthermore, six peptides specific for E. granulosus were also discovered, which may prove to be important markers in the diagnosis of CE, potentially preventing misdiagnosis and mismanagement.

Conclusion: These epitopes may be the most important vaccine targets in E. granulosus because they have the most promiscuous peptides and B cell epitopes, as well as the highest affinity for different alleles, as determined by docking scores. However, additional research using in vitro and in vivo models is undertaken.

Abstract Image

Abstract Image

预测混杂肽用于囊性棘球蚴病免疫诊断的计算机研究。
背景:由细粒棘球蚴引起的囊性棘球蚴病(CE)是一种主要的人畜共患疾病,可导致显著的人类发病率和死亡率。这种世界性疾病很难诊断、治疗和控制。迄今为止,含有抗原B或抗原5的棘球蚴囊液粗提物已被用作其免疫诊断的主要抗原来源。主要问题是它会与感染其他蠕虫的人的血清发生反应。目前还没有标准的、特异的或敏感的疾病诊断测试,也没有人类疫苗的报道。目的:考虑到高效免疫和/或免疫诊断的需要,选择了6种颗粒大肠杆菌抗原,抗原5、抗原B、热休克蛋白如Hsp-8和Hsp-90、磷酸烯醇丙酮酸羧激酶和四spanin-1。材料和方法:使用各种计算机工具,通过靶向抗原5、抗原B、热休克蛋白如Hsp-8和Hsp-90、磷酸烯醇丙酮酸羧激酶和四氢叶酸1来预测T细胞和B细胞表位(混杂肽),和构象B细胞表位。这种免疫优势肽可以用作亚单位疫苗。此外,还发现了六种颗粒大肠杆菌特异性肽,这些肽可能被证明是诊断CE的重要标志物,有可能防止误诊和管理不善。结论:这些表位可能是颗粒大肠杆菌最重要的疫苗靶点,因为它们具有最混杂的肽和B细胞表位,并且对不同等位基因的亲和力最高,这是通过对接得分确定的。然而,使用体外和体内模型进行了额外的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Tropical Parasitology
Tropical Parasitology Medicine-Infectious Diseases
CiteScore
2.40
自引率
0.00%
发文量
12
期刊介绍: Tropical Parasitology, a publication of Indian Academy of Tropical Parasitology, is a peer-reviewed online journal with Semiannual print on demand compilation of issues published. The journal’s full text is available online at www.tropicalparasitology.org. The journal allows free access (Open Access) to its contents and permits authors to self-archive final accepted version of the articles on any OAI-compliant institutional / subject-based repository. The journal will cover technical and clinical studies related to health, ethical and social issues in field of parasitology. Articles with clinical interest and implications will be given preference.
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