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一种针对盘尾丝虫病及相关丝虫病的新型多表位候选疫苗的计算设计与初步血清学分析

Computational Design and Preliminary Serological Analysis of a Novel Multi-Epitope Vaccine Candidate against Onchocerciasis and Related Filarial Diseases.

作者信息

Shey Robert Adamu, Ghogomu Stephen Mbigha, Shintouo Cabirou Mounchili, Nkemngo Francis Nongley, Nebangwa Derrick Neba, Esoh Kevin, Yaah Ntang Emmaculate, Manka'aFri Muyanui, Nguve Joel Ebai, Ngwese Roland Akwelle, Njume Ferdinand Ngale, Bertha Fru Asa, Ayong Lawrence, Njemini Rose, Vanhamme Luc, Souopgui Jacob

机构信息

Department of Biochemistry and Molecular Biology, Faculty of Science, University of Buea, Buea 99999, Cameroon.

Department of Molecular Biology, Institute of Biology and Molecular Medicine, IBMM, Université Libre de Bruxelles, Gosselies Campus, 6040 Gosselies, Belgium.

出版信息

Pathogens. 2021 Jan 21;10(2):99. doi: 10.3390/pathogens10020099.

Abstract

Onchocerciasis is a skin and eye disease that exerts a heavy socio-economic burden, particularly in sub-Saharan Africa, a region which harbours greater than 96% of either infected or at-risk populations. The elimination plan for the disease is currently challenged by many factors including amongst others; the potential emergence of resistance to the main chemotherapeutic agent, ivermectin (IVM). Novel tools, including preventative and therapeutic vaccines, could provide additional impetus to the disease elimination tool portfolio. Several observations in both humans and animals have provided evidence for the development of both natural and artificial acquired immunity. In this study, immuno-informatics tools were applied to design a filarial-conserved multi-epitope subunit vaccine candidate, (designated Ov-DKR-2) consisting of B-and T-lymphocyte epitopes of eight immunogenic antigens previously assessed in pre-clinical studies. The high-percentage conservation of the selected proteins and epitopes predicted in related nematode parasitic species hints that the generated chimera may be instrumental for cross-protection. Bioinformatics analyses were employed for the prediction, refinement, and validation of the 3D structure of the Ov-DKR-2 chimera In-silico immune simulation projected significantly high levels of IgG1, T-helper, T-cytotoxic cells, INF-γ, and IL-2 responses. Preliminary immunological analyses revealed that the multi-epitope vaccine candidate reacted with antibodies in sera from both onchocerciasis-infected individuals, endemic normals as well as loiasis-infected persons but not with the control sera from European individuals. These results support the premise for further characterisation of the engineered protein as a vaccine candidate for onchocerciasis.

摘要

盘尾丝虫病是一种皮肤和眼部疾病,会造成沉重的社会经济负担,尤其是在撒哈拉以南非洲地区,该地区感染或有感染风险的人群占比超过96%。目前,该疾病的消除计划面临诸多因素的挑战,其中包括对主要化疗药物伊维菌素(IVM)产生耐药性的潜在风险。新型工具,包括预防性和治疗性疫苗,可为疾病消除工具组合提供额外助力。在人类和动物身上的多项观察结果为自然获得性免疫和人工获得性免疫的发展提供了证据。在本研究中,免疫信息学工具被用于设计一种丝虫保守的多表位亚单位疫苗候选物(命名为Ov-DKR-2),它由之前在临床前研究中评估过的八种免疫原性抗原的B淋巴细胞和T淋巴细胞表位组成。所选蛋白质和表位在相关线虫寄生物种中的高保守率表明,所产生的嵌合体可能有助于交叉保护。采用生物信息学分析对Ov-DKR-2嵌合体的三维结构进行预测、优化和验证。计算机模拟免疫显示,IgG1、辅助性T细胞、细胞毒性T细胞、INF-γ和IL-2的反应水平显著较高。初步免疫学分析表明,该多表位疫苗候选物与盘尾丝虫病感染个体、地方性正常个体以及罗阿丝虫病感染个体血清中的抗体发生反应,但与欧洲个体的对照血清不发生反应。这些结果支持将该工程蛋白进一步表征为盘尾丝虫病疫苗候选物的前提。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/350f/7912539/202f9745dde9/pathogens-10-00099-g001.jpg

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