Multi-epitope Based Peptide Vaccine Candidate Against Babesia Infection From Rhoptry-Associated Protein 1 (RAP-1) Antigen Using Immuno-Informatics: An In Silico Approach.

IF 2.3 Q3 BIOCHEMICAL RESEARCH METHODS Bioinformatics and Biology Insights Pub Date : 2024-12-16 eCollection Date: 2024-01-01 DOI:10.1177/11779322241287114
Samson Anjikwi Malgwi, Victoria T Adeleke, Matthew Adekunle Adeleke, Moses Okpeku
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引用次数: 0

Abstract

Objective: Babesiosis is a significant haemoparasitic infection caused by apicomplexan parasites of the genus Babesia. This infection has continuously threatened cattle farmers owing to its devastating effects on productivity and severe economic implications. Failure to curb the increase of the infection has been attributed to largely ineffective vaccines. This study was designed to develop a potential vaccine candidate.

Method: Rhoptry-associated protein-1 (RAP-1) was used to identify and design a potential multi-epitope vaccine candidate due to its immunogenic properties through an immunoinformatics approach.

Results and conclusions: A multi-epitope vaccine comprising 11 CD8+, 17 CD4+, and 3 B-cell epitopes was constructed using the AAY, GPGPG, and KK linkers. Beta-defensin-3 was added as an adjuvant to potentiate the immune response using the EAAK linker. The designed vaccine was computationally predicted to be antigenic (antigenicity scores: 0.6), soluble (solubility index: 0.730), and non-allergenic. The vaccine construct comprises 595 amino acids with a molecular weight of 64 152 kDa, an instability and aliphatic index of 13.89 and 65.82, which confers stability with a Grand average of hydropathicity (GRAVY) value of 0.122, indicating the hydrophobicity of the construct. Europe has the highest combined class population coverage, with a percentage of 96.07%, while Central America has the lowest population coverage, with a value of 22.94%. The DNA sequence of the vaccine construct was optimized and successfully cloned into a pET-28a (+) plasmid vector. Analysis of binding interactions indicated the stability of the complex when docked with Toll-like receptor-2 (TLR-2). The subunit vaccine construct was predicted to induce and boost sufficient host cellular and humoral responses in silico. However, further experimental research and analysis is required to validate the findings.

Limitation: This study is purely computational, and further experimental validation of these findings through in vivo and in vitro conditions is required.

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利用免疫信息学从Rhoptry-Associated Protein 1 (RAP-1)抗原中提取多表位抗巴贝斯虫感染的多肽候选疫苗:硅学方法。
目的:巴贝斯虫病是由巴贝斯虫属顶复体寄生虫引起的一种重要的血液寄生虫感染。由于这种感染对生产力的破坏性影响和严重的经济影响,一直威胁着养牛户。未能遏制感染增加的原因主要是疫苗无效。本研究旨在开发一种潜在的候选疫苗。方法:利用鼠状体相关蛋白1 (rap1)的免疫原性,通过免疫信息学方法鉴定和设计一种潜在的多表位候选疫苗。结果和结论:使用AAY、GPGPG和KK连接体构建了包含11个CD8+、17个CD4+和3个b细胞表位的多表位疫苗。加入β -防御素-3作为佐剂,利用EAAK连接体增强免疫反应。通过计算预测,设计的疫苗具有抗原性(抗原性评分:0.6)、可溶性(溶解度指数:0.730)和非致敏性。该疫苗构建体包含595个氨基酸,分子量为64 152 kDa,不稳定性和脂肪族指数分别为13.89和65.82,具有稳定性,亲水性(GRAVY)的大平均值为0.122,表明该构建体具有疏水性。欧洲的综合阶层人口覆盖率最高,为96.07%,而中美洲的人口覆盖率最低,为22.94%。优化疫苗构建体DNA序列,成功克隆到pET-28a(+)质粒载体上。结合相互作用分析表明,当与toll样受体-2 (TLR-2)对接时,该复合物具有稳定性。亚单位疫苗构建预测诱导和促进足够的宿主细胞和体液反应在硅。然而,需要进一步的实验研究和分析来验证这些发现。局限性:本研究是纯计算性的,需要进一步通过体内和体外条件对这些发现进行实验验证。
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
Bioinformatics and Biology Insights
Bioinformatics and Biology Insights BIOCHEMICAL RESEARCH METHODS-
CiteScore
6.80
自引率
1.70%
发文量
36
审稿时长
8 weeks
期刊介绍: Bioinformatics and Biology Insights is an open access, peer-reviewed journal that considers articles on bioinformatics methods and their applications which must pertain to biological insights. All papers should be easily amenable to biologists and as such help bridge the gap between theories and applications.
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