Pangenome analysis of five representative Tropheryma whipplei strains following multiepitope-based vaccine design via immunoinformatic approaches.

IF 2.3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Ahmad Hasan, Muhammad Ibrahim, Wadi B Alonazi, Rongrong Yu, Bin Li
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Abstract

Whipple disease caused by Tropheryma whipplei a gram-positive bacterium is a systemic disorder that impacts not only the gastrointestinal tract but also the vascular system, joints, central nervous system, and cardiovascular system. Due to the lack of an approved vaccine, this study aimed to utilize immunoinformatic approaches to design multiepitope -based vaccine by utilizing the proteomes of five representative T. whipplei strains. The genomes initially comprised a total of 4,844 proteins ranging from 956 to 1012 proteins per strain. We collected 829 nonredundant lists of core proteins, that were shared among all the strains. Following subtractive proteomics, one extracellular protein, WP_033800108.1, a WhiB family transcriptional regulator, was selected for the chimeric-based multiepitope vaccine. Five immunodominant epitopes were retrieved from the WhiB family transcriptional regulator protein, indicating MHC-I and MHC-II with a global population coverage of 70.61%. The strong binding affinity, high solubility, nontoxicity, nonallergenic properties and high antigenicity scores make the selected epitopes more appropriate. Integration of the epitopes into a chimeric vaccine was carried out by applying appropriate adjuvant molecules and linkers, leading to the vaccine construct having enhanced immunogenicity and successfully eliciting both innate and adaptive immune responses. Moreover, the abilityof the vaccine to bind TLR4, a core innate immune receptor, was confirmed. Molecular dynamics simulations have also revealed the promising potential stability of the designed vaccine at 400 ns. In summary, we have designed a potential vaccine construct that has the ability not only to induce targeted immunogenicity for one strain but also for global T. whipplei strains. This study proposes a potential universal vaccine, reducing Whipple's disease risk and laying the groundwork for future research on multi-strain pathogens.

在通过免疫形式化方法进行基于多表的疫苗设计后,对五种具有代表性的 Tropheryma whipplei 株系进行庞基因组分析。
由革兰氏阳性细菌惠氏菌(Tropheryma whipplei)引起的惠普尔病是一种全身性疾病,不仅影响胃肠道,还影响血管系统、关节、中枢神经系统和心血管系统。由于缺乏已获批准的疫苗,本研究旨在利用免疫形式化方法,通过五种具有代表性的白喉杆菌菌株的蛋白质组来设计基于多位点的疫苗。这些基因组最初共包含 4844 个蛋白质,每个菌株的蛋白质数量从 956 个到 1012 个不等。我们收集了 829 个非冗余的核心蛋白列表,这些蛋白在所有菌株中都是共享的。经过减法蛋白质组学分析,我们选择了一种细胞外蛋白质 WP_033800108.1(一种 WhiB 家族转录调节因子)作为基于嵌合的多位点疫苗。从 WhiB 家族转录调控蛋白中检索到了五个免疫优势表位,分别指向 MHC-I 和 MHC-II,全球群体覆盖率为 70.61%。这些表位具有结合亲和力强、溶解度高、无毒、无致敏性和抗原性评分高等特点,因此更适合用于研究。通过应用适当的佐剂分子和连接体,将表位整合到嵌合疫苗中,使疫苗构建物具有更强的免疫原性,并成功激发先天性和适应性免疫反应。此外,疫苗与先天性免疫核心受体 TLR4 的结合能力也得到了证实。分子动力学模拟还揭示了所设计疫苗在 400 ns 时的潜在稳定性。总之,我们设计出了一种潜在的疫苗构建物,它不仅能诱导一种毒株的靶向免疫原性,还能诱导全球白喉杆菌毒株的靶向免疫原性。这项研究提出了一种潜在的通用疫苗,降低了惠普尔氏病的风险,并为未来对多菌株病原体的研究奠定了基础。
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
Molecular Genetics and Genomics
Molecular Genetics and Genomics 生物-生化与分子生物学
CiteScore
5.10
自引率
3.20%
发文量
134
审稿时长
1 months
期刊介绍: Molecular Genetics and Genomics (MGG) publishes peer-reviewed articles covering all areas of genetics and genomics. Any approach to the study of genes and genomes is considered, be it experimental, theoretical or synthetic. MGG publishes research on all organisms that is of broad interest to those working in the fields of genetics, genomics, biology, medicine and biotechnology. The journal investigates a broad range of topics, including these from recent issues: mechanisms for extending longevity in a variety of organisms; screening of yeast metal homeostasis genes involved in mitochondrial functions; molecular mapping of cultivar-specific avirulence genes in the rice blast fungus and more.
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