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Construction and Evaluation of a Novel Recombinant T Cell Epitope-Based Vaccine against Coccidioidomycosis

机译:新型的针对球虫的重组T细胞表位为基础的疫苗的构建和评价

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Clinical and animal studies of coccidioidomycosis have demonstrated that activated CD4+ T lymphocytes are essential for protection against this fungal respiratory disease. We previously reported a vaccine against Coccidioides infection which contained three recombinant CD4+ T cell-reactive proteins and induced a robust, protective immune response in mice. Due to the anticipated high cost of production and clinical assessment of this multivalent vaccine, we generated a single protein which contained immunodominant T cell epitopes of the three polypeptides. Epitopes were initially identified by computational prediction of their ability to bind promiscuously to human major histocompatibility complex class II (MHC II) molecules. Cellular immunoassays confirmed the immunogenicity of the synthesized epitope peptides, while in vitro binding assays revealed a range of peptide affinity for MHC II. A DNA construct was synthesized for bacterial expression of a recombinant protein vaccine which contained five epitopes with the highest affinity for human MHC II, each fused with leader and spacer peptides proposed to optimize epitope processing and presentation to T cell receptors. Recall assays of immune T lymphocytes obtained from human MHC II-expressing HLA-DR4 transgenic mice confirmed that 4 of the 5 epitope peptides were processed. Mice immunized with the epitope-based vaccine admixed with a synthetic oligodeoxynucleotide adjuvant or loaded into yeast glucan particles and then challenged intranasally with Coccidioides showed early lung infiltration of activated T helper-1 (Th1), Th2, and Th17 cells, elevated gamma interferon (IFN-γ) and interleukin (IL)-17 production, significant reduction of fungal burden, and prolongation of survival compared to nonvaccinated mice. This is the first report of an epitope-based vaccine against coccidioidomycosis.
机译:球孢子菌病的临床和动物研究表明,活化的CD4 + T淋巴细胞对于预防这种真菌性呼吸道疾病至关重要。我们先前报道了一种针对球虫感染的疫苗,其中包含三种重组CD4 + T细胞反应性蛋白,并在小鼠中诱导了强大的保护性免疫应答。由于这种多价疫苗的生产和临床评估成本高昂,因此我们产生了包含三种多肽的免疫性T细胞表位的单一蛋白质。抗原决定簇最初是通过计算预测其与人类主要组织相容性复合物II类(MHC II)分子混杂结合的能力来确定的。细胞免疫测定证实了合成的表位肽的免疫原性,而体外结合测定揭示了对MHC II的一系列肽亲和力。合成用于细菌表达重组蛋白疫苗的DNA构建体,该重组蛋白疫苗包含五个对人MHC II具有最高亲和力的表位,每个表位均与前导肽和间隔肽融合在一起,从而优化了表位的加工和呈递给T细胞受体。从表达人MHC II的HLA-DR4转基因小鼠获得的免疫T淋巴细胞的召回分析证实,已加工了5个表位肽中的4个。用基于表位的疫苗免疫的小鼠与合成的寡聚脱氧核苷酸佐剂混合或装入酵母葡聚糖颗粒中,然后鼻内注射球孢菌素,表现出活化的T辅助细胞1(Th1),Th2和Th17细胞在肺部早期浸润,γ干扰素(与未接种疫苗的小鼠相比,IFN-γ和白介素(IL)-17的产生显着降低了真菌的负担,并延长了生存期。这是针对球虫的基于表位的疫苗的首次报道。

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