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Generation and characterization of potential dengue vaccine candidates based on domain III of the envelope protein and the capsid protein of the four serotypes of dengue virus

机译:基于四种登革热病毒血清型的包膜蛋白和衣壳蛋白III结构域的潜在登革热疫苗候选物的产生和表征

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摘要

Dengue is currently one of the most important arthropod-borne diseases, causing up to 25,000 deaths annually. There is currently no vaccine to prevent dengue virus infection, which needs a tetravalent vaccine approach. In this work, we describe the cloning and expression in Escherichia coli of envelope domain III-capsid chimeric proteins (DIIIC) of the four dengue serotypes as a tetravalent dengue vaccine candidate that is potentially able to generate humoral and cellular immunity. The recombinant proteins were purified to more than 85 % purity and were recognized by anti-dengue mouse and human sera. Mass spectrometry analysis verified the identity of the proteins and the correct formation of the intracatenary disulfide bond in the domain III region. The chimeric DIIIC proteins were also serotype-specific, and in the presence of oligonucleotides, they formed aggregates that were visible by electron microscopy. These results support the future use of DIIIC recombinant chimeric proteins in preclinical studies in mice for assessing their immunogenicity and efficacy.
机译:登革热是目前最重要的节肢动物传播疾病之一,每年导致25,000人死亡。当前没有预防登革热病毒感染的疫苗,这需要四价疫苗方法。在这项工作中,我们描述了作为四价登革热疫苗候选物的四种登革热血清型的包膜域III-衣壳嵌合蛋白(DIIIC)的克隆和在大肠杆菌中的表达,它有可能产生体液和细胞免疫。重组蛋白被纯化至超过85%的纯度,并被抗登革热小鼠和人类血清识别。质谱分析证实了蛋白质的身份以及结构域III区域中链内二硫键的正确形成。嵌合的DIIIC蛋白也是血清型特异性的,在寡核苷酸存在的情况下,它们形成的聚集体在电子显微镜下可见。这些结果支持DIIIC重组嵌合蛋白在小鼠临床前研究中的未来应用,以评估其免疫原性和功效。

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