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首页> 外文期刊>EBioMedicine >A single-dose plasmid-launched live-attenuated Zika vaccine induces protective immunity
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A single-dose plasmid-launched live-attenuated Zika vaccine induces protective immunity

机译:单剂量质粒发射的减毒活寨卡疫苗诱导保护性免疫

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Background Vaccines are the most effective means to fight and eradicate infectious diseases. Live-attenuated vaccines (LAV) usually have the advantages of single dose, rapid onset of immunity, and durable protection. DNA vaccines have the advantages of chemical stability, ease of production, and no cold chain requirement. The ability to combine the strengths of LAV and DNA vaccines may transform future vaccine development by eliminating cold chain and cell culture with the potential for adventitious agents. Methods A DNA-launched LAV was developed for ZIKV virus (ZIKV), a pathogen that recently caused a global public health emergency. The cDNA copy of a ZIKV LAV genome was engineered into a DNA plasmid. The DNA-LAV plasmid was delivered into mice using a clinically proven device TriGrid? to launch the replication of LAV. Findings A single-dose immunization as low as 0.5?μg of DNA-LAV plasmid conferred 100% seroconversion in A129 mice. All seroconverted mice developed sterilizing immunity, as indicated by no detectable infectious viruses and no increase of neutralizing antibody titers after ZIKV challenge. The immunization also elicited robust T cell responses. In pregnant mice, the DNA-LAV vaccination fully protected against ZIKV-induced disease and maternal-to-fetal transmission. High levels of neutralizing activities were detected in fetal serum, indicating maternal-to-fetal humoral transfer. In male mice, a single-dose vaccination completely prevented testis infection, injury, and oligospermia. Interpretation The remarkable simplicity and potency of ZIKV DNA-LAV warrant further development of this vaccine candidate. The DNA-LAV approach may serve as a universal vaccine platform for other plus-sense RNA viruses. Fund National Institute of Health, Kleberg Foundation , Centers for Disease Control and Prevention , University of Texas Medical Branch.
机译:背景疫苗是对抗和根除传染病的最有效手段。减毒活疫苗(LAV)通常具有单剂量,免疫快速发作和持久保护的优势。 DNA疫苗具有化学稳定性,易于生产且无需冷链的优点。结合LAV和DNA疫苗优势的能力可能会消除冷链和细胞培养,并具有潜在的不定因素可能会改变未来的疫苗开发。方法针对最近导致全球公共卫生突发事件的病原体ZIKV病毒(ZIKV)开发了DNA发射的LAV。 ZIKV LAV基因组的cDNA拷贝被工程化为DNA质粒。 DNA-LAV质粒是使用经过临床验证的设备TriGrid?传递给小鼠的。启动LAV的复制。结果一次低剂量的DNA-LAV质粒单次免疫接种可导致A129小鼠100%的血清转化。 ZIKV攻击后,所有经血清转化的小鼠均产生了灭菌免疫力,如未检测到感染性病毒且中和抗体滴度没有增加。免疫还引起了强烈的T细胞反应。在怀孕的小鼠中,DNA-LAV疫苗接种可完全预防ZIKV诱导的疾病和母婴传播。在胎儿血清中检测到高水平的中和活性,表明母体之间的体液转移。在雄性小鼠中,单剂量疫苗接种可以完全防止睾丸感染,损伤和少精子症。解释ZIKV DNA-LAV的显着简单性和效力保证了该候选疫苗的进一步开发。 DNA-LAV方法可作为其他正向RNA病毒的通用疫苗平台。德克萨斯大学医学分院疾病控制和预防中心Kleberg基金会国家卫生研究所基金。

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