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Efficacy and safety of a modified vaccinia Ankara (MVA) vectored plague vaccine in mice

机译:改良牛痘安卡拉(MVA)载体鼠疫疫苗在小鼠中的功效和安全性

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摘要

The efficacy and safety of plague vaccines based on the modified vaccinia Ankara (MVA) viral vector was evaluated. MVA recombinants were constructed expressing Yersinia pestis antigens under the translational control of the encephalomyocarditis virus (EMCV) internal ribosomal entry site (IRES) and/or fused to the tissue plasminogen activator (tPA) secretory signal. A MVA/Y. pestis recombinant that expressed a truncated version of the low-calcium response V antigen (MVA/IRES/tPA/V-307), conferred significant protection (87.5-100%) against intranasal or intraperitoneal challenge with CO92 (encapsulated) or Java 9 (non-encapsulated) strains of Y. pestis, respectively. In contrast, a MVA/Y. pestis recombinant that expressed the full-length V antigen provided only 37.5% protection against challenge with CO92 or Java 9 strains, respectively. Interestingly, a MVA/Y. pestis recombinant that expressed the capsular protein (F1) did not elicit significant antibody titers but still conferred 50% and 25% protection against CO92 or Java 9 challenge, respectively. The MVA/Y. pestis recombinant viruses did not demonstrate any mortality or morbidity in SCID mice. Based on their safety and efficacy in mice, these MVA/Y. pestis recombinants are candidates for further development as biodefense and public health vaccines
机译:评估了基于改良牛痘安卡拉(MVA)病毒载体的鼠疫疫苗的有效性和安全性。构建了在脑心肌炎病毒(EMCV)内部核糖体进入位点(IRES)的翻译控制下表达鼠疫耶尔森氏菌抗原的MVA重组体,和/或与组织纤溶酶原激活物(tPA)分泌信号融合。 MVA / Y。表达低钙应答V抗原(MVA / IRES / tPA / V-307)的截短版本的瘟疫重组蛋白,针对CO92(封装)或Java 9的鼻内或腹膜内攻击提供了显着保护(87.5-100%)。鼠疫耶尔森氏菌)。相反,MVA / Y。表达全长V抗原的瘟疫重组仅分别提供了针对抗CO92或Java 9菌株攻击的37.5%保护。有趣的是,MVA / Y。表达荚膜蛋白(F1)的瘟疫重组蛋白未引起明显的抗体效价,但仍分别赋予了针对CO92或Java 9攻击的50%和25%保护。 MVA / Y。瘟疫重组病毒在SCID小鼠中未显示任何死亡率或发病率。基于它们在小鼠中的安全性和有效性,这些MVA / Y。瘟疫重组体有望作为生物防御和公共卫生疫苗进一步开发

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