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首页> 美国卫生研究院文献>other >Comparison of homologous and heterologous prime-boost vaccine approaches using Modified Vaccinia Ankara and soluble protein to induce neutralizing antibodies by the human cytomegalovirus pentamer complex in mice
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Comparison of homologous and heterologous prime-boost vaccine approaches using Modified Vaccinia Ankara and soluble protein to induce neutralizing antibodies by the human cytomegalovirus pentamer complex in mice

机译:使用改良的痘苗安卡拉和可溶蛋白通过人巨细胞病毒五聚体复合物诱导小鼠中和抗体的同源和异源初免-加强疫苗方法的比较

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Since neutralizing antibodies (NAb) targeting the human cytomegalovirus (HCMV) pentamer complex (PC) potently block HCMV host cell entry, anti-PC NAb induction is thought to be important for a vaccine formulation to prevent HCMV infection. By developing a vaccine strategy based on soluble PC protein and using a previously generated Modified Vaccinia Ankara vector co-expressing all five PC subunits (MVA-PC), we compared HCMV NAb induction by homologous immunization using prime-boost vaccine regimen employing only PC protein or MVA-PC and heterologous immunization using prime-boost combinations of PC protein and MVA-PC. Utilizing a recently isolated anti-PC NAb, we produced highly pure soluble PC protein that displayed conformational and linear neutralizing epitopes, interfered with HCMV entry, and was recognized by antibodies induced by HCMV during natural infection. Mice vaccinated by different immunization routes with the purified PC protein in combination with a clinically approved adjuvant formulation elicited high-titer and durable HCMV NAb. While MVA-PC and soluble PC protein either alone or in combination elicited robust HCMV NAb, significantly different potencies of these vaccine approaches were observed in dependence on immunization schedule. Using only two immunizations, vaccination with MVA-PC alone or prime-boost combinations of MVA-PC and PC protein was significantly more effective in stimulating HCMV NAb than immunization with PC protein alone. In contrast, with three immunizations, NAb induced by soluble PC protein either alone or combined with two boosts of MVA-PC increased to levels that exceeded NAb titer stimulated by MVA-PC alone. These results provide insights into the potency of soluble protein and MVA to elicit NAb by the HCMV PC via homologous and heterologous prime-boost immunization, which may contribute to develop clinically deployable vaccine strategies to prevent HCMV infection.
机译:由于靶向人巨细胞病毒(HCMV)五聚体复合物(PC)的中和抗体(NAb)有力地阻断了HCMV宿主细胞的进入,因此抗PC NAb的诱导被认为对于预防HCMV感染的疫苗制剂非常重要。通过开发基于可溶性PC蛋白的疫苗策略并使用先前表达的同时表达所有五个PC亚基的修饰牛痘安卡拉载体(MVA-PC),我们比较了仅使用PC蛋白的初免-加强疫苗接种方案通过同源免疫进行的HCMV NAb诱导MVA-PC或MVA-PC以及使用PC蛋白和MVA-PC的初免-升压组合进行异源免疫。利用最近分离的抗PC NAb,我们产生了高纯度的可溶性PC蛋白,该蛋白显示构象和线性中和表位,干扰HCMV进入,并在自然感染过程中被HCMV诱导的抗体识别。通过不同的免疫途径用纯化的PC蛋白与临床认可的佐剂制剂进行免疫的小鼠可产生高滴度和持久性的HCMV NAb。虽然单独或组合使用MVA-PC和可溶性PC蛋白可产生健壮的HCMV NAb,但根据免疫方案的不同,观察到这些疫苗方法的效价显着不同。仅使用两次免疫,单独用MVA-PC进行疫苗接种或MVA-PC和PC蛋白的初免-加强免疫组合刺激HCMV NAb的效果要比单独用PC蛋白进行免疫有效。相反,通过三种免疫,单独或与两次MVA-PC增强结合的可溶性PC蛋白诱导的NAb增加到超过单独MVA-PC刺激的NAb效价的水平。这些结果提供了对可溶性蛋白和MVA通过HCMV PC通过同源和异源初免-加强免疫引发NAb的潜能的见解,这可能有助于开发可临床部署的疫苗策略来预防HCMV感染。

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