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The successful induction of T-cell and antibody responses by a recombinant measles virus-vectored tetravalent dengue vaccine provides partial protection against dengue-2 infection

机译:重组麻疹病毒载体的四价登革热疫苗成功诱导T细胞和抗体反应为登革2型感染提供了部分保护

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摘要

[[abstract]]Dengue has a major impact on global public health, and the use of dengue vaccine is very limited. In this study, we evaluated the immunogenicity and protective efficacy of a dengue vaccine made from a recombinant measles virus (MV) that expresses envelope protein domain III (ED3) of dengue-1 to 4. Following immunization with the MV-vectored dengue vaccine, mice developed specific interferon-gamma and antibody responses against dengue virus and MV. Neutralizing antibodies against MV and dengue viruses were also induced, and protective levels of FRNT50 >/= 10 to four serotypes of dengue viruses were detected in the MV-vectored dengue vaccine-immunized mice. In addition, specific interferon-gamma and antibody responses to dengue viruses were still induced by the MV-vectored dengue vaccine in mice that were pre-infected with MV. This finding suggests that the pre-existing immunity to MV did not block the initiation of immune responses. By contrast, mice that were pre-infected with dengue-3 exhibited no effect in terms of their antibody responses to MV and dengue viruses, but a dominant dengue-3-specific T-cell response was observed. After injection with dengue-2, a detectable but significantly lower viremia and a higher titer of anti-dengue-2 neutralizing antibodies were observed in MV-vectored dengue vaccine-immunized mice versus the vector control, suggesting that an anamnestic antibody response that provided partial protection against dengue-2 was elicited. Our results with regard to T-cell responses and the effect of pre-immunity to MV or dengue viruses provide clues for the future applications of an MV-vectored dengue vaccine.
机译:[[摘要]]登革热对全球公共卫生有重大影响,登革热疫苗的使用非常有限。在这项研究中,我们评估了由重组麻疹病毒(MV)制造的登革热疫苗的免疫原性和保护功效,该病毒表达登革热1至4的包膜蛋白结构域III(ED3)。用MV载体登革热疫苗免疫后,小鼠发展出针对登革热病毒和MV的特异性干扰素-γ和抗体反应。还诱导了针对MV和登革热病毒的中和抗体,并且在MV载体登革热疫苗免疫的小鼠中检测到FRNT50≥/ = 10至四种血清型的登革热病毒的保护水平。此外,在预先感染了MV的小鼠中,MV载体登革热疫苗仍诱导了对登革热病毒的特异性干扰素-γ和抗体反应。这一发现表明,预先存在的对MV的免疫力不会阻止免疫应答的启动。相比之下,预感染登革3的小鼠对MV和登革病毒的抗体反应没有表现出任何作用,但是观察到主要的登革3特异性T细胞反应。注射登革2疫苗后,与载体对照相比,在MV载体登革热疫苗免疫小鼠中观察到可检测到但明显更低的病毒血症和更高滴度的抗登革2中和抗体,表明记忆消除抗体反应提供了部分引发了针对登革热2的保护。我们在T细胞反应以及针对MV或登革热病毒的免疫前效果方面的研究结果为MV载体登革热疫苗的未来应用提供了线索。

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    Hu, HM;

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  • 年度 2016
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