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Antibody recognition of the dengue virus proteome and implications for development of vaccines.

机译:登革病毒的抗体识别蛋白质组对疫苗的发展和影响。

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Dengue is a mosquito-borne infection caused by four distinct serotypes of dengue virus, each appearing cyclically in the tropics and subtropics along the equator. Although vaccines are currently under development, none are available to the general population. One of the main impediments to the successful advancement of these vaccines is the lack of well-defined immune correlates of protection. Here, we describe a protein microarray approach for measuring antibody responses to the complete viral proteome comprised of the structural (capsid, membrane, and envelope) and nonstructural (NS1, NS2A, NS2B, NS3, NS4A, NS4B, and NS5) components of all four dengue virus serotypes (1 to 4). We examined rhesus macaques vaccinated with tetravalent vaccines consisting of live-attenuated virus (LAV) or purified inactivated virus (PIV), followed by boosting with LAV and challenging with wild-type dengue virus. We detected temporal increases in antibodies against envelope proteins in response to either vaccine, while only the PIV/LAV vaccination strategy resulted in anticapsid antibodies. In contrast to results from vaccination, naive macaques challenged with wild-type viruses of each serotype demonstrated a balanced response to nonstructural and structural components, including responses against the membrane protein. Our results demonstrate discriminating details concerning the nature of antibody responses to dengue virus at the proteomic level and suggest the usefulness of this information for vaccine development.
机译:登革热是一种蚊媒传染病所致四个不同的登革病毒血清型,每个出现在热带和周期性沿着赤道亚热带。目前正在开发的,没有一个是什么可用于一般人群。成功发展的主要障碍这些疫苗是缺乏明确的免疫相关的保护。蛋白质微阵列方法测量完整的病毒蛋白质组抗体反应组成的结构(衣壳膜,和信封)和非结构化(NS1, NS2A NS2B,NS3、NS4A NS4B, NS5)组件的所有四个登革病毒血清型(1 - 4),我们检查了与四价的恒河猴接种疫苗疫苗组成的减毒活疫苗病毒(厕所)或纯化灭活病毒(PIV),其次是提高厕所和挑战性与野生型登革热病毒。增加膜蛋白抗体在应对疫苗,而只有PIV /洗手间疫苗接种策略导致anticapsid抗体。从接种疫苗,天真的猕猴与挑战野生型病毒的血清型了平衡的反应类型和结构对组件,包括响应膜蛋白质。识别细节有关的性质抗体反应的登革热病毒蛋白质组学水平和建议的有效性这些信息对于疫苗的发展。

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