表达携带人类和猿猴免疫缺陷病毒表位的乙肝核心颗粒的杂交DNA疫苗在小鼠和恒河猴中的免疫原性
Immunogenicity of hybrid DNA vaccines expressing hepatitis B core particles carrying human and simian immunodeficiency virus epitopes in mice and rhesus macaques.
作者信息
Fuller Deborah Heydenburg, Shipley Tim, Allen Todd M, Fuller James T, Wu Mary S, Horton Helen, Wilson Nancy, Widera Georg, Watkins David I
机构信息
PowderJect Vaccines Inc, Madison, WI 53562, USA.
出版信息
Virology. 2007 Aug 1;364(2):245-55. doi: 10.1016/j.virol.2007.02.024. Epub 2007 Apr 11.
Abstract
An effective HIV vaccine will likely need to induce broad and potent CTL responses. Epitope-based vaccines offer significant potential for inducing multi-specific CTL, but often require conjugation to T helper epitopes or carrier moieties to induce significant responses. We tested hybrid DNA vaccines encoding one or more HIV or SIV CTL epitopes fused to a hepatitis B core antigen (HBcAg) carrier gene as a means to improve the immunogenicity of epitope-based DNA vaccines. Immunization of mice with a HBcAg-HIV epitope DNA vaccine induced CD8(+) T cell responses that significantly exceeded levels induced with DNA encoding either the whole HIV antigen or the epitope alone. In rhesus macaques, a multi-epitope hybrid HBcAg-SIV DNA vaccine induced CTL responses to 13 different epitopes, including 3 epitopes that were previously not detected in SIV-infected macaques. These data demonstrate that immunization with hybrid HBcAg-epitope DNA vaccines is an effective strategy to increase the magnitude and breadth of HIV-specific CTL responses.
摘要
一种有效的HIV疫苗可能需要诱导广泛且强效的CTL反应。基于表位的疫苗在诱导多特异性CTL方面具有巨大潜力,但通常需要与T辅助表位或载体部分偶联才能诱导显著反应。我们测试了编码一个或多个与乙肝核心抗原(HBcAg)载体基因融合的HIV或SIV CTL表位的杂交DNA疫苗,以此作为提高基于表位的DNA疫苗免疫原性的一种手段。用HBcAg-HIV表位DNA疫苗免疫小鼠可诱导CD8(+) T细胞反应,该反应显著超过单独编码完整HIV抗原或表位的DNA所诱导的水平。在恒河猴中,一种多表位杂交HBcAg-SIV DNA疫苗诱导了针对13种不同表位的CTL反应,其中包括3种先前在感染SIV的猕猴中未检测到的表位。这些数据表明,用杂交HBcAg-表位DNA疫苗免疫是一种增加HIV特异性CTL反应强度和广度的有效策略。
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