首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Inactivated whole-virus vaccine derived from a proviral DNA clone of simian immunodeficiency virus induces high levels of neutralizing antibodies and confers protection against heterologous challenge.
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Inactivated whole-virus vaccine derived from a proviral DNA clone of simian immunodeficiency virus induces high levels of neutralizing antibodies and confers protection against heterologous challenge.

机译:源自猿猴免疫缺陷病毒前病毒DNA克隆的灭活全病毒疫苗可诱导高水平的中和抗体,并提供针对异源攻击的保护。

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摘要

We tested the ability of macaques vaccinated with inactivated whole simian immunodeficiency virus (SIV) to resist challenge with either homologous or heterologous cell-free uncloned SIV administered by the intravenous route. The vaccine virus was derived from a proviral DNA clone and thus was considered genetically homogeneous. Sixteen macaques received either hepatitis B surface antigen (n = 6) or the inactivated whole-SIV vaccine (n = 10) at weeks 0, 4, and 49 of the study. All SIV vaccine recipients developed high levels of homologous and heterologous neutralizing antibodies in response to vaccination. At the time of challenge (week 53), vaccinees were further stratified to receive either homologous (n = 10) or heterologous (n = 6) uncloned live SIV. The envelope glycoproteins of the homologous and heterologous challenge viruses were 94% and 81% identical to the vaccine virus, respectively. Regardless of challenge inoculum, all vaccinees in the control group (hepatitis B surface antigen) became infected, whereas all SIV vaccinees were protected against detectable infection. These data support the concept that an efficacious vaccine for HIV might be possible, and suggest that genetic variation of HIV might not be an insurmountable obstacle for vaccine development.
机译:我们测试了灭活的全猿猴免疫缺陷病毒(SIV)接种的猕猴抵抗通过静脉内途径施用的同源或异源无细胞非克隆SIV攻击的能力。疫苗病毒源自前病毒DNA克隆,因此被认为具有遗传同源性。在研究的第0、4和49周,有16只猕猴接受了乙型肝炎表面抗原(n = 6)或灭活的全SIV疫苗(n = 10)。所有SIV疫苗接种者在接种疫苗后都会产生高水平的同源和异源中和抗体。攻击时(第53周),将疫苗进一步分层,以接受同源(n = 10)或异源(n = 6)的非克隆活SIV。同源和异源攻击病毒的包膜糖蛋白分别与疫苗病毒相同,分别为94%和81%。无论挑战接种物如何,对照组中的所有疫苗(乙型肝炎表面抗原)均被感染,而所有SIV疫苗均受到保护以防止可检测到的感染。这些数据支持可能有效的针对HIV的疫苗的概念,并表明HIV的遗传变异可能不是疫苗开发不可克服的障碍。

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