Pal Ranajit, Wang Shixia, Kalyanaraman V S, Nair B C, Whitney Stephen, Keen Timothy, Hocker Lindsey, Hudacik Lauren, Rose Nicolas, Cristillo Anthony, Mboudjeka Innocent, Shen Siyuan, Wu-Chou Te-Hui, Montefiori David, Mascola John, Lu Shan, Markham Phillip
Advanced BioScience Laboratories, Kensington, MD 20895, USA.
J Med Primatol. 2005 Oct;34(5-6):226-36. doi: 10.1111/j.1600-0684.2005.00120.x.
Immunization of macaques with multivalent DNA encoding gp120 genes from HIV-1 subtypes A, B, C and E and a gag gene followed by boosting with homologous gp120 proteins elicited strong anti-gp120 antibodies capable of neutralizing homologous and to a lesser degree heterologous HIV-1 isolates. Both Env- and Gag-specific cell mediated immune (CMI) responses were detected in the immunized animals. Following rectal challenge with an SHIV isolate encoding HIV-1(Ba-L)env, plasma viremia in the infected immunized animals was significantly lower than that observed in the naïve animals. Further, one of six immunized animals was completely protected whereas all six naïve animals were infected. These results demonstrate that a vaccine based on priming with a polyvalent DNA vaccine from multiple HIV-1 subtypes followed by boosting with homologous Env proteins elicits anti-HIV-1 immune responses capable of controlling rectal transmission of SHIV(Ba-L).
用编码来自HIV-1 A、B、C和E亚型的gp120基因及一个gag基因的多价DNA免疫猕猴,随后用同源gp120蛋白加强免疫,可引发强大的抗gp120抗体,这些抗体能够中和同源HIV-1分离株,并在较小程度上中和异源HIV-1分离株。在免疫动物中检测到了Env特异性和Gag特异性细胞介导免疫(CMI)反应。在用编码HIV-1(Ba-L)env的SHIV分离株进行直肠攻击后,感染的免疫动物的血浆病毒血症显著低于未免疫动物。此外,六只免疫动物中有一只得到了完全保护,而所有六只未免疫动物均被感染。这些结果表明,基于用来自多种HIV-1亚型的多价DNA疫苗进行初免,随后用同源Env蛋白进行加强免疫的疫苗,可引发能够控制SHIV(Ba-L)直肠传播的抗HIV-1免疫反应。
