Giannecchini Simone, Isola Patrizia, Sichi Olimpia, Matteucci Donatella, Pistello Mauro, Zaccaro Lucia, Del Mauro Daniela, Bendinelli Mauro
Retrovirus Center and Virology Section, Department of Biomedicine, University of Pisa, Pisa, Italy.
J Virol. 2002 Jul;76(14):6882-92. doi: 10.1128/jvi.76.14.6882-6892.2002.
Immunogenicity and protective activity of four cell-based feline immunodeficiency virus (FIV) vaccines prepared with autologous lymphoblasts were investigated. One vaccine was composed of FIV-infected cells that were paraformaldehyde fixed at the peak of viral expression. The other vaccines were attempts to maximize the expression of protective epitopes that might become exposed as a result of virion binding to cells and essentially consisted of cells mildly fixed after saturation of their surface with adsorbed, internally inactivated FIV particles. The levels of FIV-specific lymphoproliferation exhibited by the vaccinees were comparable to the ones previously observed in vaccine-protected cats, but antibodies were largely directed to cell-derived constituents rather than to truly viral epitopes and had very poor FIV-neutralizing activity. Moreover, under one condition of testing, some vaccine sera enhanced FIV replication in vitro. As a further limit, the vaccines proved inefficient at priming animals for anamnestic immune responses. Two months after completion of primary immunization, the animals were challenged with a low dose of homologous ex vivo FIV. Collectively, 8 of 20 vaccinees developed infection versus one of nine animals mock immunized with fixed uninfected autologous lymphoblasts. After a boosting and rechallenge with a higher virus dose, all remaining animals became infected, thus confirming their lack of protection.
研究了用自体淋巴母细胞制备的四种基于细胞的猫免疫缺陷病毒(FIV)疫苗的免疫原性和保护活性。一种疫苗由在病毒表达高峰期用多聚甲醛固定的FIV感染细胞组成。其他疫苗试图使可能因病毒体与细胞结合而暴露的保护性表位的表达最大化,基本上由在用吸附的、内部灭活的FIV颗粒使其表面饱和后轻度固定的细胞组成。接种疫苗者表现出的FIV特异性淋巴细胞增殖水平与先前在疫苗保护的猫中观察到的水平相当,但抗体主要针对细胞衍生成分而非真正的病毒表位,并且FIV中和活性非常低。此外,在一种测试条件下,一些疫苗血清在体外增强了FIV复制。作为进一步的限制,疫苗在引发动物的回忆性免疫反应方面被证明效率低下。初次免疫完成两个月后,用低剂量的同源体外FIV对动物进行攻击。总体而言,20只接种疫苗者中有8只发生感染,而用固定的未感染自体淋巴母细胞进行模拟免疫的9只动物中有1只发生感染。在进行加强免疫并用更高病毒剂量再次攻击后,所有剩余动物均被感染,从而证实它们缺乏保护作用。