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用人类免疫缺陷病毒gag DNA疫苗免疫的恒河猴中持续的肽特异性γ干扰素T细胞反应。

Sustained peptide-specific gamma interferon T-cell response in rhesus macaques immunized with human immunodeficiency virus gag DNA vaccines.

作者信息

Caulfield Michael J, Wang Su, Smith Jeffrey G, Tobery Timothy W, Liu Xu, Davies Mary-Ellen, Casimiro Danilo R, Fu Tong-Ming, Simon Adam, Evans Robert K, Emini Emilio A, Shiver John

机构信息

Department of Virus and Cell Biology, Merck Research Laboratories, West Point, Pennsylvania 19486, USA.

出版信息

J Virol. 2002 Oct;76(19):10038-43. doi: 10.1128/jvi.76.19.10038-10043.2002.

Abstract

We examined the influence of dose and method of antigen delivery on the dynamics and durability of T-cell responses to candidate human immunodeficiency virus (HIV) vaccines. Codon-optimized sequences from the HIV gag gene were inserted into alternative DNA vaccine vectors to express the coding sequence with or without the tissue plasminogen activator leader sequence. We delivered the vaccines by intramuscular injection as plasmid DNA without adjuvant or as plasmid DNA formulated with a novel block copolymer adjuvant (CRL8623) and then monitored the ensuing T-cell responses by using a gamma interferon enzyme-linked immunospot assay. We demonstrated persistence of the cell-mediated immune (CMI) response in rhesus macaques for at least 18 months following a four-dose vaccination regimen. The plasmid vaccine, with or without CRL8623, was immunogenic in macaques; however, the form coadministered with adjuvant exhibited improved T-cell responses, with a bias toward more antigen-specific CD8(+) T cells. Finally, we examined the fine specificity of the T-cell response to the gag vaccines by testing the response of 23 vaccinated macaques to individual Gag 20-mer peptides. Collectively, the monkeys responded to 25 epitopes, and, on average, each monkey recognized a minimum of 2.7 epitopes. The results indicate that a broad and durable CMI response to HIV DNA vaccines can be induced in a relevant nonhuman primate model.

摘要

我们研究了抗原递送剂量和方法对候选人类免疫缺陷病毒(HIV)疫苗T细胞应答动力学和持久性的影响。将HIV gag基因的密码子优化序列插入替代DNA疫苗载体,以表达带有或不带有组织纤溶酶原激活剂前导序列的编码序列。我们通过肌肉注射无佐剂的质粒DNA或与新型嵌段共聚物佐剂(CRL8623)配制的质粒DNA来递送疫苗,然后使用γ干扰素酶联免疫斑点试验监测随后的T细胞应答。我们证明,在恒河猴中进行四剂疫苗接种方案后,细胞介导免疫(CMI)应答持续至少18个月。含或不含CRL8623的质粒疫苗在猕猴中具有免疫原性;然而,与佐剂共同给药的形式表现出改善的T细胞应答,更倾向于产生更多抗原特异性CD8(+) T细胞。最后,我们通过测试23只接种疫苗的猕猴对单个Gag 20肽的应答,研究了T细胞对gag疫苗应答的精细特异性。总体而言,这些猴子对25个表位有应答,平均每只猴子至少识别2.7个表位。结果表明,在相关的非人类灵长类动物模型中可以诱导出对HIV DNA疫苗广泛而持久的CMI应答。

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