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细胞因子基因佐剂促进小鼠抗急性和潜伏性单纯疱疹病毒感染的预防性血管内DNA疫苗。

Cytokine genetic adjuvant facilitates prophylactic intravascular DNA vaccine against acute and latent herpes simplex virus infection in mice.

作者信息

Cui F-D, Asada H, Jin M-L, Kishida T, Shin-Ya M, Nakaya T, Kita M, Ishii M, Iwai M, Okanoue T, Imanishi J, Mazda O

机构信息

Department of Microbiology, Kyoto Prefectural University of Medicine, Kyoto, Japan.

出版信息

Gene Ther. 2005 Jan;12(2):160-8. doi: 10.1038/sj.gt.3302393.

Abstract

Intravascular plasmid DNA (pDNA) vaccine encoding herpes simplex virus type 1 (HSV-1) glycoprotein B (gB) effectively induces prophylactic immunity against lethal HSV-1 infection in mice. We investigated whether the vaccine potency is further improved by coadministration of cytokine genes together with a low dose of genetic vaccine. pDNA encoding IL-12, IL-15, IL-18 or IL-21 was capable of elevating survival rates of HSV-1-infected mice when coinjected with 1 microg of gB pDNA, while IL-10 gene delivery failed to affect the effectiveness of the genetic immunization. Although only 17% of mice survived acute HSV infection after the gB pDNA vaccination at a dose of 1 microg, all mice coadministered with 1 microg each of gB and IL-12 pDNAs not only survived the acute infection but also escaped latent infection. In these animals, the neutralizing antibody against HSV-1 was abundantly produced, and CTL activity against the gB antigen was augmented. Coadministration of the gB and IL-12 genes also elevated the serum level of interferon-gamma. Adaptive transfer experiments indicated that soluble factors contributed to preventive immunity, while cell components alone were not capable of protecting mice from fatal viral infection. These results strongly suggest potential usefulness of Th1 cytokine genes as effective molecular adjuvants that facilitate specific humoral as well as cellular immune responses elicited by intravascular molecular vaccination.

摘要

编码单纯疱疹病毒1型(HSV-1)糖蛋白B(gB)的血管内质粒DNA(pDNA)疫苗可有效诱导小鼠对致死性HSV-1感染产生预防性免疫。我们研究了细胞因子基因与低剂量基因疫苗共同给药是否能进一步提高疫苗效力。当与1微克gB pDNA共同注射时,编码IL-12、IL-15、IL-18或IL-21的pDNA能够提高HSV-1感染小鼠的存活率,而IL-10基因递送未能影响基因免疫的效果。虽然在接种1微克剂量的gB pDNA疫苗后,只有17%的小鼠在急性HSV感染后存活,但所有同时接种1微克gB和IL-12 pDNA的小鼠不仅在急性感染中存活,而且还避免了潜伏感染。在这些动物中,大量产生了针对HSV-1的中和抗体,并且针对gB抗原的CTL活性增强。gB和IL-12基因的共同给药还提高了血清干扰素-γ水平。适应性转移实验表明,可溶性因子有助于预防性免疫,而单独的细胞成分不能保护小鼠免受致命的病毒感染。这些结果强烈表明Th1细胞因子基因作为有效的分子佐剂具有潜在用途,可促进血管内分子疫苗引发的特异性体液免疫和细胞免疫反应。

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