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通过给予质粒细胞因子/免疫球蛋白增强和抑制对HIV-1 DNA疫苗的免疫反应。

Augmentation and suppression of immune responses to an HIV-1 DNA vaccine by plasmid cytokine/Ig administration.

作者信息

Barouch D H, Santra S, Steenbeke T D, Zheng X X, Perry H C, Davies M E, Freed D C, Craiu A, Strom T B, Shiver J W, Letvin N L

机构信息

Division of Viral Pathogenesis, Harvard Medical School, Beth Israel Deaconess Medical Center, Boston, MA 02215, USA.

出版信息

J Immunol. 1998 Aug 15;161(4):1875-82.

PMID:9712056
Abstract

The use of cytokines has shown promise as an approach for amplifying vaccine-elicited immune responses, but the application of these immunomodulatory molecules in this setting has not been systematically explored. In this report we investigate the use of protein- and plasmid-based cytokines to augment immune responses elicited by an HIV-1 gp120 plasmid DNA vaccine (pV1J-gp120) in mice. We demonstrate that immune responses elicited by pV1J-gp120 can be either augmented or suppressed by administration of plasmid cytokines. A dicistronic plasmid expressing both gp120 and IL-2 induced a surprisingly weaker gp120-specific immune response than did the monocistronic pV1J-gp120 plasmid. In contrast, systemic delivery of soluble IL-2/Ig fusion protein following pV1J-gp120 vaccination significantly amplified the gp120-specific immune response as measured by Ab, proliferative, and CTL levels. Administration of plasmid IL-2/Ig had different effects on the DNA vaccine-elicited immune response that depended on the temporal relationship between Ag and cytokine delivery. Injection of plasmid IL-2/Ig either before or coincident with pV1J-gp120 suppressed the gp120-specific immune response, whereas injection of plasmid IL-2/Ig after pV1J-gp120 amplified this immune response. To maximize immune responses elicited by a DNA vaccine, therefore, it appears that the immune system should first be primed with a specific Ag and then amplified with cytokines. The data also show that IL-2/Ig is more effective than native IL-2 as a DNA vaccine adjuvant.

摘要

细胞因子的使用已显示出有望作为一种增强疫苗引发的免疫反应的方法,但这些免疫调节分子在这种情况下的应用尚未得到系统研究。在本报告中,我们研究了基于蛋白质和质粒的细胞因子在增强HIV-1 gp120质粒DNA疫苗(pV1J-gp120)在小鼠中引发的免疫反应方面的用途。我们证明,通过给予质粒细胞因子,pV1J-gp120引发的免疫反应可以增强或受到抑制。一种同时表达gp120和IL-2的双顺反子质粒诱导的gp120特异性免疫反应比单顺反子pV1J-gp120质粒诱导的免疫反应出人意料地弱。相比之下,在pV1J-gp120疫苗接种后全身递送可溶性IL-2/Ig融合蛋白,通过抗体、增殖和CTL水平测量,显著增强了gp120特异性免疫反应。给予质粒IL-2/Ig对DNA疫苗引发的免疫反应有不同影响,这取决于抗原和细胞因子递送之间的时间关系。在pV1J-gp120之前或同时注射质粒IL-2/Ig会抑制gp120特异性免疫反应,而在pV1J-gp120之后注射质粒IL-2/Ig则会增强这种免疫反应。因此,为了使DNA疫苗引发的免疫反应最大化,似乎免疫系统应该首先用特定抗原进行启动,然后用细胞因子进行增强。数据还表明,作为DNA疫苗佐剂,IL-2/Ig比天然IL-2更有效。

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