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肌内注射后能在小鼠体内引发乙肝表面抗原特异性细胞毒性T淋巴细胞和抗体反应的DNA载体构建体。

DNA vector constructs that prime hepatitis B surface antigen-specific cytotoxic T lymphocyte and antibody responses in mice after intramuscular injection.

作者信息

Böhm W, Kuhröber A, Paier T, Mertens T, Reimann J, Schirmbeck R

机构信息

Institute of Medical Microbiology, University of Ulm, Germany.

出版信息

J Immunol Methods. 1996 Jun 14;193(1):29-40. doi: 10.1016/0022-1759(96)00035-x.

DOI:10.1016/0022-1759(96)00035-x
PMID:8690928
Abstract

We tested the efficiency of induction of immune responses to the small hepatitis B surface antigen (HBsAg) in mice by intramuscular DNA immunization using different vector constructs that allow high levels of HBsAg expression in mouse cells. The HBsAg-specific responses of class I-restricted cytotoxic T lymphocytes (CTL) and of B cells (serum antibody titers) were measured. Following the intramuscular inoculation of 'naked' DNA, five different vector constructs of 4-8 kb, that contained or did not contain an intron and/or the neo gene, in which HBsAg expression was driven by promoter sequences derived from the immediate early region of HCMV, the SV40 enhancer/promoter region, or a retroviral 3' LTR efficiently primed responses of class I-restricted CD8+ CTL precursors. In contrast, the constructs in which HBsAg expression was driven by HCMV-derived promoter sequences stimulated significantly higher levels of HBsAg-specific serum antibody titers after intramuscular DNA injection than the SV40 or MPSV vector constructs. Large (15 kb) episomal vector constructs did not stimulate CTL or antibody responses. The data demonstrate that: (i) intramuscular DNA immunization represents an efficient technique for priming CTL and antibody responses to HBsAg; (ii) many vectors can be constructed that express an immunogenic product after intramuscular inoculation of 'naked' DNA; (iii) the efficiency of the tested vector constructs to prime after DNA immunization, either a CTL response, or an antibody response, differs.

摘要

我们使用不同的载体构建体通过肌肉内DNA免疫来测试小鼠对小乙肝表面抗原(HBsAg)免疫应答的诱导效率,这些构建体可使HBsAg在小鼠细胞中高水平表达。我们检测了I类限制性细胞毒性T淋巴细胞(CTL)和B细胞(血清抗体滴度)的HBsAg特异性应答。在肌肉内接种“裸”DNA后,五种4 - 8 kb的不同载体构建体,其中包含或不包含内含子和/或新霉素基因,HBsAg的表达由源自人巨细胞病毒(HCMV)立即早期区域的启动子序列、SV40增强子/启动子区域或逆转录病毒3' 长末端重复序列(LTR)驱动,有效地引发了I类限制性CD8 + CTL前体的应答。相比之下,在肌肉内注射DNA后,由HCMV衍生的启动子序列驱动HBsAg表达的构建体刺激产生的HBsAg特异性血清抗体滴度水平明显高于SV40或莫洛尼鼠肉瘤病毒(MPSV)载体构建体。大型(15 kb)附加型载体构建体未刺激CTL或抗体应答。数据表明:(i)肌肉内DNA免疫是引发对HBsAg的CTL和抗体应答的有效技术;(ii)可以构建许多在肌肉内接种“裸”DNA后表达免疫原性产物的载体;(iii)经测试的载体构建体在DNA免疫后引发CTL应答或抗体应答的效率有所不同。

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DNA vector constructs that prime hepatitis B surface antigen-specific cytotoxic T lymphocyte and antibody responses in mice after intramuscular injection.肌内注射后能在小鼠体内引发乙肝表面抗原特异性细胞毒性T淋巴细胞和抗体反应的DNA载体构建体。
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J Mol Med (Berl). 2004 Feb;82(2):144-52. doi: 10.1007/s00109-003-0502-3. Epub 2003 Dec 2.
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Codelivery of a DNA vaccine and a protein vaccine with aluminum phosphate stimulates a potent and multivalent immune response.
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