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用表达人绒毛膜促性腺激素β嵌合体的质粒进行DNA免疫。

DNA immunization with plasmids expressing hCGbeta-chimeras.

作者信息

Terrazzini Nadia, Hannesdóttir Sólveig, Delves Peter J, Lund Torben

机构信息

Department of Immunology and Molecular Pathology, University College London, 46 Cleveland Street, London W1T 4JF, UK.

出版信息

Vaccine. 2004 Jun 2;22(17-18):2146-53. doi: 10.1016/j.vaccine.2003.12.002.

Abstract

Human chorionic gonadotropin has been used as an anti-fertility vaccine and as a target for cancer immunotherapy. We have explored the use of DNA immunization with the aim of improving the immunogenicity of this hormone. Stimulating the muscle with electric pulses following intramuscular injection of plasmids expressing hCGbeta resulted in higher levels of human chorionic gonadotropin (hCG)-specific antibodies, which could be further enhanced following a protein boost with hCG mixed with adjuvant. DNA vaccines encoding a membrane attached or a secreted form of hCGbeta produced similar-albeit relatively modest-antibody responses. Providing hCGbeta with additional T cell help by vaccinating with a plasmid encoding a hCGbeta-hFc fusion protein did not further increase the antibody levels in the immunized animals. However, immunization of mice with a construct encoding hCGbeta fused to C3d(3) produced significantly lower antibody levels relative to mice immunized with the hCGbeta-alone expression plasmid, even though the hCGbeta-C3d(3) chimera was expected to facilitate cross-linking of the antigen-specific B-cell receptor and CR2 thereby lowering the threshold of activation. Thus the limiting factor determining the antibody levels following hCGbeta immunization, at least for DNA immunization, is related to the amount of protein available rather than the form of protein produced or lack of T cell epitopes.

摘要

人绒毛膜促性腺激素已被用作抗生育疫苗和癌症免疫治疗的靶点。我们探索了DNA免疫的用途,目的是提高这种激素的免疫原性。在肌肉注射表达hCGβ的质粒后用电脉冲刺激肌肉,可产生更高水平的人绒毛膜促性腺激素(hCG)特异性抗体,在用hCG与佐剂混合进行蛋白加强免疫后,抗体水平可进一步提高。编码膜附着形式或分泌形式hCGβ的DNA疫苗产生了相似的——尽管相对适度的——抗体反应。通过用编码hCGβ-hFc融合蛋白的质粒进行疫苗接种为hCGβ提供额外的T细胞辅助,并没有进一步提高免疫动物体内的抗体水平。然而,用编码与C3d(3)融合的hCGβ的构建体免疫小鼠,相对于用单独的hCGβ表达质粒免疫的小鼠,产生的抗体水平显著降低,尽管hCGβ-C3d(3)嵌合体预计会促进抗原特异性B细胞受体和CR2的交联,从而降低激活阈值。因此,决定hCGβ免疫后抗体水平的限制因素,至少对于DNA免疫来说,与可用蛋白的量有关,而不是与产生的蛋白形式或缺乏T细胞表位有关。

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