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与疫苗抗原基因融合的异源五聚体霍乱毒素B亚基嵌合分子可诱导全身和黏膜免疫反应:一种将重组疫苗抗原靶向黏膜免疫系统的潜在新策略。

Heteropentameric cholera toxin B subunit chimeric molecules genetically fused to a vaccine antigen induce systemic and mucosal immune responses: a potential new strategy to target recombinant vaccine antigens to mucosal immune systems.

作者信息

Harakuni Tetsuya, Sugawa Hideki, Komesu Ai, Tadano Masayuki, Arakawa Takeshi

机构信息

Division of Molecular Microbiology, Center of Molecular Biosciences, University of the Ryukyus, Nishihara, Okinawa 903-0213, Japan.

出版信息

Infect Immun. 2005 Sep;73(9):5654-65. doi: 10.1128/IAI.73.9.5654-5665.2005.

DOI:10.1128/IAI.73.9.5654-5665.2005
PMID:16113283
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1231140/
Abstract

Noninvasive mucosal vaccines are attractive alternatives to parenteral vaccines. Although the conjugation of vaccine antigens with the B subunit of cholera toxin (CTB) is one of the most promising strategies for vaccine delivery to mucosal immune systems, the molecule cannot tolerate large-protein fusion, as it severely impairs pentamerization and loses affinity for GM1-ganglioside. Here we report a new strategy, in which steric hindrance between CTB-antigen fusion subunits is significantly reduced through the integration of unfused CTB "molecular buffers" into the pentamer unit, making them more efficiently self-assemble into biologically active pentamers. In addition, the chimeric protein took a compact configuration, becoming small enough to be secreted, and one-step affinity-purified proteins, when administered through a mucosal route, induced specific immune responses in mice. Since our results are not dependent on the use of a particular expression system or vaccine antigen, this strategy could be broadly applicable to bacterial enterotoxin-based vaccine design.

摘要

非侵入性黏膜疫苗是注射用疫苗颇具吸引力的替代方案。尽管将疫苗抗原与霍乱毒素(CTB)的B亚基偶联是将疫苗递送至黏膜免疫系统最具前景的策略之一,但该分子无法耐受大蛋白融合,因为这会严重损害其五聚化并丧失对GM1神经节苷脂的亲和力。在此,我们报告一种新策略,通过将未融合的CTB“分子缓冲器”整合到五聚体单元中,显著降低CTB-抗原融合亚基之间的空间位阻,使其更有效地自组装成具有生物活性的五聚体。此外,嵌合蛋白呈紧密构象,小到足以分泌,且经黏膜途径给药时,一步亲和纯化的蛋白能在小鼠体内诱导特异性免疫反应。由于我们的结果不依赖于特定表达系统或疫苗抗原的使用,该策略可广泛应用于基于细菌肠毒素的疫苗设计。

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本文引用的文献

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Expression and characterization of cholera toxin B-pneumococcal surface adhesin A fusion protein in Escherichia coli: ability of CTB-PsaA to induce humoral immune response in mice.霍乱毒素B-肺炎球菌表面黏附素A融合蛋白在大肠杆菌中的表达与鉴定:CTB-PsaA诱导小鼠体液免疫应答的能力
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Induction of a mucosal immune response to the streptococcal M protein by intramuscular administration of a PADRE-ASREAK peptide.通过肌肉注射PADRE-ASREAK肽诱导对链球菌M蛋白的黏膜免疫反应。
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Coupling of antigen to cholera toxin for dendritic cell vaccination promotes the induction of MHC class I-restricted cytotoxic T cells and the rejection of a cognate antigen-expressing model tumor.将抗原与霍乱毒素偶联用于树突状细胞疫苗接种可促进MHC I类限制性细胞毒性T细胞的诱导以及对表达同源抗原的模型肿瘤的排斥。
Eur J Immunol. 2004 May;34(5):1272-81. doi: 10.1002/eji.200324368.
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High-level expression of codon optimized foot-and-mouth disease virus complex epitopes and cholera toxin B subunit chimera in Hansenula polymorpha.密码子优化的口蹄疫病毒复合表位与霍乱毒素B亚基嵌合体在多形汉逊酵母中的高水平表达
Biochem Biophys Res Commun. 2004 Feb 27;315(1):235-9. doi: 10.1016/j.bbrc.2004.01.037.
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Structural basis of a flavivirus recognized by its neutralizing antibody: solution structure of the domain III of the Japanese encephalitis virus envelope protein.
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