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多价合成疫苗:T细胞表位与免疫原性之间的关系

Polyvalent synthetic vaccines: relationship between T epitopes and immunogenicity.

作者信息

Jolivet M, Lise L, Gras-Masse H, Tartar A, Audibert F, Chedid L

机构信息

Department of Immunology and Microbiology, University of South Florida College of Medicine, Tampa 33612-4799.

出版信息

Vaccine. 1990 Feb;8(1):35-40. doi: 10.1016/0264-410x(90)90175-l.

DOI:10.1016/0264-410x(90)90175-l
PMID:1690488
Abstract

Three different synthetic polyvalent vaccines have been constructed by conjugating four synthetic peptides without any carrier protein. The peptides were copy fragments of two bacterial antigens (Streptococcus pyogenes M protein and diphtheria toxin), two parasitic antigens (circumsporozoite protein of Plasmodium falciparum and Plasmodium knowlesi), and one viral antigen (hepatitis B surface antigen). Outbred guinea-pigs immunized with polyvalent vaccine containing streptococcal, diphtheric, P. knowlesi and hepatitis peptides raised high specific antibody response against the four specificities. Individual T cell analysis demonstrated that hepatitis peptide bears T dominant epitope. A similar immune response was obtained with a second polyvalent vaccine where the P. knowlesi peptide had been replaced by the P. falciparum peptide. In both experiments the malarial peptides behave like pure B epitopes. Prediction of immunodominant helper T-cell antigenic sites were performed with the five peptides using computer algorithm. Hepatitis and diphtheric peptides were selected whereas the streptococcal peptide was rejected although it can experimentally contain a T epitope. To confirm this result animals were immunized with a third polyvalent vaccine which does not contain the hepatitis peptide. No T cell proliferation or antipeptide antibodies were detected. These results demonstrate that the cooperative immune response requires a certain degree of antigenic complexity for the induction of antibody response.

摘要

通过将四种合成肽与任何载体蛋白偶联,构建了三种不同的合成多价疫苗。这些肽是两种细菌抗原(化脓性链球菌M蛋白和白喉毒素)、两种寄生虫抗原(恶性疟原虫和诺氏疟原虫的环子孢子蛋白)以及一种病毒抗原(乙型肝炎表面抗原)的复制片段。用含有链球菌、白喉、诺氏疟原虫和肝炎肽的多价疫苗免疫远交系豚鼠,可引发针对这四种特异性的高特异性抗体反应。单个T细胞分析表明,肝炎肽带有T优势表位。用第二种多价疫苗也获得了类似的免疫反应,其中诺氏疟原虫肽被恶性疟原虫肽取代。在两个实验中,疟疾肽的行为都类似于纯B表位。使用计算机算法对这五种肽进行了免疫显性辅助性T细胞抗原位点的预测。选择了肝炎肽和白喉肽,而链球菌肽虽然在实验中可能含有T表位,但被排除。为了证实这一结果,用第三种不含肝炎肽的多价疫苗免疫动物。未检测到T细胞增殖或抗肽抗体。这些结果表明,协同免疫反应需要一定程度的抗原复杂性来诱导抗体反应。

相似文献

1
Polyvalent synthetic vaccines: relationship between T epitopes and immunogenicity.多价合成疫苗:T细胞表位与免疫原性之间的关系
Vaccine. 1990 Feb;8(1):35-40. doi: 10.1016/0264-410x(90)90175-l.
2
Vaccine engineering: enhancement of immunogenicity of synthetic peptide vaccines related to hepatitis in chemically defined models consisting of T- and B-cell epitopes.疫苗工程:在由T细胞和B细胞表位组成的化学限定模型中增强与肝炎相关的合成肽疫苗的免疫原性。
Proc Natl Acad Sci U S A. 1989 Dec;86(23):9084-8. doi: 10.1073/pnas.86.23.9084.
3
Peptide vaccines incorporating a 'promiscuous' T-cell epitope bypass certain haplotype restricted immune responses and provide broad spectrum immunogenicity.包含“混杂”T细胞表位的肽疫苗可绕过某些单倍型受限的免疫反应,并提供广谱免疫原性。
J Mol Recognit. 1993 Jun;6(2):81-94. doi: 10.1002/jmr.300060206.
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Induction of biologically active antibodies by a polyvalent synthetic vaccine constructed without carrier.由无载体构建的多价合成疫苗诱导产生生物活性抗体。
Infect Immun. 1987 Jun;55(6):1498-502. doi: 10.1128/iai.55.6.1498-1502.1987.
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Hepatitis B virus core and e antigen: immune recognition and use as a vaccine carrier moiety.乙肝病毒核心抗原与e抗原:免疫识别及作为疫苗载体部分的应用
Intervirology. 1996;39(1-2):104-10. doi: 10.1159/000150481.
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Immunogenicity and vaccine efficacy of synthetic peptides containing Semliki Forest virus B and T cell epitopes.含有塞姆利基森林病毒B和T细胞表位的合成肽的免疫原性及疫苗效力
J Gen Virol. 1992 Sep;73 ( Pt 9):2267-72. doi: 10.1099/0022-1317-73-9-2267.
7
A universal T cell epitope-containing peptide from hepatitis B surface antigen can enhance antibody specific for HIV gp120.一种来自乙肝表面抗原的含通用T细胞表位的肽可增强针对HIV gp120的特异性抗体。
J Immunol. 1992 Jun 15;148(12):3970-7.
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Specificity of antibodies reactive with hepatitis B surface antigen following immunization with synthetic peptides.用合成肽免疫后与乙型肝炎表面抗原反应的抗体的特异性
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Co-dominant and reciprocal T-helper cell activity of epitopic sequences and formation of junctional B-cell determinants in synthetic T:B chimeric immunogens.
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Immunogenicity of multiple antigen peptides (MAP) containing T and B cell epitopes of the repeat region of the P. falciparum circumsporozoite protein.包含恶性疟原虫环子孢子蛋白重复区域T细胞和B细胞表位的多抗原肽(MAP)的免疫原性。
Eur J Immunol. 1991 Dec;21(12):3015-20. doi: 10.1002/eji.1830211217.