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Proliferating and helper T lymphocytes display distinct fine specificities in response to human fibrinopeptide B.

作者信息

Peterson L B, Wilner G D, Thomas D W

出版信息

J Immunol. 1983 Jun;130(6):2542-5.

PMID:6189893
Abstract

The fine specificity of T cell responses involved in the generation of help for antibody production and proliferation was examined by using the 14 amino acid peptide human fibrinopeptide B (hFPB, B beta 1-14) and its synthetic peptide homologues B beta 1-14(Lys14), B beta 1-13, and B beta 3-14. Peritoneal exudate or lymph node T cells from C57BL/10 and B10.BR mice immunized with hFPB or its synthetic homologues were used to measure in vitro proliferative responses. T cells from hFPB-immunized B10.BR mice showed specific proliferation to hFPB, but were unresponsive to B beta 1-14(Lys14), B beta 1-13, and B beta 3-14. B10.BR mice immunized with B beta 1-14(Lys14), B beta 1-13, or B beta 3-14 were unresponsive to all peptides tested. T cells from C57BL/10 mice showed no specific proliferation after immunization and challenge with any of the peptide antigens. In contrast to the patterns of T cell proliferation, immunization of both B10.BR and C57BL/10 mice with hFPB, B beta 1-14(Lys14), B beta 1-13, or B beta 3-14 primed for significant helper T cell activity, as assessed by the augmentation of a primary in vitro B cell IgM anti-FITC plaque-forming cell response after culture with B beta 1-1(Lys14)-FITC. Significant peptide-specific helper activity was observed when the FITC moiety was conjugated to the carboxyl terminal lysine (B beta 1-14(Lys14)-FITC) as well as FITC substitution at the amino terminus (FITC-B beta 3-13 or FITC-B beta 3-14). These results suggest that the fine specificity of T cell responses to peptide antigens are different for helper and proliferating T cells and that responsiveness by one T cell subpopulation does not predict the response pattern of other functional subpopulations.

摘要

相似文献

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Proliferating and helper T lymphocytes display distinct fine specificities in response to human fibrinopeptide B.
J Immunol. 1983 Jun;130(6):2542-5.
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Immunogenetics. 1994;39(1):21-8. doi: 10.1007/BF00171793.
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In vitro antigen-induced antibody responses to hepatitis B surface antigen in man. Kinetic and cellular requirements.人对乙型肝炎表面抗原的体外抗原诱导抗体反应。动力学和细胞需求。
J Clin Invest. 1984 Oct;74(4):1204-13. doi: 10.1172/JCI111529.
3
Mechanisms of genetic control of immune responses. I. Evidence for distinct multi-step helper T-cell pathways in cellular and humoral responses to GAT.
免疫反应的遗传控制机制。I. 对谷氨酸-丙氨酸-酪氨酸(GAT)的细胞免疫和体液免疫反应中不同多步骤辅助性T细胞途径的证据。
Immunogenetics. 1984;19(5):391-407. doi: 10.1007/BF00364643.
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In vitro immune responses to hepatitis B surface antigen (Pre-S2 and S) following remote infection by hepatitis B virus in humans.人类感染乙肝病毒后对乙肝表面抗原(前S2和S)的体外免疫反应。
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