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1型辅助性T细胞刺激对初始及回忆性变应原特异性2型辅助性T细胞介导反应的抑制作用

Inhibition of primary and recall allergen-specific T helper cell type 2-mediated responses by a T helper cell type 1 stimulus.

作者信息

Scott D E, Agranovich I, Inman J, Gober M, Golding B

机构信息

Center for Biologics Evaluation and Research, Division of Hematology, Food and Drug Administration, Bethesda, MD 20892, USA.

出版信息

J Immunol. 1997 Jul 1;159(1):107-16.

PMID:9200445
Abstract

Allergic responses are characterized by the production of Ag-specific IgE Abs that are dependent upon Th2-mediated T cell help. We determined whether heat-killed Brucella abortus (BA), an inducer of Th1 responses, could influence the allergic Th2-mediated IgE response to OVA adsorbed to alum (O/A). BA plus O/A, but not O/A alone, induced high levels of mRNA for IFN-gamma and IL-12 promptly after injection. Furthermore, initial treatment with BA plus O/A rendered both BALB/c and C57Bl/6 mice incapable of mounting high IgE responses even after repeated challenges with allergen alone. Long term abrogation of anti-OVA IgE correlated with an increased frequency of IFN-gamma-secreting OVA-specific cells and a decreased frequency of IL-4-secreting OVA-specific cells. Initial treatment with anti-IL-12 prevented BA-induced early IFN-gamma production and secondary IgG2a responses, but did not abrogate IgE suppression. Additionally, secondary OVA-specific IgE responses were down-regulated by BA conjugated to OVA or by BA given with O/A. BA-induced down-regulation of secondary IgE responses was associated with increased frequency of Ag-specific IFN-gamma-secreting cells. These results suggest the possibility that even recall Th2-mediated immune responses can be attenuated if Ag is given with a carrier or adjuvant that induces potent Th1-promoting cytokines.

摘要

过敏反应的特征是产生依赖于Th2介导的T细胞辅助的抗原特异性IgE抗体。我们确定了作为Th1反应诱导剂的热灭活布鲁氏菌流产株(BA)是否会影响对吸附于明矾的卵清蛋白(O/A)的过敏性Th2介导的IgE反应。注射后,BA加O/A而非单独的O/A迅速诱导了高水平的IFN-γ和IL-12 mRNA。此外,用BA加O/A进行初始治疗使BALB/c和C57Bl/6小鼠即使在仅用变应原反复攻击后也无法产生高IgE反应。抗OVA IgE的长期消除与分泌IFN-γ的OVA特异性细胞频率增加和分泌IL-4的OVA特异性细胞频率降低相关。用抗IL-12进行初始治疗可预防BA诱导的早期IFN-γ产生和继发性IgG2a反应,但不能消除IgE抑制。此外,与OVA偶联的BA或与O/A一起给予的BA可下调继发性OVA特异性IgE反应。BA诱导的继发性IgE反应下调与抗原特异性分泌IFN-γ的细胞频率增加有关。这些结果表明,如果抗原与诱导强效Th1促进细胞因子的载体或佐剂一起给予,即使是回忆性Th2介导的免疫反应也可能减弱。

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