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自身载体在免疫应答和耐受性中的作用。V. 通过阻断H-2抗原逆转三硝基苯基修饰的自身对B细胞应答的抑制作用。

Role of self carriers in the immune response and tolerance. V. Reversal of trinitrophenyl-modified self suppression of the B-cell response by blocking of H-2 antigens.

作者信息

Jandinski J J, Li J, Wettstein P J, Frelinger J A, Scott D W

出版信息

J Exp Med. 1980 Jan 1;151(1):133-43. doi: 10.1084/jem.151.1.133.

Abstract

Trinitrophenylated syngeneic spleen cells (TNP-SC) are potent tolerogens of the anti-TNP plaque-forming cell (PFC) response in vivo and in vitro. This unresponsive state requires T cells for both its induction and maintenance. Because H-2K/D-restricted cytotoxic T cells are also induced by exposure to TNP-SC, we determined the role(s) of histocompatibility antigens (K, I, and D) in the suppression of the PFC response by TNP-SC. We treated syngeneic TNP-modified stimulator cells with antiserum directed at K-, I-, or D-region determinants and found that blocking of H-2K or D antigens on TNP-SC transformed these tolerogens into immunogens capable of eliciting an anti-TNP PFC response in the absence of extrinsic immunogens like TNP-polymerized flagellin. In H-2k or H-2a(k/d) mice, only H-2Kk needs to be blocked on the stimulator cells, whereas H-2K or D recognition was apparent in B10.A(4R) mice. These observations indicate that suppression of the PFC response by TNP-SC shows the same restriction in recognition as does the cytotoxic T-cell response. Furthermore, our results suggest that TNP-I-A is recognized by the helper cells in this system as the intrinsic antigen. When both TNP-K and TNP-I-A are present and available on the same stimulator cell, suppression (via modified K recognition) is dominant over help.

摘要

三硝基苯基化的同基因脾细胞(TNP-SC)在体内和体外都是抗TNP斑块形成细胞(PFC)反应的有效耐受原。这种无反应状态的诱导和维持都需要T细胞。由于暴露于TNP-SC也会诱导H-2K/D限制性细胞毒性T细胞,我们确定了组织相容性抗原(K、I和D)在TNP-SC抑制PFC反应中的作用。我们用针对K区、I区或D区决定簇的抗血清处理同基因TNP修饰的刺激细胞,发现阻断TNP-SC上的H-2K或D抗原可将这些耐受原转化为免疫原,能够在没有TNP-聚合鞭毛蛋白等外源性免疫原的情况下引发抗TNP PFC反应。在H-2k或H-2a(k/d)小鼠中,只需在刺激细胞上阻断H-2Kk,而在B10.A(4R)小鼠中则明显存在H-2K或D识别。这些观察结果表明,TNP-SC对PFC反应的抑制在识别上与细胞毒性T细胞反应具有相同的限制性。此外,我们的结果表明,在该系统中,辅助细胞将TNP-I-A识别为内在抗原。当TNP-K和TNP-I-A同时存在于同一个刺激细胞上且可被识别时,抑制(通过修饰的K识别)比辅助作用占主导地位。

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