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从长期T细胞受体下调中恢复的T细胞受体αβ⁺ T细胞的致敏作用。

Sensitization of T-cell receptor-alpha beta+ T cells recovered from long-term T-cell receptor downmodulation.

作者信息

Omoto K, Kong Y Y, Nomoto K, Umesue M, Murakami Y, Eto M, Nomoto K

机构信息

Department of Immunology, Kyushu University, Fukuoka, Japan.

出版信息

Immunology. 1996 Jun;88(2):230-7. doi: 10.1111/j.1365-2567.1996.tb00009.x.

Abstract

Although the survival of fully allogeneic skin grafts was prominently prolonged by adult thymectomy in anti-T-cell receptor-alpha beta monoclonal antibody (TCR-alpha beta mAb)-treated mice compared with that of non-adult thymectomized (ATX) mice, the skin allografts were eventually rejected. In the anti-TCR-alpha beta mAb-treated ATX mice, as shown in the present study, most of TCR-alpha beta+ cells were promptly activated on day 2 and then rapidly disappeared by day 7, but some TCR-alpha beta- Thy-1+ cells remained at that time. These TCR-alpha beta- Thy-1+ cells which have downmodulated their TCR-alpha beta expression may be refractory to depletion events by the mAb treatment. Although these downmodulated T cells re-expressed their TCR-alpha beta on day 50, they could not respond to stimuli via TCR such as TCR cross-linking or alloantigens. However, they recovered the reactivity to donor antigens on day 85. These results indicate that the downmodulated T cells by anti-TCR-alpha beta mAb treatment are long-lived and re-express their TCR-alpha beta at a late stage to be sensitized to donor antigen, which suggests that additional regimens may be required to get permanent, or very long-term, graft acceptance.

摘要

与未进行成年胸腺切除(ATX)的小鼠相比,在抗T细胞受体αβ单克隆抗体(TCR-αβ mAb)处理的小鼠中,成年胸腺切除显著延长了完全同种异体皮肤移植物的存活时间,但皮肤同种异体移植物最终还是被排斥了。如本研究所示,在抗TCR-αβ mAb处理的ATX小鼠中,大多数TCR-αβ⁺细胞在第2天迅速被激活,然后在第7天迅速消失,但此时仍有一些TCR-αβ⁻ Thy-1⁺细胞存在。这些下调了TCR-αβ表达的TCR-αβ⁻ Thy-1⁺细胞可能对mAb处理的清除事件具有抗性。尽管这些下调的T细胞在第50天重新表达了它们的TCR-αβ,但它们无法通过TCR对诸如TCR交联或同种异体抗原等刺激做出反应。然而,它们在第85天恢复了对供体抗原的反应性。这些结果表明,抗TCR-αβ mAb处理下调的T细胞寿命长,并在后期重新表达其TCR-αβ以对供体抗原敏感,这表明可能需要额外的方案来实现永久或非常长期的移植物接受。

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Peripheral tolerance as a multi-step mechanism.外周耐受作为一种多步骤机制。
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