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导致致死性移植物抗宿主病的T细胞表面标志物与I类和II类H-2差异。

Surface markers of T cells causing lethal graft-vs-host disease to class I vs class II H-2 differences.

作者信息

Korngold R, Sprent J

出版信息

J Immunol. 1985 Nov;135(5):3004-10.

PMID:3876371
Abstract

Information was sought on the phenotype of lymphoid cells causing lethal graft-vs-host disease (GVHD) in irradiated mice expressing whole or partial H-2 differences. In all strain combinations tested, pretreating donor lymph node (LN) cells with anti-Thy-1 monoclonal antibodies (MAb) plus complement (C) abolished mortality. With GVHD directed to class I H-2 differences, pretreating LN cells with anti-Lyt-2 MAb prevented mortality, whereas MAb specific for Ly-1 or L3T4 cell surface determinants caused severe mortality. These data imply that lethal GVHD directed to class I H-2 differences is mediated by L3T4-, Lyt-2+ cells; this subset of T cells was shown previously to control GVHD directed to multiple minor histocompatibility antigens, i.e., antigens seen in the context of self-class I molecules. With whole H-2 differences, GVHD appeared to be controlled largely but not exclusively by L3T4+, Lyt-2-T cells. This T cell subset was also the predominant cause of GVHD directed to class II differences. With class II incompatibilities, depleting donor cells of L3T4+ T cells, either by pretreatment with anti-L3T4 MAb + C or by fluorescence activated cell sorter selection, greatly reduced but did not completely abolish GVHD. These data might imply that L3T4-, Lyt-2+ cells have some capacity to elicit anti-class II GVHD. A more likely possibility, however, is that the residual GVHD to class II differences observed with Lyt-2+-enriched cells reflected minor contamination with L3T4+ cells.

摘要

我们研究了在表达全部或部分H-2差异的受辐照小鼠中,引发致死性移植物抗宿主病(GVHD)的淋巴细胞表型。在所有测试的品系组合中,用抗Thy-1单克隆抗体(MAb)加补体(C)预处理供体淋巴结(LN)细胞可消除死亡率。对于针对I类H-2差异的GVHD,用抗Lyt-2 MAb预处理LN细胞可预防死亡,而针对Ly-1或L3T4细胞表面决定簇的MAb则会导致严重死亡。这些数据表明,针对I类H-2差异的致死性GVHD是由L3T4-、Lyt-2+细胞介导的;先前已证明该T细胞亚群可控制针对多种次要组织相容性抗原的GVHD,即在自身I类分子背景下可见的抗原。对于全部H-2差异,GVHD似乎在很大程度上但并非完全由L3T4+、Lyt-2-T细胞控制。该T细胞亚群也是针对II类差异的GVHD的主要原因。对于II类不相容性,通过用抗L3T4 MAb + C预处理或通过荧光激活细胞分选仪选择来耗尽供体细胞中的L3T4+ T细胞,可大大降低但并未完全消除GVHD。这些数据可能意味着L3T4-、Lyt-2+细胞具有引发抗II类GVHD的某种能力。然而,更有可能的情况是,用富含Lyt-2+细胞观察到的针对II类差异的残留GVHD反映了L3T4+细胞的轻微污染。

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