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对肿瘤抗原免疫反应的调节。VI. 抑制性T细胞或其产物与效应性T细胞的差异特异性。

Regulation of the immune response to tumor antigen. VI. Differential specificities of suppressor T cells or their products and effector T cells.

作者信息

Greene M I, Perry L L

出版信息

J Immunol. 1978 Dec;121(6):2363-6.

PMID:82582
Abstract

Suppressor T cells arising during the development of certain murine methylcholanthrene-induced fibrosarcomas have previously been shown capable of limiting only those effector responses generated against the homologous tumor. Thus, S1509a-induced suppressor T cells inhibit immune reactivity only to the S1509a tumor in S1509a immune mice and have no effect on the rejection of SAI tumors in SAI-immune animals. In contrast to this is the cross-reactivity of effector cells in this system, whereby animals rendered immune to either the S1509a or SAI sarcoma are equally capable of rejecting a challenge of the opposite tumor. The specificity of suppression has been further defined in the present study, which demonstrates that S1509a-induced suppressor cells can inhibit responsiveness only to the S1509a sarcoma, even in the simultaneous presence of both the S1509a and SAI tumors. Furthermore, the suppressor factor that is obtainable from suppressor T cells demonstrates a similar precise specificity in its ability to limit selectively reactivity only against the inducing tumor, regardless of the simultaneous expression of antigens on other tumors recognized by cross-reactive effector cells. These results suggest that the antigenic determinants recognized by effector and suppressor T cells are different, and may provide a model for further dissection of suppressor cell function in vivo.

摘要

先前已表明,在某些小鼠甲基胆蒽诱导的纤维肉瘤发展过程中产生的抑制性T细胞仅能限制针对同源肿瘤产生的那些效应反应。因此,S1509a诱导的抑制性T细胞仅抑制S1509a免疫小鼠对S1509a肿瘤的免疫反应性,而对SAI免疫动物中SAI肿瘤的排斥没有影响。与此相反的是该系统中效应细胞的交叉反应性,即对S1509a或SAI肉瘤产生免疫的动物同样能够排斥相反肿瘤的攻击。在本研究中,抑制作用的特异性得到了进一步明确,该研究表明,即使在同时存在S1509a和SAI肿瘤的情况下,S1509a诱导的抑制性细胞也仅能抑制对S1509a肉瘤的反应性。此外,从抑制性T细胞中获得的抑制因子在其仅选择性地限制针对诱导肿瘤的反应性的能力方面表现出类似的精确特异性,而不考虑交叉反应性效应细胞识别的其他肿瘤上抗原的同时表达。这些结果表明,效应性T细胞和抑制性T细胞识别的抗原决定簇不同,可能为进一步剖析体内抑制性细胞功能提供一个模型。

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