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新生儿耐受中细胞毒性T细胞库的改变。对耐受原亲和力低的细胞优先存活的证据。

Modification of the cytotoxic T cell repertoire in neonatal tolerance. Evidence for preferential survival of cells with low avidity for tolerogen.

作者信息

Wood P J, Socarras S, Streilein J W

机构信息

Department of Microbiology and Immunology, University of Miami School of Medicine, FL 33134.

出版信息

J Immunol. 1987 Nov 15;139(10):3236-44.

PMID:3316382
Abstract

Clonal deletion of developing lymphocytes with potential reactivity for self is thought to play a crucial role in the establishment of self tolerance. One prediction of the clonal deletion hypothesis is that cells bearing receptors with high affinity for self are more likely than cells with low affinity receptors to be deleted from the repertoire. Experimental models of B cell tolerance have provided evidence for the preferential survival of low affinity cells with specificity for tolerogen in tolerant animals, but no comparable evidence exists for T cells. To examine this issue in T cells, cytotoxic T cell lines specific for the Kb mutant class I H-2 molecule, bm1, were generated from C57BL/6 mice rendered neonatally tolerant of bm1 and compared with anti-bm1 lines generated from normal mice. Compared with normal lines, those from tolerant mice differed in five ways: 1) they grew more slowly; 2) they were less efficient at lysing bm1 targets; 3) they showed different patterns of lysis against a panel of third party targets; 4) their cytotoxic activity against bm1 could be increased in the presence of leukoagglutinin, whereas the activity of normal lines was not increased by leukoagglutinin; and 5) their cytotoxic activity was more susceptible to inhibition by anti-Lyt-2 antibody. Taken together, these results demonstrate that the repertoire of the remaining tolerogen-specific cytotoxic T cells in neonatally tolerant mice is different from the normal C57BL/6 anti-bm1 repertoire, and the results are consistent with the idea that the remaining tolerogen-specific cells are low avidity cells that have preferentially escaped the clonal deletion process.

摘要

对自身具有潜在反应性的发育中淋巴细胞的克隆清除,被认为在自身耐受的建立中起关键作用。克隆清除假说的一个预测是,与自身具有高亲和力受体的细胞比具有低亲和力受体的细胞更有可能从细胞库中被清除。B细胞耐受的实验模型为耐受动物中对耐受原具有特异性的低亲和力细胞的优先存活提供了证据,但对于T细胞则不存在类似的证据。为了在T细胞中研究这个问题,从新生期耐受bm1的C57BL/6小鼠中产生了对Kb突变I类H-2分子bm1特异的细胞毒性T细胞系,并与从正常小鼠产生的抗bm1细胞系进行比较。与正常细胞系相比,来自耐受小鼠的细胞系在五个方面有所不同:1)它们生长较慢;2)它们裂解bm1靶标的效率较低;3)它们对一组第三方靶标的裂解模式不同;4)在白细胞凝集素存在下,它们对bm1的细胞毒性活性可以增加,而正常细胞系的活性则不会因白细胞凝集素而增加;5)它们的细胞毒性活性更容易受到抗Lyt-2抗体的抑制。综上所述,这些结果表明,新生期耐受小鼠中剩余的耐受原特异性细胞毒性T细胞库与正常的C57BL/6抗bm1细胞库不同,并且这些结果与以下观点一致,即剩余(的)耐受原特异性细胞是优先逃脱克隆清除过程的低亲和力细胞。

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