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T杀伤细胞在同种异体骨髓移植排斥反应中起作用,但在杂种抗性中不起作用。

T killer cells play a role in allogeneic bone marrow graft rejection but not in hybrid resistance.

作者信息

Dennert G, Anderson C G, Warner J

出版信息

J Immunol. 1985 Dec;135(6):3729-34.

PMID:3905963
Abstract

Results of recent experiments have provided compelling evidence supporting the hypothesis that the acute rejection of bone marrow transplants by allogeneic and semiallogeneic recipients is principally due to the action of natural killer (NK) cells. The observed specificity of graft rejection is likely induced by target-specific antibody that guides the NK cells in an antibody-dependent cytolytic reaction resulting in the elimination of the graft. The sole involvement of NK cells in marrow graft rejection, however, is contradicted by several observations that point to the environment of specific T cells. Results presented in this paper demonstrate that in allogeneic marrow graft rejection models, T killer cells are capable of causing graft rejection provided a prior sensitization phase is allowed. Thus, mice not able to reject marrow grafts in a primary response via their NK cells will do so in a primed secondary response via their T cells. Rejection is specific in that only marrow grafts H-2 identical to the sensitizing marrow graft are rejected. Sensitization for NK cell independent marrow graft rejection can be accomplished by prior priming with allogeneic tumor cells or by injection of cloned T killer cells. In contrast to bone marrow allograft rejection, the hybrid resistance model in which F1 hybrid mice reject parental marrow grafts does not appear to induce T killer cells in vivo. Neither marrow grafts nor tumor cells prime F1 hybrids for a second-set parental graft rejection. Moreover, F1 hybrid antiparental T killer cells induced in vitro and adoptively transferred in vivo fail to transfer hybrid resistance. Therefore, there appear to be potent mechanisms acting in vivo that suppress the action or induction of F1 hybrid T killer cells specific to parental antigens.

摘要

近期实验结果提供了有力证据,支持以下假说:同种异体和半同种异体受体对骨髓移植的急性排斥反应主要归因于自然杀伤(NK)细胞的作用。观察到的移植物排斥特异性可能是由靶特异性抗体诱导的,该抗体在抗体依赖性细胞溶解反应中引导NK细胞,从而导致移植物被清除。然而,NK细胞在骨髓移植物排斥反应中的唯一作用与一些指向特异性T细胞环境的观察结果相矛盾。本文给出的结果表明,在同种异体骨髓移植排斥模型中,如果给予预先致敏阶段,杀伤性T细胞能够导致移植物排斥。因此,无法通过NK细胞在初次反应中排斥骨髓移植物的小鼠,将在致敏后的二次反应中通过T细胞做到这一点。排斥具有特异性,因为只有与致敏骨髓移植物H-2相同的骨髓移植物才会被排斥。对NK细胞非依赖性骨髓移植物排斥的致敏可通过用同种异体肿瘤细胞预先致敏或注射克隆的杀伤性T细胞来实现。与骨髓同种异体移植排斥不同,F1杂种小鼠排斥亲代骨髓移植物的杂种抗性模型似乎不会在体内诱导杀伤性T细胞。骨髓移植物和肿瘤细胞都不会使F1杂种小鼠对第二次亲代移植物排斥产生致敏。此外,体外诱导并体内过继转移的F1杂种抗亲代杀伤性T细胞未能转移杂种抗性。因此,似乎存在强大的体内机制抑制针对亲代抗原的F1杂种杀伤性T细胞的作用或诱导。

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