Förster E, Krenger W, Joergensen J, Hof R, Geha R S, Holländer G A
Department of Research, Basel University Medical School, Switzerland.
Transplantation. 1999 May 15;67(9):1284-7. doi: 10.1097/00007890-199905150-00016.
Costimulation through CD40-CD154 plays an important role in T-cell activation. Although systemic administration of anti-CD154 antibody prevents or delays rejection of organ allografts in animal models, the molecular mechanisms responsible for this effect are not well defined.
We have previously demonstrated that priming of mice (H2d) with CD40-/- but not with wildtype naive B cells (H2b) leads to alloantigen-specific T-cell hyporesponsiveness in vitro. In the present study, we investigated whether such priming modifies allograft rejection in a major histocompatibility complex-mismatched murine cardiac transplantation model.
Priming of hosts with donor-specific CD40-/- B cells delayed rejection of subsequently transplanted wild-type cardiac allografts by 8.0 days (P<0.001). The lack of CD40 on the cardiac graft delayed rejection in unprimed or primed hosts by 3-5 days. Prolongation of graft survival correlated with the failure of infused CD40-/- B cells to express B7.2 and ICAM-1 in vivo.
Our data suggest that CD40-CD154 costimulation contributes to T cell priming to alloantigens in vivo and to a second set rejection phase in which donor antigens are presented to primed T cells.
通过CD40 - CD154的共刺激在T细胞活化中起重要作用。尽管在动物模型中全身给予抗CD154抗体可预防或延迟器官同种异体移植的排斥反应,但导致这种效应的分子机制尚未明确。
我们先前已证明,用CD40 - / - 小鼠(H2d)而非野生型幼稚B细胞(H2b)对小鼠进行预刺激,可导致体外同种异体抗原特异性T细胞低反应性。在本研究中,我们调查了这种预刺激是否会在主要组织相容性复合体不匹配的小鼠心脏移植模型中改变同种异体移植排斥反应。
用供体特异性CD40 - / - B细胞对宿主进行预刺激可使随后移植的野生型心脏同种异体移植物的排斥反应延迟8.0天(P < 0.001)。心脏移植物上缺乏CD40可使未预刺激或预刺激的宿主中的排斥反应延迟3 - 5天。移植物存活时间的延长与注入的CD40 - / - B细胞在体内未能表达B7.2和ICAM - 1相关。
我们的数据表明,CD40 - CD154共刺激在体内有助于T细胞对同种异体抗原的致敏以及有助于将供体抗原呈递给致敏T细胞的二次排斥反应阶段。
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