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Cytokine profiles in early rejection following OKT3 treatment in liver transplant patients.

机译:OKT3治疗后肝移植患者早期排斥反应中的细胞因子谱。

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摘要

OKT3 , a murine monoclonal antibody specific to the human CD3 complex, induces immunosuppression by depletion of T cells. Administration of OKT3 results in significant release of proinflammatory cytokines, such as TNFalpha and IL1beta. Liver recipients who experience rejection within 3 weeks after transplantation with OKT3 prophylaxis recover their T cells by postoperative day 10 despite complete initial clearance. We sought to analyze the role of proinflammatory and Th-1 cytokines in T cell recovery and rejection after liver transplantation with OKT3 prophylaxis. In plasma samples from 32 patients, we measured TNFalpha, IL1beta and IL6 (before transplant and on postoperative days 1, 2 and 3) and IL2, IFNgamma, sIL2R and slCAM (postoperative days 5, 7 and 10) and examined possible correlations with T-cell recovery and occurrence of rejection within 3 weeks. TNFalpha, IL1beta, and IL6 did not correlate with T-cell recovery. In patients who rejected, IL2 and IFNgamma on postoperative days 5 and 7 correlated with degree of T-cell recovery by day 10; a significant rise in sIL2R over time also correlated with T-cell recovery in this group. Our results emphasize the role of Th-1 cytokines in rejection following OKT3 induction and suggest that markers of T cell activation may predict risk.
机译:OKT3是人CD3复合物特异的鼠类单克隆抗体,可通过耗竭T细胞来诱导免疫抑制。 OKT3的使用导致促炎性细胞因子(如TNFalpha和IL1beta)的大量释放。尽管最初已完全清除,但在接受OKT3预防的移植后3周内出现排斥反应的肝受体在术后10天仍能恢复其T细胞。我们试图分析在使用OKT3预防肝移植后促炎和Th-1细胞因子在T细胞恢复和排斥中的作用。在32例患者的血浆样本中,我们测量了TNFalpha,IL1beta和IL6(在移植前以及术后第1、2和3天)以及IL2,IFNgamma,sIL2R和s​​lCAM(术后第5、7和10天),并检查了与T的可能相关性-细胞恢复并在3周内出现排斥反应。 TNFalpha,IL1beta和IL6与T细胞恢复无关。在被拒绝的患者中,术后第5天和第7天的IL2和IFNgamma与第10天的T细胞恢复程度相关。 sIL2R随时间的显着升高也与该组的T细胞恢复相关。我们的结果强调了OKT3诱导后Th-1细胞因子在排斥反应中的作用,并暗示T细胞活化的标志物可预测风险。

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