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接受基于钙调神经磷酸酶抑制剂药物方案治疗的患者中效应性T细胞和调节性T细胞的差异动力学。

Differential kinetics of effector and regulatory T cells in patients on calcineurin inhibitor-based drug regimens.

作者信息

Presser Daniela, Sester Urban, Mohrbach Janine, Janssen Martin, Köhler Hans, Sester Martina

机构信息

Department of Internal Medicine IV, University of the Saarland, Homburg D-66421, Germany.

出版信息

Kidney Int. 2009 Sep;76(5):557-66. doi: 10.1038/ki.2009.198. Epub 2009 Jun 3.

Abstract

Besides iatrogenic immunosuppression, endogenous suppression by regulatory T cells (Tregs) may also mediate inhibition of effector T cells after transplantation. Here we determined the effect of common immunosuppressive drug regimens on both Treg and effector T cells. Tregs and cytomegalovirus (CMV)-specific T cells were quantified in 88 renal transplant recipients, 58 hemodialysis patients, and 22 controls. T cell dynamics were longitudinally assessed within 20 weeks after transplantation. The number of Tregs was quantified by measurement of CD25 and/or FOXP3-positive cells and by functional assays. CMV-specific T cells were quantified by stimulation-induced intracellular cytokine analysis. Treg frequencies in transplant recipients were significantly lower compared to those in hemodialysis patients and controls. These lower Treg levels were associated with a less pronounced suppression of effector function. Treg levels decreased within the first weeks after transplantation and remained low in the long term. In contrast, although decreased at early post-transplant, long-term levels of CMV-specific T cells normalized to levels found in hemodialysis patients and controls. These studies suggest that there is an initial decrease of Tregs and effector T cells as a consequence of a direct inhibitory effect of immunosuppressive drugs. In the long term, persistently low Treg levels may favor normalization of effector T cells to ensure sufficient pathogen control.

摘要

除了医源性免疫抑制外,调节性T细胞(Tregs)的内源性抑制也可能介导移植后效应T细胞的抑制。在此,我们确定了常见免疫抑制药物方案对Tregs和效应T细胞的影响。对88例肾移植受者、58例血液透析患者和22例对照者的Tregs和巨细胞病毒(CMV)特异性T细胞进行了定量分析。在移植后20周内纵向评估T细胞动力学。通过测量CD25和/或FOXP3阳性细胞以及功能测定来定量Tregs的数量。通过刺激诱导的细胞内细胞因子分析来定量CMV特异性T细胞。与血液透析患者和对照者相比,移植受者中的Treg频率显著降低。这些较低的Treg水平与效应功能抑制不明显相关。Treg水平在移植后的最初几周内下降,并长期保持在较低水平。相比之下,尽管移植后早期CMV特异性T细胞水平下降,但其长期水平恢复到血液透析患者和对照者中的水平。这些研究表明,由于免疫抑制药物的直接抑制作用,Tregs和效应T细胞最初会减少。从长期来看,持续较低的Treg水平可能有利于效应T细胞的正常化,以确保对病原体的充分控制。

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