Pretransplant, Th17 dominant alloreactivity in highly sensitized kidney transplant candidates

Sarita Negi, Alissa K Rutman, C. Saw, S. Paraskevas, J. Tchervenkov
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Abstract

Sensitization to donor human leukocyte antigen (HLA) molecules prior to transplantation is a significant risk factor for delayed access to transplantation and to long-term outcomes. Memory T cells and their cytokines play a pivotal role in shaping immune responses, thereby increasing the risk of allograft rejection among highly sensitized patients. This study aims to elucidate the precise contribution of different CD4+ memory T cell subsets to alloreactivity in highly sensitized (HS) kidney transplant recipients.Stimulation of peripheral blood mononuclear cells (PBMC) with various polyclonal stimulating agents to assess non-specific immune responses revealed that HS patients exhibit elevated immune reactivity even before kidney transplantation, compared to non-sensitized (NS) patients. HS patients' PBMC displayed higher frequencies of CD4+ T cells expressing IFNγ, IL4, IL6, IL17A, and TNFα and secreted relatively higher levels of IL17A and IL21 upon stimulation with PMA/ionomycin. Additionally, PBMC from HS patients stimulated with T cell stimulating agent phytohemagglutinin (PHA) exhibited elevated expression levels of IFNγ, IL4 and, IL21. On the other hand, stimulation with a combination of resiquimod (R848) and IL2 for the activation of memory B cells demonstrated higher expression of IL17A, TNFα and IL21, as determined by quantitative real-time PCR. A mixed leukocyte reaction (MLR) assay, employing third-party donor antigen presenting cells (APCs), was implemented to evaluate the direct alloreactive response. HS patients demonstrated notably higher frequencies of CD4+ T cells expressing IL4, IL6 and IL17A. Interestingly, APCs expressing recall HLA antigens triggered a stronger Th17 response compared to APCs lacking recall HLA antigens in sensitized patients. Furthermore, donor APCs induced higher activation of effector memory T cells in HS patients as compared to NS patients.These results provide an assessment of pretransplant alloreactive T cell subsets in highly sensitized patients and emphasize the significance of Th17 cells in alloimmune responses. These findings hold promise for the development of treatment strategies tailored to sensitized kidney transplant recipients, with potential clinical implications.
高度致敏肾移植候选者移植前的 Th17 显性异体反应
移植前对供体人类白细胞抗原(HLA)分子致敏是导致移植手术延迟和长期预后的一个重要风险因素。记忆 T 细胞及其细胞因子在形成免疫反应方面起着关键作用,从而增加了高度致敏患者发生异体移植排斥反应的风险。用各种多克隆刺激剂刺激外周血单核细胞(PBMC)以评估非特异性免疫反应,结果显示,与非致敏(NS)患者相比,HS 患者甚至在肾移植前就表现出较高的免疫反应性。HS 患者的 PBMC 中表达 IFNγ、IL4、IL6、IL17A 和 TNFα 的 CD4+ T 细胞频率较高,在 PMA/ionomycin 刺激下分泌的 IL17A 和 IL21 水平也相对较高。此外,用刺激 T 细胞的植物血凝素(PHA)刺激 HS 患者的 PBMC,其 IFNγ、IL4 和 IL21 的表达水平也会升高。另一方面,用瑞喹莫德(R848)和 IL2 联合刺激以激活记忆 B 细胞时,经实时定量 PCR 检测,IL17A、TNFα 和 IL21 的表达较高。采用第三方供体抗原递呈细胞(APCs)进行混合白细胞反应(MLR)测定,以评估直接异体反应。HS患者表达IL4、IL6和IL17A的CD4+T细胞频率明显更高。有趣的是,在致敏患者中,与缺乏回顾性HLA抗原的APC相比,表达回顾性HLA抗原的APC能引发更强的Th17反应。这些结果提供了对高度致敏患者移植前异体反应T细胞亚群的评估,并强调了Th17细胞在异体免疫反应中的重要性。这些发现为开发针对致敏肾移植受者的治疗策略带来了希望,并具有潜在的临床意义。
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