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Quantification of Torque Teno Virus and Epstein-Barr Virus Is of Limited Value for Predicting the Net State of Immunosuppression After Lung Transplantation

机译:量化扭矩Teno病毒和Epstein-Barr病毒对预测肺移植后免疫抑制的净状态具有有限的价值

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BackgroundMajor hurdles for survival after lung transplantation are rejections and infectious complications. Adequate methods for monitoring immune suppression status are lacking. Here, we evaluated quantification of torque teno virus (TTV) and Epstein-Barr virus (EBV) as biomarkers for defining the net state of immunosuppression in lung-transplanted patients.MethodsThis prospective single-center study included 98 patients followed for 2 years after transplantation. Bacterial infections, fungal infections, viral respiratory infections (VRTI), cytomegalovirus (CMV) viremia, and acute rejections, as well as TTV and EBV levels, were monitored.ResultsThe levels of torque teno virus DNA increased rapidly after transplantation, likely due to immunosuppressive treatment. A modest increase in levels of Epstein-Barr virus DNA was also observed after transplantation. There were no associations between either TTV or EBV and infectious events or acute rejection, respectively, during follow-up. When Tacrolimus was the main immunosuppressive treatment, TTV DNA levels were significantly elevated 6–24 months after transplantation as compared with Cyclosporine treatment.ConclusionsAlthough replication of TTV, but not EBV, appears to reflect the functionality of the immune system, depending on the type of immunosuppressive treatment, quantification of TTV or EBV as biomarkers has limited potential for defining the net state of immune suppression.
机译:背景肺移植后生存的主要障碍是排斥反应和感染性并发症。缺乏监测免疫抑制状态的适当方法。在这里,我们评估了扭力腱病毒(TTV)和爱泼斯坦-巴尔病毒(EBV)的定量作为生物标记物,以定义肺移植患者免疫抑制的净状态。方法这项前瞻性单中心研究包括98位患者,随访了2年。 。监测细菌感染,真菌感染,病毒性呼吸道感染(VRTI),巨细胞病毒(CMV)病毒血症和急性排斥反应以及TTV和EBV水平。结果移植后扭矩Teno病毒DNA的水平迅速增加,可能是由于免疫抑制治疗。移植后还观察到爱泼斯坦-巴尔病毒DNA水平的适度增加。在随访期间,TTV或EBV与感染事件或急性排斥反应之间没有关联。当他克莫司是主要的免疫抑制治疗时,与环孢霉素治疗相比,移植后6-24个月TTV DNA水平显着升高。结论尽管TTV的复制而非EBV的复制似乎反映了免疫系统的功能,具体取决于免疫抑制治疗,将TTV或EBV量化为生物标记物的潜力有限,无法定义免疫抑制的净状态。

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