首页> 外文期刊>Pediatric transplantation. >Quantiferon‐Cytomegalovirus assay: A potentially useful tool in the evaluation of CMV CMV ‐specific CD CD 8+ T‐cell reconstitution in pediatric hematopoietic stem cell transplant patients
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Quantiferon‐Cytomegalovirus assay: A potentially useful tool in the evaluation of CMV CMV ‐specific CD CD 8+ T‐cell reconstitution in pediatric hematopoietic stem cell transplant patients

机译:Quantiferon-cytomegalovirus测定:在儿科造血干细胞移植患者中评估CMV CMV-特异性CD 8 + T细胞重构的潜在有用的工具

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Abstract Pediatric HSCT recipients are at high risk for CMV reactivation due to their immature immune system and therapy following transplantation. Reconstitution of CMV ‐specific T‐cell immunity is associated with control and protection against CMV . The clinical utility of monitoring CMV ‐specific CMI to predict CMV viremia in pediatric HSCT patients using the Quantiferon‐ CMV ( QIAGEN ? ) test was investigated prospectively. Thirty‐seven pediatric allogeneic HSCT recipients were enrolled from 3/2010‐6/2012. CMV viremia was detected via weekly real‐time PCR . The Quantiferon‐ CMV test was conducted pretransplant, early after transplantation, 30, 90 , 180 , 270, and 360?days post‐transplantation. The incidence of CMV viremia was 51% (19/37) with half of the episodes within ≤30?days post‐transplant. Fifteen patients showed CMV ‐specific immunity (average of 82?days). The cumulative incidence of CMV reactivation in patients who developed CMV ‐specific immunity was lower than those who did not (15% vs 53%; P ?=?.023). The ROC statistical analysis showed that the AUC was 0.725 in predicting viremia, for Quantiferon‐ CMV test. In this cohort, the Quantiferon‐ CMV assay was a valuable method for identifying pediatric HSCT patients at high risk for CMV viremia, suggesting potential clinical utility to individualize patient's management post‐transplant.
机译:摘要儿科HSCT接受者由于其未成熟的免疫系统和移植后治疗而导致CMV再激活的风险高。 CMV-特异性T细胞免疫的重构与对CMV的控制和保护有关。预期监测CMV-特异性CMI监测CMV-特异性CMI在儿科HSCT患者中预测CMV病毒血症的疗效试验。来自3 / 2010-6 / 2012的三十七个儿科同质的HSCT接受者。通过每周实时PCR检测CMV病毒血症。在移植后,在移植后30,90,180,270和360℃下进行预传递,早期进行预移植。 CMV病毒血症的发生率为51%(19/37),在移植后≤30天内的一半发作。十五名患者表现出CMV-特异性免疫(平均82天)。开发CMV-特异性免疫的患者CMV重新激活的累积发生率低于未(15%Vs 53%; P?= 023)。 ROC统计分析表明,预测病毒血症的AUC为0.725,用于量体 - CMV试验。在这种队列中,QuantiFeron-CMV测定是一种有价值的方法,用于鉴定CMV病毒血症的高风险的儿科HSCT患者,表明移植后个性化患者管理的潜在临床效用。

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