Fernández-Ruiz Mario, Nuévalos Marcos, Rodríguez-Goncer Isabel, García-Ríos Estéfani, Ruiz-Merlo Tamara, Redondo Natalia, Trujillo Hernando, González Esther, Polanco Natalia, Caso José María, Aparicio-Minguijón Eduardo, López-Medrano Francisco, San Juan Rafael, Andrés Amado, Pérez-Romero Pilar, Aguado José María
Unit of Infectious Diseases, Hospital Universitario "12 de Octubre", Instituto de Investigación Sanitaria Hospital "12 de Octubre" (imas12), Madrid, Spain.
Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Instituto de Salud Carlos III (ISCIII), Madrid, Spain.
Transpl Infect Dis. 2025 Jan 10:e14437. doi: 10.1111/tid.14437.
Kidney transplant (KT) recipients at intermediate risk for cytomegalovirus (CMV) infection constitute a potential target for individualized prevention strategies informed by the CMV-specific cell-mediated immunity (CMV-CMI). The optimal method for the functional assessment of CMV-CMI in this group remains unclear.
We included 74 CMV-seropositive KT recipients that did not receive T-cell-depleting induction and were managed by preemptive therapy. CMV-CMI was monitored at baseline and months 1, 3, 6, and 12 by intracellular cytokine staining (ICS) and a interferon (IFN)-γ-release assay (QuantiFERON-CMV [QTF-CMV]). Both methods were compared for discriminative capacity (areas under the receiving operating characteristic curve [auROCs]) and diagnostic accuracy to predict protection against high-level (≥1000 IU/mL) CMV DNAemia and/or disease.
Eighteen patients (24.3%) experienced high-level CMV DNAemia or disease. There were no significant differences in the discriminative capacity to predict protection of CMV-specific CD8+ (auROC: 0.719) and CD4+ T-cell counts (auROC: 0.664) enumerated by ICS and IFN-γ production measured by QTF-CMV (auROC: 0.666). Optimal cutoff values of ≥9.8 CMV-specific CD4+ T-cells/µL and ≥5.7 CD8+ T-cells/µL by ICS yielded excellent specificity (95.7% and 86.9%, respectively) and positive predictive values (PPVs) (>98.0%), but a sensitivity below 60%. A reactive QTF-CMV (IFN-γ ≥0.2 IU/mL) provided good sensitivity (81.6%) and PPV (92.5%), at the expense of a poor specificity (22.2%).
The discriminative capacity to predict immune protection against clinically relevant CMV infection among intermediate-risk KT recipients was comparable for ICS and QTF-CMV. A selected ICS threshold may provide better specificity than the interpretative cut-off values currently recommended for QTF-CMV.
巨细胞病毒(CMV)感染中风险的肾移植(KT)受者是基于CMV特异性细胞介导免疫(CMV-CMI)的个体化预防策略的潜在目标人群。该人群中CMV-CMI功能评估的最佳方法仍不明确。
我们纳入了74例未接受耗竭T细胞诱导治疗且采用抢先治疗的CMV血清学阳性KT受者。通过细胞内细胞因子染色(ICS)和干扰素(IFN)-γ释放试验(QuantiFERON-CMV [QTF-CMV])在基线以及第1、3、6和12个月监测CMV-CMI。比较两种方法的鉴别能力(受试者操作特征曲线下面积[auROCs])和预测预防高水平(≥1000 IU/mL)CMV病毒血症和/或疾病的诊断准确性。
18例患者(24.3%)发生了高水平CMV病毒血症或疾病。ICS计数的CMV特异性CD8 +(auROC:0.719)和CD4 + T细胞(auROC:0.664)以及QTF-CMV检测的IFN-γ产生量(auROC:0.666)在预测CMV保护方面的鉴别能力无显著差异。ICS检测CMV特异性CD4 + T细胞≥9.8个/µL和CD8 + T细胞≥5.7个/µL的最佳临界值具有出色的特异性(分别为95.7%和86.9%)和阳性预测值(PPV)(>98.0%),但敏感性低于60%。QTF-CMV反应性(IFN-γ≥0.2 IU/mL)具有良好的敏感性(81.6%)和PPV(92.5%),但特异性较差(22.2%)。
在中风险KT受者中,ICS和QTF-CMV预测针对临床相关CMV感染的免疫保护的鉴别能力相当。选定的ICS阈值可能比目前QTF-CMV推荐的解释性临界值具有更好的特异性。
