肺移植受者中更昔洛韦耐药巨细胞病毒感染与不良预后相关,尽管使用含膦甲酸酯的方案进行了治疗。
Ganciclovir-resistant cytomegalovirus infections among lung transplant recipients are associated with poor outcomes despite treatment with foscarnet-containing regimens.
机构信息
Division of Infectious Diseases, Department of Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.
出版信息
Antimicrob Agents Chemother. 2014;58(1):128-35. doi: 10.1128/AAC.00561-13. Epub 2013 Oct 21.
Ganciclovir-resistant cytomegalovirus (CMV) infections are reported infrequently among lung transplant recipients receiving extended valganciclovir prophylaxis. We performed a single-center, retrospective review of ganciclovir-resistant CMV infections in a program that employed valganciclovir prophylaxis for ≥6 months after lung transplant. CMV infections were diagnosed in 28% (170/607) of patients. UL97 mutations were detected in 9.4% (16/170) of CMV-infected patients at a median of 8.5 months posttransplant (range, 5 to 21) and despite prophylaxis for a median of 7 months (range, 4 to 21). UL97 mutations were canonical; 25% (4/16) of strains carried concurrent UL54 mutations. Ganciclovir-resistant CMV was more likely with breakthrough infections (75% [12/16] versus 19% [30/154]; P = 0.00001) and donor positive/recipient negative (D+/R-) serostatus (75% versus 45% [69/154]; P = 0.03). The median whole-blood CMV load was 4.13 log10 copies/cm(3) (range, 2.54 to 5.53), and 93% (14/15) of patients had low-moderate immune responses (Cylex Immunoknow). Antiviral therapy was successful, failed, or eradicated viremia followed by relapse in 12% (2/16), 31% (5/16), and 56% (9/16) of patients, respectively. Eighty-seven percent (14/16) of patients were treated with foscarnet-containing regimens; toxicity developed in 78% (11/14) of these. Median viral load half-life and time to viremia eradication among foscarnet-treated patients were 2.6 and 23 days, respectively, and did not correlate with protection from relapse. Sixty-nine percent (11/16) of patients developed CMV pneumonitis, and 25% (4/16) died of it. Serum viral load was independently associated with death among foscarnet-treated patients (P = 0.04). In conclusion, ganciclovir-resistant CMV infections remained a major cause of morbidity and mortality following lung transplantation. Foscarnet-based regimens often eradicated viremia rapidly but were ineffective in the long term and limited by toxicity.
更昔洛韦耐药的巨细胞病毒 (CMV) 感染在接受更昔洛韦延长预防的肺移植受者中罕见。我们对一个采用更昔洛韦预防治疗 6 个月以上的肺移植项目中更昔洛韦耐药的 CMV 感染进行了单中心回顾性研究。在 607 例患者中,28%(170/607)诊断为 CMV 感染。在移植后中位时间 8.5 个月(范围 5 至 21)时,检测到 9.4%(16/170)CMV 感染患者存在 UL97 突变,尽管中位时间预防治疗 7 个月(范围 4 至 21)。UL97 突变是典型的;25%(4/16)株同时携带 UL54 突变。突破性感染更易发生更昔洛韦耐药 CMV(75%[12/16]与 19%[30/154];P=0.00001)和供体阳性/受体阴性(D+/R-)血清状态(75%与 45%[69/154];P=0.03)。全血 CMV 负荷中位数为 4.13 log10 拷贝/cm3(范围 2.54 至 5.53),93%(14/15)患者有低中度免疫应答(Cylex Immunoknow)。抗病毒治疗成功、失败或清除病毒血症后复发分别占 12%(2/16)、31%(5/16)和 56%(9/16)的患者。87%(14/16)的患者接受含膦甲酸酯的治疗方案;14 例中有 78%(11/14)出现毒性。膦甲酸酯治疗患者的病毒载量半衰期和病毒血症清除时间中位数分别为 2.6 天和 23 天,与预防复发无关。69%(11/16)的患者发生 CMV 肺炎,25%(4/16)死于 CMV 肺炎。血清病毒载量与接受膦甲酸酯治疗患者的死亡独立相关(P=0.04)。总之,肺移植后,更昔洛韦耐药的 CMV 感染仍然是发病率和死亡率的主要原因。基于膦甲酸酯的方案通常能迅速清除病毒血症,但长期效果不佳,且受毒性限制。
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