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人疱疹病毒6相关的纯红细胞再生障碍、继发性移植物失败以及异基因造血细胞移植后临床严重免疫抑制经膦甲酸钠成功治疗。

Human herpesvirus 6-related pure red cell aplasia, secondary graft failure, and clinical severe immune suppression after allogeneic hematopoietic cell transplantation successfully treated with foscarnet.

作者信息

Lagadinou E D, Marangos M, Liga M, Panos G, Tzouvara E, Dimitroulia E, Tiniakou M, Tsakris A, Zoumbos N, Spyridonidis A

机构信息

Department of Internal Medicine, Patras University Medical Center, Rio/Patras, Greece.

出版信息

Transpl Infect Dis. 2010 Oct;12(5):437-40. doi: 10.1111/j.1399-3062.2010.00515.x.

Abstract

Human herpesvirus 6 (HHV-6) is frequently detected after allogeneic hematopoietic cell transplantation (allo-HCT); however, the clinical interpretation of HHV-6 viremia in a transplant patient is challenging as it may signify asymptomatic reactivation, chromosomal integration of the virus genome in the donor or recipient with no clinical significance, or severe HHV-6 disease. Here we present a case of HHV-6 disease after allo-HCT presenting as pure red cell aplasia, secondary graft failure, and severe immunosuppression causing multiple severe bacterial super-infections. Examination of pre-transplant patient and donor samples as well as serial determination of HHV-6 DNA copy numbers after transplantation were necessary to definitively interpret HHV-6 viremia as active HHV-6 infection with a causative role in pancytopenia and immune suppression. Foscarnet treatment resulted both in viral load decline and disappearance of HHV-6-related bone marrow suppression and predisposition to severe infections. Clinicians should be aware of the wide array of clinical manifestations and the diagnostic pitfalls of post-transplant HHV-6 disease. These issues are extremely challenging, as they may result either in dangerous underestimation of HHV-6 disease or in the institution of unnecessary antiviral therapy. Late bone marrow aplasia and late severe infections after allo-HCT without other obvious causes may be HHV-6 related.

摘要

人疱疹病毒6型(HHV-6)在异基因造血细胞移植(allo-HCT)后经常被检测到;然而,对移植患者中HHV-6病毒血症的临床解读具有挑战性,因为它可能意味着无症状再激活、病毒基因组在供体或受体中的染色体整合(无临床意义),或严重的HHV-6疾病。在此,我们报告1例allo-HCT后发生HHV-6疾病的病例,表现为纯红细胞再生障碍、继发性移植物功能衰竭以及导致多次严重细菌重叠感染的严重免疫抑制。检查移植前患者和供体样本以及移植后连续测定HHV-6 DNA拷贝数对于明确将HHV-6病毒血症解读为活动性HHV-6感染并确定其在全血细胞减少和免疫抑制中的致病作用是必要的。膦甲酸钠治疗导致病毒载量下降以及HHV-6相关的骨髓抑制消失和严重感染易感性降低。临床医生应意识到移植后HHV-6疾病的广泛临床表现和诊断陷阱。这些问题极具挑战性,因为它们可能导致对HHV-6疾病的危险低估或不必要的抗病毒治疗。allo-HCT后无其他明显原因的晚期骨髓再生障碍和晚期严重感染可能与HHV-6有关。

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