巨细胞病毒和HHV-6再激活对血液恶性肿瘤患者造血干细胞移植后早期病程的影响

T. V. Antonova, M. S. Nozhkin, О. Е. Pobegalova, О. V. Gorchakova, N. V. Sabadash, D. Lioznov
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摘要

目标。评估巨细胞病毒和HHV-6再激活对血液系统恶性肿瘤患者移植后早期病程的影响。材料。回顾性分析339例接受造血干细胞移植(HSCT)的恶性血液病患者的病历,检测巨细胞病毒(CMV)和HHV-6感染标志物(特异性IgG, EIA)。在移植后早期(最多100天)对HSCT受者的血液和其他材料进行病毒DNA检测(PCR)。结果。177例HSCT患者(52.2%)发现HSCT后病毒感染再激活:23%的HSCT患者检测到CMV感染,17.4%的HSCT患者检测到HHV-6, 11.6%的HSCT患者检测到CMV+HHV-6。CMV DNA主要在血液中发现,而HHV-6 DNA在GIT粘膜和骨髓中更常见。在99例HHV-6再激活的患者中,40%合并CMV+HHV-6再激活。在该组中,感染的临床表现明显更频繁。发热性中性粒细胞减少症在巨细胞病毒再激活的HSCT受者中更常见,败血症和移植物功能低下在HHV-6和主要是HHV-6+巨细胞病毒感染的情况下更常见。利用Spearman方法揭示了CMV和HHV-6再激活与白细胞生成恢复、移植期和移植功能低下之间的直接相关性。采用logistic回归分析证实疱疹病毒感染再激活对移植物功能减退和白细胞生成延迟恢复的影响;揭示了它对嵌合的影响。在72%的病例中,移植后早期移植失败发生在疱疹感染再激活的患者中。结论。HSCT术后早期HHV-6和巨细胞病毒的再激活与白细胞生成恢复相关,有助于并发症的发生,并且是加重移植后病程的另一个因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
An impact of CMV and HHV-6 reactivation on the course of early period after hematopoietic stem cell transplantation in patients with hematologic malignancies
   Objective. To assess the impact of CMV and HHV-6 reactivation on the course of early post-transplant period in patients with hematologic malignancies.   Materials. Retrospective analysis of medical records of 339 patients with hematologic malignancies who received hematopoietic stem cell transplantation (HSCT) was performed, and markers of CMV and HHV-6 infections were detected (specific IgG, EIA). Blood and other materials from HSCT recipients were tested (PCR) for viral DNA in early post-transplant period (up to Day 100).   Results. Reactivation of viral infections after HSCT was discovered in 177 patients (52,2 %): CMV-infection was detected in 23 %, HHV-6 in 17,4 %, CMV+HHV-6 in 11,6 % of HSCT recipients. CMV DNA was predominantly identified in blood, while HHV-6 DNA was more frequently discovered in GIT mucosa and bone marrow. 40 % of 99 patients with HHV-6 reactivation had concomitant CMV+HHV-6 reactivation. In this group, the clinical manifestation of infections was registered significantly more frequently. Febrile neutropenia was more frequent in HSCT recipients with CMV reactivation, sepsis and graft hypofunction were diagnosed more frequently in presence of HHV-6 and predominantly HHV-6+CMV infections. The direct correlation (using Spearman’s method) between CMV and HHV-6 reactivation and terms of leukopoiesis recovery, engraftment terms, and transplant hypofunction was revealed. An impact of herpetic infections reactivation on the graft hypofunction and late recovery of leukopoiesis was confirmed using the logistic regression; its impact on the chimerism was revealed. In 72 % of cases, the graft failure in early post-transplant period occurred in patients with herpetic infections reactivation.   Conclusion. HHV-6 and CMV reactivation in the early period after HSCT correlates with terms of leukopoiesis recovery, contributes to development of complications, and is an additional factor aggravating the course of the post-transplant period.
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