肾移植后极早期巨细胞病毒感染:单中心20年观察。

Q1 Medicine Virology: Research and Treatment Pub Date : 2019-04-02 eCollection Date: 2019-01-01 DOI:10.1177/1178122X19840371
M R Jorgenson, J L Descourouez, B C Astor, J A Smith, F Aziz, R R Redfield, D A Mandelbrot
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引用次数: 7

摘要

背景:移植后第一个月巨细胞病毒(CMV)感染的风险很小;然而,流行病学尚未进行专门调查,特别是在现代有效的免疫抑制方案和普遍的巨细胞病毒预防。目的:本研究的目的是描述移植后30天内发生巨细胞病毒的发生率和相关危险因素,并评估早期巨细胞病毒对预后的影响。方法:回顾性、单中心研究1994年1月1日至2014年12月31日成人肾移植(RTX)受者。结果:在研究期间,共有5225例接受肾移植的患者在移植后不到30天内出现巨细胞病毒感染。其中,只有14例患者表现出这一发现,总发病率为0.27%。这些患者中有一半被认为是高风险的,因为他们是非原发性移植的接受者或长期免疫抑制。剩下的7名患者没有已知的早期巨细胞病毒危险因素进行评估。本组从移植到巨细胞病毒感染的时间为13.5±7天。大多数(57.1%,n = 4)是高危血清状态(CMV D+/R-),发生在缬更昔洛韦时代(71.4%,n = 5)。淋巴细胞消耗诱导为主(57.1%,n = 4)。平均冷缺血时间(CIT) 19.7±7.7小时。3例出现术后并发症,2例因出血需开腹探查。在评估结果时,43% (n = 3)的患者随后出现巨细胞病毒感染,28.6% (n = 2)出现排斥反应,28.6% (n = 2)死亡。移植后小于30天的巨细胞病毒感染患者和大于30天的巨细胞病毒感染患者的结局无显著差异。结论:在我们对5000多例肾移植的回顾中,肾移植后前30天巨细胞病毒感染的发生率为0.2%。值得注意的常见患者特征包括出血需要再次手术和CIT延长。移植后超过30天发生CMV的结果与CMV相似。这项研究应该为临床医生提供一些保证;尽管有效的免疫抑制治疗,巨细胞病毒感染在头30天是不可能的。
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Very Early Cytomegalovirus Infection After Renal Transplantation: A Single-Center 20-Year Perspective.

Background: Cytomegalovirus (CMV) infection risk in the first month after transplantation is felt to be minimal; however, the epidemiology has not been specifically investigated, particularly in the modern era of potent immunosuppressive regimens and universal CMV prophylaxis.

Objective: The aim of this study was to describe the incidence of and risk factors associated with CMV occurring less than 30 days after transplant and evaluate the effect of very early CMV on outcomes.

Methods: Retrospective, single-center study of adult renal transplant (RTX) recipients between January 1, 1994 and December 31, 2014.

Results: A total of 5225 patients who received a renal transplant in the study time period were reviewed for the presence of CMV infection occurring less than 30 days after transplant. Of these, only 14 patients demonstrated this finding for an overall incidence of 0.27%. Half of these patients were considered to be at heightened risk due to being a recipient of a non-primary transplant or on chronic immunosuppression. This left seven patients without known risk factors for very early CMV to evaluate. In this group, time from transplant to CMV infection was 13.5 ± 7 days. The majority (57.1%, n = 4) were high-risk serostatus (CMV D+/R-) and occurred in the valganciclovir era (71.4%, n = 5). Lymphocyte-depleting induction predominated (57.1%, n = 4). Average cold ischemic time (CIT) was 19.7 ± 7.7 hours. Three patients had post-operative complications, two required exploratory-laparotomy for hemorrhage. When evaluating outcomes, 43% (n = 3) had subsequent episodes of CMV infection, 28.6% (n = 2) developed rejection, and 28.6% (n = 2) died. Outcomes between patients with CMV infection less than 30 days and those with CMV infection more than 30 days after transplant were not significantly different.

Conclusions: In our review of over 5000 kidney transplants, the incidence of CMV infection in the first 30 days after renal transplant is 0.2%. Notable common patient characteristics include hemorrhage requiring re-operation and prolonged CIT. Outcomes were similar to CMV occurring more than 30 days after transplant. This study should provide the clinician with some reassurance; despite potent immunosuppressive therapy, CMV infection in the first 30 days is unlikely.

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Virology: Research and Treatment
Virology: Research and Treatment Medicine-Infectious Diseases
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