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首页> 外文期刊>Journal of Clinical Microbiology >Human Cytomegalovirus-Specific T-Cell Immune Reconstitution in Preemptively Treated Heart Transplant Recipients Identifies Subjects at Critical Risk for Infection
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Human Cytomegalovirus-Specific T-Cell Immune Reconstitution in Preemptively Treated Heart Transplant Recipients Identifies Subjects at Critical Risk for Infection

机译:在抢先治疗的心脏移植受者中人类巨细胞病毒特异的T细胞免疫重建确定了感染的关键风险受试者

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摘要

Human cytomegalovirus (CMV) infection represents a major threat for heart transplant recipients (HTXs). CMV-specific T cells effectively control virus infection, and thus, assessment of antiviral immune recovery may have clinical utility in identifying HTXs at risk of infection. In this study, 10 CMV-seropositive (R+) pretransplant patients and 48 preemptively treated R+ HTXs were examined before and after 100 days posttransplant. Preemptive treatment is supposed to favor the immune recovery. CMV DNAemia and gamma interferon enzyme-linked immunosorbent spot (ELISPOT) assay were employed to assess the viremia and immune reconstitution. HTXs could be categorized into three groups characterized by high (>100), medium (50 to 100), and low (<50) spot levels. Early-identified high responders efficiently controlled the infection and also maintained high immunity levels after 100 days after transplant. No episodes of grade ≥2R rejection occurred in the high responders. Midresponders were identified as a group with heterogeneous trends of immune reconstitution. Low responders were 41% and 21% of HTXs before and after 100 days posttransplant, respectively. Low responders were associated with a higher incidence of infection. The effect of viremia on immune recovery was investigated: a statistically significant inverse correlation between magnitude of viremia and immune recovery emerged; in particular, each 10-fold increase in viremia (>4 log10 DNAemia/ml) was associated with a 36% decrease of the ELISPOT assay spot levels. All episodes of high viremia (>4 log10 DNAemia/ml) occurred from 1 to 60 days after transplant. Thus, the concomitant evaluation of viremia and CMV immune reconstitution has clinical utility in identifying HTXs at risk of infection and may represent a helpful guide in making therapeutic choices.
机译:人巨细胞病毒(CMV)感染对心脏移植受者(HTX)构成了主要威胁。 CMV特异的T细胞可有效控制病毒感染,因此,抗病毒免疫恢复的评估可能在临床上具有识别感染风险的HTX的实用性。在这项研究中,我们对10例CMV血清阳性(R + )移植前患者和48例经抢先治疗的R + HTX进行了研究,研究的时间分别为移植后100天。抢先治疗应该有利于免疫恢复。使用CMV DNAemia和γ干扰素酶联免疫吸附斑点(ELISPOT)测定来评估病毒血症和免疫重建。 HTX可以分为三类,其特征是高(> 100),中(50至100)和低(<50)斑点水平。早期识别的高反应者可以有效控制感染,并且在移植后100天后仍保持高免疫力。在高应答者中没有发生≥2R级排斥反应的发作。中度应答者被确定为免疫重建趋势不同的人群。移植后100天之前和之后,低应答者分别为HTX的41%和21%。低反应者与较高的感染发生率相关。研究了病毒血症对免疫恢复的影响:出现了病毒血症程度与免疫恢复之间的统计学显着负相关;尤其是病毒血症每增加10倍(> 4 log 10 DNAemia / ml)与ELISPOT分析斑点水平降低36%有关。高病毒血症(> 4 log 10 DNAemia / ml)的所有发作均发生在移植后1至60天。因此,病毒血症和CMV免疫重建的伴随评估在临床上具有确定感染风险的HTX的临床效用,并可能在做出治疗选择方面提供有用的指导。

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