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Profiles of Serum Cytokines in Acute Drug-Induced Liver Injury and Their Prognostic Significance

机译:急性药物性肝损伤中血清细胞因子的变化及其预后意义

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摘要

Drug-induced liver injury (DILI) is the most common cause of acute liver failure in the United-States. The aim of the study was to describe serum immune profiles associated with acute DILI, to investigate whether there are profiles associated with clinical features or types of DILI and/or with prognosis, and to assess temporal changes in levels. Twenty-seven immune analytes were measured in the sera of 78 DILI subjects in the Drug-Induced Liver Injury Network (DILIN) and compared with 40 healthy controls. Immune analytes (14 cytokines, 7 chemokines and 6 growth factors) were measured by BioPlex multiplex ELISA at DILI onset and after 6 months. A modeling process utilizing immune principles was used to select a final set of variables among 27 immune analytes and several additional clinical lab values for prediction of early death (within 6 months of DILI onset). Nineteen of the 27 immune analytes were differentially expressed among healthy control, DILI onset and 6-month cohorts. Disparate patterns of immune responses, especially innate and adaptive cellular (mostly TH17) immunity were evident. Low values of four immune analytes (IL-9, IL-17, PDGF-bb and RANTES) and serum albumin are predictive of early death [PPV = 88% (95% CI, 65%-100%), NPV = 97% (95% CI, 93%-100%), accuracy = 96% (95% CI, 92%-100%)]. ConclusionsAcute DILI is associated with robust and varying immune responses. High levels of expression of cytokines associated with innate immunity are associated with a poor prognosis, whereas high levels of expression of adaptive cytokines are associated with good long-term prognosis and eventual recovery. Serum immune analyte profiles at DILI onset appear to be of prognostic, and perhaps, diagnostic significance.
机译:在美国,药物性肝损伤(DILI)是急性肝衰竭的最常见原因。该研究的目的是描述与急性DILI相关的血清免疫谱,研究是否存在与DILI的临床特征或类型和/或预后相关的谱,并评估水平的暂时变化。在药物诱发的肝损伤网络(DILIN)的78位DILI受试者的血清中测量了27种免疫分析物,并与40名健康对照进行了比较。免疫分析物(14种细胞因子,7种趋化因子和6种生长因子)通过BioPlex多重ELISA在DILI发作时和6个月后进行测量。利用免疫原理的建模过程用于从27种免疫分析物中选择最后一组变量,并选择多个其他临床实验室值来预测早期死亡(DILI发作6个月内)。 27种免疫分析物中有19种在健康对照,DILI发作和6个月队列中差异表达。明显不同的免疫反应模式,尤其是先天性和适应性细胞(主要是TH17)免疫。四种免疫分析物(IL-9,IL-17,PDGF-bb和RANTES)和血清白蛋白的低值可预测早期死亡[PPV = 88%(95%CI,65%-100%),NPV = 97% (95%CI,93%-100%),准确度= 96%(95%CI,92%-100%)]。结论急性DILI与强大而多样的免疫反应有关。与先天免疫相关的细胞因子高水平表达与不良预后相关,而适应性细胞因子高水平表达与长期预后及最终恢复相关。 DILI发作时的血清免疫分析物谱似乎具有预后性,并且可能具有诊断意义。

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