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移植前丙型肝炎病毒准种可能预测肝移植后的结局。

Pretransplantation hepatitis C virus quasispecies may be predictive of outcome after liver transplantation.

作者信息

Pelletier S J, Raymond D P, Crabtree T D, Iezzoni J C, Sawyer R G, Hahn Y S, Pruett T L

机构信息

Charles O. Strickler Transplant Center, University of Virginia Health Sciences Center, Charlottesville, VA, USA.

出版信息

Hepatology. 2000 Aug;32(2):375-81. doi: 10.1053/jhep.2000.9089.

Abstract

The evolution of hepatitis C virus (HCV) envelope variation was studied using a liver-transplant model to evaluate the role of HCV quasispecies for hepatocyte infection. Twelve HCV polymerase chain reaction (PCR)-positive liver-transplant recipients (6 with posttransplantation biochemical hepatitis and 6 without hepatitis [controls]) were prospectively evaluated and underwent detailed quasispecies analysis of pre- and postoperative serum samples. HCV amino acid sequence diversity and complexity at the first hypervariable region (HVR1) of the second envelope protein (E2) was correlated with outcome. Recurrence of HCV-induced allograft injury was defined by persistently elevated serum alanine transaminase (ALT) levels. The major variant (sequences >10% of all clones) of recipients with hepatitis accounted for a significantly smaller percent of all preoperative clones compared with controls (41% +/- 6% vs. 69% +/- 8%; P <.015). Recipients with hepatitis had an increased number of pretransplantation major variants (2.5 +/- 0.3 vs. 1.1 +/- 0.2; P <.006). Eighty-three percent of controls had a predominant variant (accounting for >50% of clones) compared with 17% of those with recurrence (P <.05). These differences did not persist postoperatively. In addition, recipients without a pretransplantation predominant variant demonstrated an increased allograft fibrosis score (2.3 +/- 0.3 vs. 0.5 +/- 0.3; P <.015) at 181 to 360 days posttransplantation compared with those in whom a predominant variant was present. Increased HCV envelope complexity may act as a stronger antigenic stimulus or improve hepatocyte receptor binding and lead to allograft hepatitis and fibrosis. Although pretransplantation differences in HCV quasispecies did not persist postoperatively, pretransplantation quasispecies may be a predictor of HCV-induced hepatitis and graft fibrosis after liver transplantation.

摘要

利用肝移植模型研究丙型肝炎病毒(HCV)包膜变异的演变,以评估HCV准种在肝细胞感染中的作用。对12例HCV聚合酶链反应(PCR)阳性的肝移植受者(6例发生移植后生化性肝炎,6例未发生肝炎[对照组])进行前瞻性评估,并对术前和术后血清样本进行详细的准种分析。将第二包膜蛋白(E2)的第一个高变区(HVR1)的HCV氨基酸序列多样性和复杂性与结局相关联。HCV诱导的移植肝损伤复发定义为血清丙氨酸转氨酶(ALT)水平持续升高。与对照组相比,发生肝炎的受者的主要变异株(序列占所有克隆的10%以上)在所有术前克隆中所占百分比显著更小(41%±6%对69%±8%;P<.015)。发生肝炎的受者移植前主要变异株数量增加(2.5±0.3对1.1±0.2;P<.006)。83%的对照组有一个优势变异株(占克隆的50%以上),而复发者中这一比例为17%(P<.05)。这些差异在术后未持续存在。此外,与存在优势变异株的受者相比,移植前无优势变异株的受者在移植后181至360天的移植肝纤维化评分更高(2.3±0.3对0.5±0.3;P<.015)。HCV包膜复杂性增加可能作为更强的抗原刺激或改善肝细胞受体结合,并导致移植肝肝炎和纤维化。虽然HCV准种的移植前差异在术后未持续存在,但移植前准种可能是肝移植后HCV诱导的肝炎和移植肝纤维化的一个预测指标。

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