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Biomarkers of disease differentiation: HCV recurrence versus acute cellular rejection

机译:疾病分化的生物标志物:HCV复发与急性细胞排斥

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摘要

The wound-healing process induced by chronic hepatitis C virus (HCV) infection triggers liver damage characterized by fibrosis development and finally cirrhosis. Liver Transplantation (LT) is the optimal surgical treatment for HCV-cirrhotic patients at end-stage liver disease. However, acute cellular rejection (ACR) and HCV recurrence disease represent two devastating complications post-LT. The accurate differential diagnosis between both conditions is critical for treatment choice, and similar histological features represent a challenge for pathologists. Moreover, the HCV recurrence disease severity is highly variable post-LT. HCV recurrence disease progression is characterized by an accelerated fibrogenesis process, and almost 30% of those patients develop cirrhosis at 5-years of follow-up. Whole-genome gene expression (WGE) analyses through well-defined oligonucleotide microarray platforms represent a powerful tool for the molecular characterization of biological process. In the present manuscript, the utility of microarray technology is applied for the ACR and HCV-recurrence biological characterization in post-LT liver biopsy samples. Moreover, WGE analysis was performed to identify predictive biomarkers of HCV recurrence severity in formalin-fixed paraffin-embedded liver biopsies prospectively collected.
机译:慢性丙型肝炎病毒(HCV)感染引起的伤口愈合过程触发了以纤维化发展为特征的肝损伤,最终导致肝硬化。肝移植(LT)是HCV肝硬化末期肝病患者的最佳手术治疗方法。然而,急性细胞排斥(ACR)和HCV复发性疾病代表LT后的两种破坏性并发症。两种情况之间的准确鉴别诊断对于治疗选择至关重要,并且相似的组织学特征对病理学家提出了挑战。此外,HCV复发疾病的严重程度在LT后变化很大。 HCV复发性疾病进展的特征是纤维化过程加快,并且其中近30%的患者在随访5年后发展为肝硬化。通过定义明确的寡核苷酸微阵列平台进行的全基因组基因表达(WGE)分析代表了生物学过程分子表征的强大工具。在本手稿中,微阵列技术的实用性用于LT后肝活检样本中的ACR和HCV复发生物学表征。此外,进行了WGE分析,以鉴定前瞻性收集的福尔马林固定石蜡包埋的肝活检组织中HCV复发严重程度的预测性生物标志物。

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