Overexpression of Regulatory T Cells Type 1 (Tr1) Specific Markers in a Patient with HCV-Induced Hepatocellular Carcinoma.

ISRN hepatology Pub Date : 2013-10-23 eCollection Date: 2013-01-01 DOI:10.1155/2013/928485
Laurissa Ouaguia, Olivier Morales, Dhafer Mrizak, Khaldoun Ghazal, Emmanuel Boleslawski, Claude Auriault, Véronique Pancré, Yvan de Launoit, Filoména Conti, Nadira Delhem
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引用次数: 7

Abstract

Hepatitis C virus (HCV) is an important causative agent of liver disease, but factors that determine the resolution or progression of infection are poorly understood. In this study, we suggested that existence of immunosuppressive mechanisms, supported by regulatory T cells and especially the regulatory T cell 1 subset (Tr1), may explain the impaired immune response during infection and thus the fibrosis aggravation to hepatocellular carcinoma (HCC). Using quantitative real-time PCR, we investigated the intra-hepatic presence of Tr1 cells in biopsies from a genotype 1b infected patient followed for an 18-year period from cirrhosis to HCC. We described a significant increase of gene expression in particular for the cytokines IL-10, TGF-β, and their receptors that were perfectly correlated with an increased expression of the Tr1 specific markers (combined expression of CD4, CD18, and CD49b). This was strongly marked since the patient evolved in the pathology and could explain the failure of the treatment. In conclusion, evidence of regulatory T cell installation in the liver of chronically infected patient with cirrhosis and HCC suggests for the first time a key role for these cells in the course of HCV infection.

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调节性T细胞1型(Tr1)特异性标志物在hcv诱导的肝细胞癌患者中的过表达
丙型肝炎病毒(HCV)是肝脏疾病的重要病原体,但决定感染消退或进展的因素尚不清楚。在本研究中,我们认为,在调节性T细胞,特别是调节性T细胞1亚群(Tr1)的支持下,免疫抑制机制的存在可能解释了感染期间免疫反应受损,从而导致肝细胞癌(HCC)纤维化加重。利用实时定量PCR技术,我们研究了一名基因型1b感染患者肝组织活检中Tr1细胞的存在,该患者从肝硬化到HCC随访了18年。我们描述了基因表达的显著增加,特别是细胞因子IL-10、TGF-β及其受体,它们与Tr1特异性标记物(CD4、CD18和CD49b的联合表达)的表达增加完全相关。自从病人在病理上进化以来,这是明显的,可以解释治疗的失败。总之,调节性T细胞在肝硬化和HCC慢性感染患者的肝脏中安装的证据首次表明这些细胞在HCV感染过程中起关键作用。
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