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与肝移植受者丙型肝炎及早期纤维化进展相关的基因表达模式。

Gene expression patterns that correlate with hepatitis C and early progression to fibrosis in liver transplant recipients.

作者信息

Smith Maria W, Walters Kathie-Anne, Korth Marcus J, Fitzgibbon Matthew, Proll Sean, Thompson Jill C, Yeh Matthew M, Shuhart Margaret C, Furlong Jeffrey C, Cox Paula P, Thomas David L, Phillips John D, Kushner James P, Fausto Nelson, Carithers Robert L, Katze Michael G

机构信息

Department of Microbiology, School of Medicine, University of Washington, Seattle, Washington 98195-8070, USA.

出版信息

Gastroenterology. 2006 Jan;130(1):179-87. doi: 10.1053/j.gastro.2005.08.015.

Abstract

BACKGROUND & AIMS: Liver transplant recipients infected with hepatitis C virus (HCV) develop recurrent hepatitis soon after transplantation and, in some cases, progress to fibrosis within the first 2 years. Our goals were to identify molecular processes influencing the liver disease progression and to find potential gene markers of early fibrosis.

METHODS

We performed gene expression profiling on serial liver biopsy specimens obtained from 13 (11 infected and 2 uninfected) transplant recipients within the first year after transplantation at 0, 3, 6, and 12 months. The data were compared with clinical observations and with a gene expression database obtained for 55 nontransplant HCV-infected and uninfected liver samples.

RESULTS

We identified several specific gene expression patterns. The first pattern was unique for the transplant recipients regardless of their infection status. The corresponding genes encoded stress response proteins and blood proteins involved in coagulation that were differentially expressed in response to posttransplantation graft recovery. The second pattern was specific to HCV-infected samples and included up-regulation of genes encoding components of the interferon-mediated antiviral response and immune system (antigen presentation, cytotoxic response). This up-regulation pattern was absent or suppressed in the patients who developed early fibrosis, indicating that the disease progression might result from an impaired liver response to infection. Finally, we identified gene expression patterns that were specific for 12-month biopsy specimens in all 4 HCV-infected patients who developed early fibrosis.

CONCLUSIONS

The identified gene expression patterns may prove useful for diagnostic and prognostic applications in HCV-infected patients, including predicting early progression to fibrosis.

摘要

背景与目的

丙型肝炎病毒(HCV)感染的肝移植受者在移植后不久就会发生复发性肝炎,在某些情况下,会在头2年内进展为纤维化。我们的目标是确定影响肝病进展的分子过程,并寻找早期纤维化的潜在基因标志物。

方法

我们对13名(11名感染HCV和2名未感染HCV)移植受者在移植后第1年的0、3、6和12个月时获取的系列肝脏活检标本进行基因表达谱分析。将这些数据与临床观察结果以及从55份非移植的HCV感染和未感染肝脏样本中获得的基因表达数据库进行比较。

结果

我们确定了几种特定的基因表达模式。第一种模式对于移植受者是独特的,无论其感染状态如何。相应的基因编码应激反应蛋白和参与凝血的血液蛋白,它们在移植后移植物恢复过程中差异表达。第二种模式特定于HCV感染的样本,包括编码干扰素介导的抗病毒反应和免疫系统(抗原呈递、细胞毒性反应)成分的基因上调。在发生早期纤维化的患者中,这种上调模式不存在或受到抑制,表明疾病进展可能是由于肝脏对感染的反应受损所致。最后,我们确定了在所有4名发生早期纤维化的HCV感染患者中,12个月活检标本特有的基因表达模式。

结论

所确定的基因表达模式可能在HCV感染患者的诊断和预后应用中证明有用,包括预测早期纤维化进展。

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