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肝纤维化的分子血清标志物

Molecular serum markers of liver fibrosis.

作者信息

Liu Tianhui, Wang Xiaoming, Karsdal Morten A, Leeming Diana J, Genovese Federica

机构信息

Liver Research Center, Beijing Friendship Hospital, Capital Medical University, Beijing, China.

出版信息

Biomark Insights. 2012;7:105-17. doi: 10.4137/BMI.S10009. Epub 2012 Jul 23.

Abstract

Fibrosis is a hallmark histologic event of chronic liver diseases and is characterized by the excessive accumulation and reorganization of the extracellular matrix (ECM). The gold standard for assessment of fibrosis is liver biopsy. As this procedure has various limitations, including risk of patient injury and sampling error, a non-invasive serum marker for liver fibrosis is desirable. The increasing understanding of the pathogenesis of hepatic fibrosis has suggested several markers which could be useful indicators of hepatic fibrogenesis and fibrosis. These markers include serum markers of liver function, ECM synthesis, fibrolytic processes, ECM degradation and fibrogenesis related cytokines. Recently, neo-epitopes, which are post-translational modifications of proteins, have been successfully used in bone and cartilage diseases which are characterized by extensive ECM remodeling. Increasing numbers of studies are being undertaken to identify neo-epitopes generated during liver fibrosis, and which ultimately might be useful for diagnosing and monitoring fibrogenesis. To date, the metalloproteinases generated fragment of collagen I, III, IV and VI have been proven to be elevated in two rat models of fibrosis. This review summarizes the recent efforts that have been made to identify potentially reliable non-invasive serum markers. We used the recently proposed BIPED (Burden of disease, Investigative, Prognostic, Efficacy and Diagnostic) system to characterize potential serum markers and neo-epitope markers that have been identified to date.

摘要

肝纤维化是慢性肝病的标志性组织学事件,其特征是细胞外基质(ECM)过度积聚和重塑。评估肝纤维化的金标准是肝活检。由于该操作存在多种局限性,包括患者受伤风险和抽样误差,因此需要一种用于肝纤维化的非侵入性血清标志物。对肝纤维化发病机制的深入了解提示了几种可能作为肝纤维化发生和纤维化有用指标的标志物。这些标志物包括肝功能、ECM合成、纤溶过程、ECM降解和纤维化相关细胞因子的血清标志物。最近,新表位作为蛋白质的翻译后修饰,已成功应用于以广泛ECM重塑为特征的骨和软骨疾病。越来越多的研究致力于鉴定肝纤维化过程中产生的新表位,这些新表位最终可能有助于诊断和监测纤维化的发生。迄今为止,在两种肝纤维化大鼠模型中已证实,金属蛋白酶产生的I、III、IV和VI型胶原片段升高。本综述总结了最近为鉴定潜在可靠的非侵入性血清标志物所做的努力。我们使用最近提出的BIPED(疾病负担、研究、预后、疗效和诊断)系统来描述迄今为止已鉴定的潜在血清标志物和新表位标志物。

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