一种蛋白质组学策略,用于识别脂肪性肝病患者中肝硬化和肝细胞癌的新型血清生物标志物。
A proteomic strategy to identify novel serum biomarkers for liver cirrhosis and hepatocellular cancer in individuals with fatty liver disease.
作者信息
Gray Joe, Chattopadhyay Dipankar, Beale Gary S, Patman Gillian L, Miele Luca, King Barry P, Stewart Stephen, Hudson Mark, Day Christopher P, Manas Derek M, Reeves Helen L
机构信息
Northern Institute for Cancer Research, The Medical School, Newcastle University, Newcastle-upon-Tyne, UK.
出版信息
BMC Cancer. 2009 Aug 5;9:271. doi: 10.1186/1471-2407-9-271.
BACKGROUND
Non-alcoholic fatty liver disease (NAFLD) has a prevalence of over 20% in Western societies. Affected individuals are at risk of developing both cirrhosis and hepatocellular cancer (HCC). Presently there is no cost effective population based means of identifying cirrhotic individuals and even if there were, our ability to perform HCC surveillance in the at risk group is inadequate. We have performed a pilot proteomic study to assess this as a strategy for serum biomarker detection.
METHODS
2D Gel electrophoresis was performed on immune depleted sera from 3 groups of patients, namely those with (1) pre-cirrhotic NAFLD (2) cirrhotic NAFLD and (3) cirrhotic NAFLD with co-existing HCC. Five spots differentiating at least one of these three groups were characterised by mass spectroscopy. An ELISA assay was optimised and a cross sectional study assessing one of these serum spots was performed on serum from 45 patients with steatohepatitis related cirrhosis and HCC and compared to 77 patients with histologically staged steatohepatitis.
RESULTS
Four of the spots identified were apolipoprotein isoforms, the pattern of which was able to differentiate the three groups. The 5th spot, seen in the serum of cirrhotic individuals and more markedly in those with HCC, was identified as CD5 antigen like (CD5L). By ELISA assay, although CD5L was markedly elevated in a number of cirrhotic individuals with HCC, its overall ability to distinguish non-cancer from cancer individuals as determined by AUC ROC analysis was poor. However, serum CD5L was dramatically increased, independently of age, sex, and the presence of necroinflammation, in the serum of individuals with NAFLD cirrhosis relative to those with pre-cirrhotic disease.
CONCLUSION
This novel proteomic strategy has identified a number of candidate biomarkers which may have benefit in the surveillance and diagnosis of individuals with chronic liver disease and/or HCC.
背景
非酒精性脂肪性肝病(NAFLD)在西方社会的患病率超过20%。受影响的个体有发生肝硬化和肝细胞癌(HCC)的风险。目前,尚无基于人群的经济有效的方法来识别肝硬化个体,即便有这样的方法,我们在高危人群中进行HCC监测的能力也不足。我们开展了一项蛋白质组学初步研究,以评估其作为血清生物标志物检测策略的可行性。
方法
对3组患者的免疫去除血清进行二维凝胶电泳,这3组患者分别为:(1)肝硬化前NAFLD患者;(2)肝硬化NAFLD患者;(3)合并HCC的肝硬化NAFLD患者。通过质谱分析对区分这三组中至少一组的5个蛋白点进行了表征。优化了酶联免疫吸附测定(ELISA)法,并对45例脂肪性肝炎相关肝硬化和HCC患者的血清进行了横断面研究,评估其中一个血清蛋白点,并与77例组织学分期的脂肪性肝炎患者进行比较。
结果
鉴定出的4个蛋白点为载脂蛋白异构体,其模式能够区分这三组。第5个蛋白点在肝硬化个体血清中可见,在HCC患者中更为明显,被鉴定为CD5抗原样蛋白(CD5L)。通过ELISA法检测,虽然CD5L在许多合并HCC的肝硬化个体中显著升高,但根据曲线下面积(AUC)ROC分析,其区分非癌症个体与癌症个体的总体能力较差。然而,相对于肝硬化前疾病患者,NAFLD肝硬化患者血清中的CD5L显著升高,且与年龄、性别和坏死性炎症的存在无关。
结论
这种新的蛋白质组学策略已鉴定出一些候选生物标志物,这些生物标志物可能有助于慢性肝病和/或HCC患者的监测和诊断。
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