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肝细胞癌中内质网蛋白的裂解:患者血清中生成片段的检测

Cleavage of endoplasmic reticulum proteins in hepatocellular carcinoma: Detection of generated fragments in patient sera.

作者信息

Chignard Nicolas, Shang Sufen, Wang Hong, Marrero Jorge, Bréchot Christian, Hanash Samir, Beretta Laura

机构信息

Department of Microbiology and Immunology, University of Michigan Medical School, Ann Arbor, Michigan, USA.

出版信息

Gastroenterology. 2006 Jun;130(7):2010-22. doi: 10.1053/j.gastro.2006.02.058.

Abstract

BACKGROUND & AIMS: In the past decade, there has been a rising incidence of hepatocellular carcinoma (HCC) and a progressive increase in HCC-related mortality in the United States and Western Europe. The poor survival of patients with HCC is largely related to the lack of reliable tools for early diagnosis.

METHODS

We have applied proteomics tools to the comparative analysis of protein profiles between HCC and adjacent nontumor tissues as a means for discovering novel molecular markers.

RESULTS

Forty-seven protein spots that showed reproducible variation were identified by mass spectrometry, corresponding to 23 distinct genes. A positive correlation between transcript and protein level variations was observed for only 7 out of the 23 genes. Proteolytic cleavage accounted for the discrepancies between messenger RNA and protein level changes for 7 genes including calreticulin, PDIA3, PDI, and GRP78. We detected a fragment of each of these 4 endoplasmic reticulum proteins in the culture supernatant of the PLC-PRF5 hepatoma cell line, suggesting that their cleavage leads to release of selected cleaved products in the extracellular compartment. We also detected calreticulin and PDIA3 cleavage products in sera of patients with HCC. A statistically highly significant difference in calreticulin and PDIA3 fragment serum levels between patients with HCC and healthy individuals was observed. Amounts of calreticulin and PDIA3 fragments were also significantly different between patients with HCC and at-risk patients (patients with chronic hepatitis or cirrhosis).

CONCLUSIONS

Specific isoforms in general and cleavage products in particular should therefore be further evaluated as new markers for HCC.

摘要

背景与目的

在过去十年中,美国和西欧肝细胞癌(HCC)的发病率不断上升,且HCC相关死亡率持续增加。HCC患者生存率低很大程度上与缺乏可靠的早期诊断工具有关。

方法

我们应用蛋白质组学工具对HCC组织和相邻非肿瘤组织的蛋白质谱进行比较分析,以发现新的分子标志物。

结果

通过质谱鉴定出47个显示出可重复变化的蛋白质斑点,对应23个不同的基因。23个基因中只有7个观察到转录本和蛋白质水平变化之间存在正相关。蛋白水解切割解释了包括钙网蛋白、PDIA3、PDI和GRP78在内的7个基因在信使RNA和蛋白质水平变化之间的差异。我们在PLC-PRF5肝癌细胞系的培养上清液中检测到这4种内质网蛋白各自的一个片段,表明它们的切割导致特定切割产物释放到细胞外区室。我们还在HCC患者血清中检测到钙网蛋白和PDIA3的切割产物。观察到HCC患者与健康个体之间钙网蛋白和PDIA3片段血清水平存在统计学上的高度显著差异。HCC患者与高危患者(慢性肝炎或肝硬化患者)之间钙网蛋白和PDIA3片段的量也存在显著差异。

结论

因此,一般的特定异构体尤其是切割产物应作为HCC的新标志物进一步评估。

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