Serum GP73 and hepcidin levels are corelated with the prognosis of hepatitis B-related liver cancer patients

Abstract

Abstract: Objective To explore the changes of Golgi protein 73 (GP73) and hepcidin (Hepc) levels in the serum of hepatitis B-related liver cancer patients and their correlation with the patients’ prognosis. Methods Ninety-eight patients with hepatitis B-related liver cancer admitted between September 2017 to September 2018 were enrolled in this study as the research group. Ninety-two healthy examined people during the same time period were collected as the control group. Serum GP73 and Hepc levels were compared between the research and the control groups, and between the death and survival patients with hepatitis B-related liver cancer. Logistic regression analysis was performed to identify the risk factors affecting the patients’ survival. Receiver operating characteristic curve (ROC) was drawn for analyzing the efficacy of serum GP73 and Hepc levels in predicting the prognosis of patients with hepatitis B-related liver cancer. Results Serum GP73 and Hepc levels in the study group were (204.7±10.3) ng/mL and (128.3±12.6) μg/L, respectively, which were significantly higher than those in the control group [(38.1±6.7) ng/mL and (77.9±9.5) μg/ L, respectively] (P<0.05). After 2 years of follow-up, the mortality of patients with hepatitis B-related liver cancer was 28.4%. The serum GP73 and Hepc levels of dead patients were (261.6±12.7) ng/mL and (165.8±13.2) μg/L,respectively, which were significantly higher than those of surviving patients [(182.5±5.9) ng/mL and (113.1±10.4) μg/L, respectively] (P<0.05). Logistic multivariate analysis showed that TNM stage III-IV, high serum levels of GP73 and Hepc were all independent risk factors affecting the survival of patients with hepatitis B-related liver cancer (OR=2.570, 1.984, 2.121, all P<0.05). ROC analysis showed that the best cut-off points of serum GP73 and Hepc levels for predicting death of hepatitis B-related liver cancer patients were 25.3 ng/mL and 130.0 μg/L, respectively. The sensitivity were 70.4%, 88.9%, and the specificity were 89.7%, 72.1%, respectively. The area under the curve (AUC) were 0.887 (95%CI: 0.805~0.943) and 0.883 (95%CI: 0.801~0.940). Conclusion Serum GP73 and Hepc levels in patients with hepatitis B-related liver cancer are abnormally elevated. TNM stages III to IV, high levels of GP73 and Hepc are independent risk factors that affect the survival of patients with hepatitis B-related liver cancer.

Key words: Hepatitis B related liver cancer, Hepatitis B, Golgi protein 73, Hepcidin, Prognosis

CHEN Chao, YAO Ling, QIU Bang-dong, WANG Xiao-yan. Serum GP73 and hepcidin levels are corelated with the prognosis of hepatitis B-related liver cancer patients[J]. Chinese Hepatolgy, 2021, 26(9): 1007-1010.

References

[1] Gao Q, Zhu H, Dong L, et al. Integrated proteogenomic characterization of HBV-related hepatocellular carcinoma . Cell, 2019, 179:561-577.
[2] Lin CL, Kao JH. Review article: the prevention of hepatitis B-related hepatocellular carcinoma . Aliment Pharmacol Ther, 2018, 48:5-14.
[3] Zhou Z, Li Y, Hao H, et al. Screening hub genes as prognostic biomarkers of hepatocellular carcinoma by bioinformatics analysis . Cell Transplant, 2019, 28:76S-86S.
[4] Jiao C, Cui L, Piao J, et al. Clinical significance and expression of serum Golgi protein 73 in primary hepatocellular carcinoma . J Cancer Res Ther, 2018, 14:1239-1244.
[5] Ismail MM, Morsi HK, Abdulateef NA, et al. Evaluation of prothrombin induced by vitamin K absence, macrophage migration inhibitory factor and Golgi protein-73 versus alpha fetoprotein for hepatocellular carcinoma diagnosis and surveillance . Scand J Clin Lab Invest, 2017, 77:175-183.
[6] Udali S, Castagna A, Corbella M, et al. Hepcidin and DNA promoter methylation in hepatocellular carcinoma . Eur J Clin Invest, 2018, 48:128-136.
[7] 俞顺章, 穆丽娜. 乙型肝炎与肝癌. 天津: 天津科学技术出版社, 2015:92-95.
[8] Lim CJ, Lee YH, Pan L, et al. Multidimensional analyses reveal distinct immune microenvironment in hepatitis B virus-related hepatocellular carcinoma . Gut, 2019, 68:916-927.
[9] Kudo M, Ueshima K, Osaki Y, et al. B-mode ultrasonography versus contrast-enhanced ultrasonography for surveillance of hepatocellular carcinoma: a prospective multicenter randomized controlled trial . Liver Cancer, 2019, 8:271-280.
[10] Yanming L, Yue C, Wencan C, et al. Combined detection of AFP-L3, GP73 and TIP30 enhances diagnostic accuracy for HBV-related cirrhosis and hepatocellular carcinoma . J Pak Med Assoc, 2019, 69:1279-1286.
[11] 王钢, 陈涛, 卢峰, 等. 血清高尔基体糖蛋白73在慢性肝病诊断中的应用研究. 临床输血与检验, 2018, 20:97-100.
[12] 严舒, 岳飞利, 李勇, 等. 肝癌结节中Hepcidin、BMP6表达及铁含量与肝癌临床特征的相关性分析. 热带医学杂志, 2019, 19:1003-1007,1065.
[13] Gatselis NK, Tornai T, Shums Z, et al. Golgi protein-73: A biomarker for assessing cirrhosis and prognosis of liver disease patients . World J Gastroenterol, 2020, 26:5130-5145.
[14] Fillebeen C, Charlebois E, Wagner J, et al. Transferrin receptor 1 controls systemic iron homeostasis by fine-tuning hepcidin expression to hepatocellular iron load . Blood, 2019, 133:344-355.
[15] Shaker MK, Attia FM, Hassan AA, et al. Evaluation of Golgi Protein 73 (GP73) as a potential biomarkers for hepatocellular carcinoma . Clin Lab, 2020, 66:275-282.