酒精相关性肝病中肝细胞癌的发病率和预测:对 136 571 名慢性肝病患者的回顾性研究

B. Chang, Hui Tian, Ang Huang, Xingran Zhai, Qiaoling Wang, Lin Han, Xueyuan Jin, Li Gao, Qing-xiang Liang, Baosen Li, Yinying Lu, Huan Xie, Dong Ji, Zhengsheng Zou
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Afterward, the new established model was validated using external cohort by receiver operating characteristic curves analysis. For external cohort, 1646 patients with ALD admitted to our hospital from 2019 to 2021 were included. ALD was diagnosed on the basis of a history of sustained heavy alcohol intake greater than 40 g/day for men and 20 g/day for women for >5 years, clinical evidence of liver disease and supporting laboratory abnormalities.Over the last 17 years, trends showed obviously increases in ALD. ALD-related HCC experienced a significant increase from 5.8% to 30.7%, whereas hepatitis B virus (HBV)-related HCC declined from 77.6% to 52.0%. In patients with ALD-related HCC (5119), 3816 (74.54%) cases had HBV infection, 493 (9.63%) cases had hepatitis C virus (HCV) infection, 71 (1.39%) cases were coinfected with both HBV and HCV, and 739 (14.44%) cases had neither HBV nor HCV infection. 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引用次数: 0

摘要

目的:探讨酒精相关肝细胞癌(HCC)的发病率,评估酒精与众所周知的HCC相关风险因素之间可能存在的协同作用,并建立预测酒精相关肝病(ALD)相关HCC风险的提名图。通过病历回顾收集数据。采用多元逻辑回归确定与 HCC 相关的独立高危因素,并将其纳入新的提名图。随后,通过接收者操作特征曲线分析,利用外部队列对新建立的模型进行了验证。在外部队列中,纳入了我院在2019年至2021年期间收治的1646名ALD患者。ALD的诊断依据是男性持续大量摄入酒精超过40克/天,女性持续大量摄入酒精超过20克/天,且持续时间超过5年,有肝脏疾病的临床证据和支持性实验室异常。在过去的 17 年中,ALD 的发病率呈明显上升趋势,与 ALD 相关的 HCC 从 5.8% 显著上升至 30.7%,而与乙型肝炎病毒(HBV)相关的 HCC 则从 77.6% 下降至 52.0%。在与 ALD 相关的 HCC 患者(5119 例)中,有 3816 例(74.54%)感染了 HBV,493 例(9.63%)感染了丙型肝炎病毒(HCV),71 例(1.39%)同时感染了 HBV 和 HCV,739 例(14.44%)既未感染 HBV 也未感染 HCV。饮酒年限(OR 1.009,95% CI(1.000 至 1.017))、年龄(OR 1.060,95% CI(1.051 至 1.069))、糖尿病(OR 1.314,95% CI(1.123 至 1.538))、HBV 感染(OR 4.905,95% CI(4.肝硬化(OR 4.922,95% CI (3.887 to 6.232))和男性(OR 17.011,95%CI (2.296 to 126.013))与 ALD 患者罹患 HCC 的风险增加有关。提名图的一致性指数为 0.786(95% CI 0.773 至 0.799),校准曲线拟合良好。这些结果在内部队列和外部队列中都得到了成功验证。本研究建立的提名图模型具有准确度高、易于使用等特点,可对ALD患者的HCC发展情况进行最佳预测,从而帮助临床医生制定个体化的精准治疗策略。
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Prevalence and prediction of hepatocellular carcinoma in alcohol-associated liver disease: a retrospective study of 136 571 patients with chronic liver diseases
To explore the incidence of alcohol-related hepatocellular carcinoma (HCC), evaluate possible synergisms between alcohol and well-known risk factors associated with HCC and establish a nomogram to predict alcohol-associated liver disease (ALD)-related HCC risk.A database of 136 571 inpatients in the Fifth Medical Center of Chinese PLA General Hospital from 2002 to 2018 with chronic liver disease was established. Data were collected by medical records review. Multivariate logistic regression was used to identify the independent high-risk factors associated with HCC, and then were incorporated into a novel nomogram. Afterward, the new established model was validated using external cohort by receiver operating characteristic curves analysis. For external cohort, 1646 patients with ALD admitted to our hospital from 2019 to 2021 were included. ALD was diagnosed on the basis of a history of sustained heavy alcohol intake greater than 40 g/day for men and 20 g/day for women for >5 years, clinical evidence of liver disease and supporting laboratory abnormalities.Over the last 17 years, trends showed obviously increases in ALD. ALD-related HCC experienced a significant increase from 5.8% to 30.7%, whereas hepatitis B virus (HBV)-related HCC declined from 77.6% to 52.0%. In patients with ALD-related HCC (5119), 3816 (74.54%) cases had HBV infection, 493 (9.63%) cases had hepatitis C virus (HCV) infection, 71 (1.39%) cases were coinfected with both HBV and HCV, and 739 (14.44%) cases had neither HBV nor HCV infection. Drinking years (OR 1.009, 95% CI (1.000 to 1.017)), age (OR 1.060, 95% CI (1.051 to 1.069)), diabetes mellitus (OR 1.314, 95% CI (1.123 to 1.538)), HBV infection (OR 4.905, 95% CI (4.242 to 5.671)), liver cirrhosis (OR 4.922, 95% CI (3.887 to 6.232)) and male sex (OR 17.011, 95%CI (2.296 to 126.013)) were associated with increased risk of HCC in patients with ALD. A nomogram had a concordance index of 0.786 (95% CI 0.773 to 0.799) and had well-fitted calibration curves. These results were successfully validated both in the internal cohort and external cohort.The prevalence of ALD and ALD-related HCC has been increased dramatically. The nomogram model established here with its high accuracy and easy-to-use features achieved an optimal prediction of HCC development in patients with ALD, which can help clinicians to develop an individualised and precise treatment strategy.
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