乙型肝炎表面抗原
医学
肝细胞癌
HBeAg
内科学
危险系数
胃肠病学
乙型肝炎
置信区间
乙型肝炎病毒
比例危险模型
免疫学
病毒
作者
Hsin‐Che Lin,Wen‐Juei Jeng,Jessica Liu,Mei‐Hung Pan,Mei‐Hsuan Lee,Richard Batrla‐Utermann,Sheng‐Nan Lu,Chuen–Fei Chen,Hwai‐I Yang,Chien–Jen Chen
摘要
Summary Background High hepatitis B surface antigen (HBsAg) level predicts hepatocellular carcinoma (HCC) in chronic hepatitis B (CHB) patients with low viral load. The role of longitudinal HBsAg levels in predicting HCC in HBeAg‐positive CHB patients remains unknown. Method HBeAg‐positive CHB participants from the REVEAL‐HBV cohort with ≥2 HBsAg measurements before HBeAg seroclearance were enrolled. Group‐based trajectory modelling identified distinct HBsAg trajectory groups during a median of 11 years of HBeAg‐positive status. Cox regression models were applied for investigating independent predictors of HCC and estimating adjusted hazard ratio (HR adj ) with a 95% confidence interval (CI). A p ‐value less than 0.05 was considered statistically significant. Results A total of 319 patients were enrolled and classified by HBsAg trajectory patterns as (A) persistently high group ( n = 72): HBsAg persistently ≥10 4 IU/mL, and (B) non‐stationary group ( n = 233): low HBsAg at baseline or declining to <10 4 IU/mL during the follow‐up. Group B had higher proportions of abnormal ALT levels, HBV genotype C and basal core mutation than group A ( p < 0.05); age at entry and gender were comparable. The annual incidence of HCC in group A and group B were 0.37% and 1.16%, respectively ( p = 0.03). In multivariate analysis, age >40 years (HR adj [95% CI] = 4.11 [2.26–7.48]), genotype C (HR adj [95% CI] = 4.39 [1.96–9.81]) and the non‐stationary group (HR adj [95% CI] = 3.50 [1.49–8.21]) were independent predictors of HCC. Basal core promoter mutation was the only risk factor of HCC in the persistently high HBsAg group (HR adj [95% CI] = 32.75 [5.41–198.42]). Conclusion Patients with persistently high HBsAg levels during HBeAg‐seropositive stage represent a unique population with low risk of HCC development.
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