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PAGE-B incorporating moderate HBV DNA levels predicts risk of HCC among patients entering into HBeAg-positive chronic hepatitis B

Authors
Chun, Ho SooPapatheodoridis, George V.Lee, MinjongLee, Hye AhKim, Yeong HwaKim, Seo HyunOh, Yun-SeoPark, Su JinKim, JihyeLee, Han AhKim, Hwi YoungKim, Tae HunYoon, Eileen L.Jun, Dae WonAhn, Sang HoonSypsa, VanaYurdaydin, CihanLampertico, PietroCalleja, Jose LuisJanssen, Harry LA.Dalekos, George N.Goulis, JohnBerg, ThomasButi, MariaKim, Seung UpKim, Yoon Jun
Issue Date
Jan-2024
Publisher
Elsevier BV
Keywords
HBeAg-positive chronic hepatitis B; HBeAg-positive chronic infection; hepatocellular carcinoma; risk prediction model
Citation
Journal of Hepatology, v.80, no.1, pp 20 - 30
Pages
11
Indexed
SCIE
SCOPUS
Journal Title
Journal of Hepatology
Volume
80
Number
1
Start Page
20
End Page
30
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/196821
DOI
10.1016/j.jhep.2023.09.011
ISSN
0168-8278
1600-0641
Abstract
Background & Aims: Recent studies reported that moderate HBV DNA levels are significantly associated with hepatocellular carcinoma (HCC) risk in hepatitis B e antigen (HBeAg)-positive, non-cirrhotic patients with chronic hepatitis B (CHB). We aimed to develop and validate a new risk score to predict HCC development using baseline moderate HBV DNA levels in patients entering into HBeAg-positive CHB from chronic infection. Methods: This multicenter cohort study recruited 3,585 HBeAg-positive, non-cirrhotic patients who started antiviral treatment with entecavir or tenofovir disoproxil fumarate at phase change into CHB from chronic infection in 23 tertiary university-affiliated hospitals of South Korea (2012-2020). A new HCC risk score (PAGED-B) was developed (training cohort, n = 2,367) based on multivariable Cox models. Internal validation using bootstrap sampling and external validation (validation cohort, n = 1,218) were performed. Results: Sixty (1.7%) patients developed HCC (median follow-up, 5.4 years). In the training cohort, age, gender, platelets, diabetes and moderate HBV DNA levels (5.00-7.99 log10 IU/ml) were independently associated with HCC development; the PAGED-B score (based on these five predictors) showed a time-dependent AUROC of 0.81 for the prediction of HCC development at 5 years. In the validation cohort, the AUROC of PAGED-B was 0.85, significantly higher than for other risk scores (PAGE-B, mPAGE-B, CAMD, and REAL-B). When stratified by the PAGED-B score, the HCC risk was significantly higher in highrisk patients than in low-risk patients (sub-distribution hazard ratio = 8.43 in the training and 11.59 in the validation cohorts, all p <0.001). Conclusions: The newly established PAGED-B score may enable risk stratification for HCC at the time of transition into HBeAgpositive CHB.
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