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IDDF2024-ABS-0205 Impact of long-term treatment with continuous tenofovir alafenamide (TAF) or after switch from tenofovir disoproxil fumarate (TDF) on hepatocellular carcinoma (HCC) incidence in patients with chronic hepatitis B (CHB)

替诺福韦-阿拉芬酰胺 肝细胞癌 医学 胃肠病学 内科学 入射(几何) 肝硬化 乙型肝炎 替诺福韦 免疫学 病毒载量 人类免疫缺陷病毒(HIV) 光学 物理 抗逆转录病毒疗法
作者
Young‐Suk Lim,Grace Wong,Sang Hoon Ahn,Wai Kay Seto,Kosh Agarwal,Harry L.A. Janssen,Calvin Q. Pan,Wan‐Long Chuang,Scott Fung,S. Shalimar,Maurizia Rossana Brunetto,Aric J. Hui,Ting‐Tsung Chang,Seng Gee Lim,Frida Abramov,John F. Flaherty,Hongyuan Wang,Leland J. Yee,Jia–Horng Kao,Patrick Marcellin,Edward Gane,Marı́a Buti
标识
DOI:10.1136/gutjnl-2024-iddf.189
摘要

Background

In an integrated analysis of 2 global Phase 3 studies, we evaluated HCC incidence and risk at 8 years in patients treated with TAF and those treated initially with TDF and then switched to TAF for up to 6 years (y).

Methods

In 2 studies, HBeAg-positive (n=859) and -negative (n=439) patients with HBV DNA ≥20,000 IU/mL and ALT >60 U/L (males) or >38 U/L (females) were randomized to TAF or TDF in a double-blind (DB) phase for up to 3 y, followed by open-label (OL) TAF through Y8. HCC was assessed by local standards of care and by hepatic ultrasonography. Three validated models (REACH-B, aMAP, and mPAGE-B) were utilized to assess HCC risk by initial treatment assignment and collectively. Using the REACH-B model, standard incidence ratios (SIRs) for HCC were calculated.

Results

Through Y8, HCC was diagnosed in 21/1298 patients (1.6%; TAF 1.4%; TDF→TAF 2.1%; P=0.33)— 11 in DB/10 in OL phase. Eight of 21 HCC cases were in cirrhotic patients. The median time to HCC onset was 729 days (TAF 1291, TDF→TAF 460 days). Advanced age, male, and cirrhosis were more common in HCC vs non-HCC patients (P<0.05). Proportionately, more HCC patients were HBV genotype C (76% vs 47%) and had BL HBV DNA between 6 to ≤ 8 log10IU/mL (57% vs 38%). With treatment over 8y, by REACH-B, HCC incidence was significantly reduced (21 observed vs 74.6 predicted; SIR [95% CI] 0.28; P<0.0001; figure 1). Of patients predicted to be low risk for HCC at BL, nearly all remained low risk at Y8 by aMAP (98%) and mPAGE-B (97%), and substantial proportions estimated to be medium or high risk at BL shifted to lower risk at Y8 (aMAP: 45% and 72%; mPAGE-B: 27% and 51%, respectively).

Conclusions

CHB patients treated with TAF alone or switched from TDF to TAF for up to 8 y showed a reduced observed vs predicted risk for HCC development.
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