Switching to besifovir in patients with chronic hepatitis B receiving tenofovir disoproxil fumarate: A randomized trialopen access
- Authors
- Yim, Hyung Joon; Seo, Yeon Seok; Kim, Ji Hoon; Kim, Won; Jung, Young Kul; Jang, Jae Young; Lee, Sae Hwan; Kim, Yun Soo; Kim, Chang Wook; Kim, Hyoung Su; Shim, Jae-Jun; Cho, Eun-Young; Kim, In Hee; Lee, Byung Seok; Lee, Jeong-Hoon; Kim, Byung Seok; Jang, Jeong Won; Lee, Hyun Woong; Kwon, Jung Hyun; Kim, Moon Young; Song, Do Seon; Park, Jung Gil; Lee, Yoon Seok; Yoon, Eileen L.; Lee, Han Ah; Kang, Seong Hee; Yang, Jin Mo
- Issue Date
- Jul-2025
- Publisher
- 대한간학회
- Keywords
- Antiviral therapy; Bone mineral density; Hepatitis B; Nephrotoxicity; Sustained virologic response
- Citation
- Clinical and Molecular Hepatology, v.31, no.3, pp 810 - 822
- Pages
- 13
- Indexed
- SCIE
SCOPUS
KCI
- Journal Title
- Clinical and Molecular Hepatology
- Volume
- 31
- Number
- 3
- Start Page
- 810
- End Page
- 822
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/209994
- DOI
- 10.3350/cmh.2024.0819
- ISSN
- 2287-2728
2287-285X
- Abstract
- Background/Aims: Besifovir (BSV) showed comparable antiviral activity and superior safety profiles to tenofovir disoproxil fumarate (TDF) in treatment-naïve chronic hepatitis B (CHB). However, no data are available regarding the antiviral efficacy and safety of BSV in patients with CHB who switched from long-term TDF to BSV. This study aimed to evaluate the outcome of a 48-week BSV therapy in patients with CHB who switched from long-term TDF treatment. Methods: In this non-inferiority trial, 153 CHB patients treated with TDF for ≥48 weeks who had hepatitis B virus (HBV) DNA <20 IU/mL were randomized to receive either BSV 150 mg or TDF 300 mg for 48 weeks. Results: The per-protocol analysis included 130 patients (BSV group, 64; TDF group, 66). The median duration of TDF use before enrollment was 4.14 years. After 48 weeks, 100.0% and 98.5% patients in the BSV and TDF groups, respectively, met the primary endpoint (HBV DNA <20 IU/mL), demonstrating the non-inferior antiviral efficacy of BSV to TDF (95% confidence interval –0.01 to 0.04; P>0.999), with a predefined margin of –0.18. The mean percentage changes in estimated glomerular filtration rates were slightly better in the BSV group (1.67±11.73%) than in the TDF group (–1.24±11.02%). The BSV group showed a significant improvement in bone turnover biomarkers compared to the TDF group; accordingly, hip and spine bone mineral density increased in the BSV group. Conclusions: In patients with CHB receiving long-term TDF, switching to BSV may improve renal and bone safety with non-inferior antiviral efficacy compared to that of maintaining TDF.
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