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IDDF2024-ABS-0195 Long-term efficacy of tenofovir alafenamide in HBeAg-positive and -negative chronic hepatitis B patients treated for up to 8 years in 2 phase 3 studies
  1. Wai Kay Seto1,
  2. Maria Buti2,
  3. Kosh Agarwal3,
  4. Henry Lik Yuen Chan4,
  5. Young-Suk Lim5,
  6. Maurizia Brunetto6,
  7. Wan-Long Chuang7,
  8. Harry Janssen8,
  9. Scott Fung9,
  10. Namiki Izumi10,
  11. Maciej Jablkow11,
  12. Frida Abramov12,
  13. Hongyuan Wang12,
  14. Leland Yee12,
  15. Roberto Mateo12,
  16. John Flaherty12,
  17. Calvin Pan13,
  18. Dr Shalimar14,
  19. Patrick Marcellin15,
  20. Edward Gane16
  1. 1Department of Medicine and School of Clinical Medicine, The University of Hong Kong, Hong Kong
  2. 2Hospital Universitario Vall d’Hebron, CIBEREHD del Instituto Carlos III, Spain
  3. 3Institute of Liver Studies, King’s College Hospital NHS Foundation Trust, UK
  4. 4Faculty of Medicine, the Chinese University of Hong Kong, Hong Kong
  5. 5Faculty of Medicine, the Chinese University of Hong Kong, Korea, South
  6. 6Azienda Ospedaliero-Universitaria Pisana, Italy
  7. 7Kaohsiung Medical University Hospital, Kaohsiung Medical University, Taiwan
  8. 8Toronto Centre for Liver Disease, University Health Network, Canada
  9. 9University of Toronto, Department of Medicine, Canada
  10. 10Department of Gastroenterology and Hepatology, Japanese Red Cross Musashino Hospital, Japan
  11. 11Medical University of Łódź, Poland
  12. 12Gilead Sciences, USA
  13. 13NYU Langone Health, New York University Grossman School of Medicine, USA
  14. 14All India Institute of Medical Sciences, India
  15. 15Hepatology Department, Hôpital Beaujon, APHP, INSERM, University of Paris, France
  16. 16Auckland Clinical Studies, New Zealand

Abstract

Background In 2 similarly designed double-blind (DB), randomized (2:1), Phase 3 studies (Study 108 in HBeAg-negative patients [N=425] and Study 110 in HBeAg-positive patients [N=873]), tenofovir alafenamide (TAF) demonstrated non-inferior efficacy relative to tenofovir disoproxil fumarate (TDF) in the blinded assessments. After completing up to 3 years (yr) of DB treatment, all patients were eligible to receive open-label (OL) TAF through week 384 (yr 8). Here, we present the final 8-yr results.

Methods Efficacy was assessed for each study by missing equals excluded (M=E) approach of the full analysis set and included serial assessments for viral suppression (HBV DNA < 29 IU/mL), ALT normalization by 2018 AASLD criteria, serologic responses, and fibrosis change by serum FibroTest. Resistance analyses, including deep sequencing of HBV pol/RT (at baseline and annually), for those with virologic breakthrough/blip, persistent viremia, or treatment discontinuation with viremia were performed, as was phenotyping of qualifying samples.

Results Of 1298 randomized and treated patients, 1157 (89%; 775 TAF; 382 TDF) entered the OL phase, including 180 and 202 TDF-treated patients who began OL TAF at week 96 (TDF-OL TAF 6 yr) or week 144 (TDF-OL TAF 5 yr) based on the timing of a protocol amendment. Overall, 974 (75%) participants completed OL study treatment. The most common reasons for discontinuation were withdrawal of consent, loss to follow-up, or investigator discretion. Similar high rates of virologic suppression and ALT normalization were achieved and maintained over 8 yr in all treatment groups (IDDF2024-ABS-0195 Table 1). Sequence/phenotyping analysis through 6 yr showed no resistance to TAF; resistance analyses at yr 8 are ongoing.

Abstract IDDF2024-ABS-0195 Table 1

Results at Yr 8a

Conclusions After 8 yr of treatment with TAF or up to 6 yr after switching from TDF, virologic suppression rates remained high across all groups; up to 33% achieved HBeAg/HBeAb seroconversion, while HBsAg loss was low (≤5%).

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