Sofosbuvir/Velpatasvir for Hepatitis C Virus Infection: Real-World Effectiveness and Safety from a Nationwide Registry in Taiwan

TACR investigators

doi:10.1007/s40121-021-00576-7

Sofosbuvir/Velpatasvir for Hepatitis C Virus Infection: Real-World Effectiveness and Safety from a Nationwide Registry in Taiwan

TACR investigators

Taipei Medical University Hospital

Research output: Contribution to journal › Article › peer-review

5 Citations (Scopus)

Abstract

Introduction: Pangenotypic direct-acting antivirals are expected to cure hepatitis C virus (HCV) in more than 95% of treated patients. However, data on the effectiveness and safety of sofosbuvir/velpatasvir (SOF/VEL) in Taiwan are limited. This study aims to characterize the patient population in the nationwide Taiwan Association for the Study of the Liver (TASL) HCV Registry and evaluate treatment outcome in Taiwanese patients receiving SOF/VEL. Methods: This study was a retrospective-prospective, observational, multicenter, real-world analysis. Adults with chronic hepatitis C were treated with SOF/VEL 400/100 mg ± ribavirin for 12 weeks. The primary outcome was sustained virologic response 12 weeks after end of therapy (SVR12). Factors associated with not achieving SVR12 were evaluated using logistic regression and covariate analysis. Safety was also assessed. Results: In total, 3480 patients were included: 86.8% genotype 1/2, 2.8% genotype 3, 0.1% genotype 4/5, 9.6% genotype 6; unclassified, 0.8%; 12.2% compensated cirrhosis; 3.3% decompensated cirrhosis; and 15.8% chronic kidney disease. Overall SVR12 rate was 99.4% (genotype 1, 99.5%; genotype 2, 99.4%; genotype 3, 96.9%; genotype 4, 100%; genotype 6, 99.7%). SVR12 rates among patients with compensated cirrhosis, decompensated cirrhosis, and chronic kidney disease stages 4–5 were 99.5%, 100%, and 100%, respectively. There were 21 patients (0.6%) who did not achieve SVR12. Factors associated with failure were treatment adherence below 60%, high viral load, and genotype 3 (p < 0.001, p = 0.028, and p = 0.001, respectively). Adverse events occurred in 10% of patients; 0.6% were serious and one was related to treatment. Treatment discontinuation occurred in 0.3% of patients; none were treatment related. The estimated glomerular filtration rate remained stable throughout treatment and follow-up, regardless of baseline values and cirrhosis status. Conclusion: SOF/VEL was highly effective and well tolerated in Taiwanese patients, irrespective of viral genotype, liver disease severity, and comorbidities.

Original language	English
Pages (from-to)	485-500
Number of pages	16
Journal	Infectious Diseases and Therapy
Volume	11
Issue number	1
DOIs	https://doi.org/10.1007/s40121-021-00576-7
Publication status	Published - Feb 2022

Keywords

Direct-acting antivirals
Hepatitis C
Real-world
Sofosbuvir
Taiwan
Velpatasvir

ASJC Scopus subject areas

Microbiology (medical)
Infectious Diseases

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1007/s40121-021-00576-7

Cite this

@article{051b49bd626440448c02eaf1fe3be1b9,

title = "Sofosbuvir/Velpatasvir for Hepatitis C Virus Infection: Real-World Effectiveness and Safety from a Nationwide Registry in Taiwan",

abstract = "Introduction: Pangenotypic direct-acting antivirals are expected to cure hepatitis C virus (HCV) in more than 95% of treated patients. However, data on the effectiveness and safety of sofosbuvir/velpatasvir (SOF/VEL) in Taiwan are limited. This study aims to characterize the patient population in the nationwide Taiwan Association for the Study of the Liver (TASL) HCV Registry and evaluate treatment outcome in Taiwanese patients receiving SOF/VEL. Methods: This study was a retrospective-prospective, observational, multicenter, real-world analysis. Adults with chronic hepatitis C were treated with SOF/VEL 400/100 mg ± ribavirin for 12 weeks. The primary outcome was sustained virologic response 12 weeks after end of therapy (SVR12). Factors associated with not achieving SVR12 were evaluated using logistic regression and covariate analysis. Safety was also assessed. Results: In total, 3480 patients were included: 86.8% genotype 1/2, 2.8% genotype 3, 0.1% genotype 4/5, 9.6% genotype 6; unclassified, 0.8%; 12.2% compensated cirrhosis; 3.3% decompensated cirrhosis; and 15.8% chronic kidney disease. Overall SVR12 rate was 99.4% (genotype 1, 99.5%; genotype 2, 99.4%; genotype 3, 96.9%; genotype 4, 100%; genotype 6, 99.7%). SVR12 rates among patients with compensated cirrhosis, decompensated cirrhosis, and chronic kidney disease stages 4–5 were 99.5%, 100%, and 100%, respectively. There were 21 patients (0.6%) who did not achieve SVR12. Factors associated with failure were treatment adherence below 60%, high viral load, and genotype 3 (p < 0.001, p = 0.028, and p = 0.001, respectively). Adverse events occurred in 10% of patients; 0.6% were serious and one was related to treatment. Treatment discontinuation occurred in 0.3% of patients; none were treatment related. The estimated glomerular filtration rate remained stable throughout treatment and follow-up, regardless of baseline values and cirrhosis status. Conclusion: SOF/VEL was highly effective and well tolerated in Taiwanese patients, irrespective of viral genotype, liver disease severity, and comorbidities.",

keywords = "Direct-acting antivirals, Hepatitis C, Real-world, Sofosbuvir, Taiwan, Velpatasvir",

author = "{TACR investigators} and Cheng, {Pin Nan} and Mo, {Lein Ray} and Chen, {Chun Ting} and Chen, {Chi Yi} and Huang, {Chung Feng} and Kuo, {Hsing Tao} and Lo, {Ching Chu} and Tseng, {Kuo Chih} and Huang, {Yi Hsiang} and Tai, {Chi Ming} and Peng, {Cheng Yuan} and Bair, {Ming Jong} and Chen, {Chien Hung} and Yeh, {Ming Lun} and Lin, {Chih Lang} and Lin, {Chun Yen} and Lee, {Pei Lun} and Chong, {Lee Won} and Hung, {Chao Hung} and Chang, {Te Sheng} and Huang, {Jee Fu} and Yang, {Chi Chieh} and Hu, {Jui Ting} and Lin, {Chih Wen} and Wang, {Chia Chi} and Su, {Wei Wen} and Hsieh, {Tsai Yuan} and Lin, {Chih Lin} and Tsai, {Wei Lun} and Lee, {Tzong Hsi} and Chen, {Guei Ying} and Wang, {Szu Jen} and Chang, {Chun Chao} and Yang, {Sheng Shun} and Wu, {Wen Chih} and Huang, {Chia Sheng} and Chou, {Kwok Hsiung} and Kao, {Chien Neng} and Tsai, {Pei Chien} and Liu, {Chen Hua} and Lee, {Mei Hsuan} and Cheng, {Chien Yu} and Tsai, {Ming Chang} and Liu, {Chun Jen} and Dai, {Chia Yen} and Lin, {Han Chieh} and Kao, {Jia Horng} and Chuang, {Wan Long} and Yu, {Ming Lung}",

note = "Funding Information: The study was partly supported by grants from Kaohsiung Medical University (MOST 109-2314-B-037-044, KMU-K1110002, MOST 108-2314-B-037-066-MY3, KMU-TC108B06 [Center for Liquid Biopsy], KMU-TC108B07 & KMU-DK109002 [Cohort Research Center], 105KMUOR08 [Center for Cancer Research KMU Global Networking Talent Plan Grant], and KMU-TC109B05 [Center for Liquid Biopsy and Cohort Research]) and Kaohsiung Medical University Hospital (KMUH109-9R06, KMUH109-9R05, MOHW109-TDU-B-212-114006 and KMUH-IIT-109-2-05). The journal{\textquoteright}s Rapid Service Fee is funded by Gilead Sciences Hong Kong Ltd. Funding Information: Medical writing assistance was provided by Ridda Jabbar and Julia Heagerty from Elements Communications Ltd, United Kingdom, funded by Gilead Sciences Hong Kong Ltd. Gilead had no control over the final content of this manuscript. Funding Information: Pin-Nan Cheng: Advisory board for AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Speaker for Abbott, AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Research grants from Gilead Sciences and Merck Sharp & Dohme. Jia-Horng Kao: Speaker, consultant and/or advisory board member for AbbVie, Arbutus Biopharma, Bristol Myers Squibb, Fujirebio, Gilead Sciences, Johnson & Johnson, MSD, Polaris, Sysmex and Roche. Ming-Lung Yu: Research support (grant) from Abbott, BMS, Gilead Sciences and Merck Sharp & Dohme. Consultant of AbbVie, Abbott, BMS, Gilead Sciences, Merck Sharp & Dohme, and Roche Diagnostics. Speaker for AbbVie, Abbott, BMS, Gilead Sciences, IPSEN, Merck Sharp & Dohme and Roche. Chung-Feng Huang: Speaker for AbbVie, BMS, Gilead Sciences, Merck Sharp & Dohme, and Roche. Chen-Hua Liu: Advisory board for AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Speaker for Abbott, AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Research grants from AbbVie, Gilead Sciences, and Merck Sharp & Dohme. All other authors (Lein-Ray Mo, Chun-Ting Chen, Chi-Yi Chen, Hsing-Tao Kuo, Ching-Chu Lo, Kuo-Chih Tseng, Yi-Hsiang Huang, Chi-Ming Tai, Cheng-Yuan Peng, Ming-Jong Bair, Chien-Hung Chen, Ming-Lun Yeh, Chih-Lang Lin, Chun-Yen Lin, Pei-Lun Lee, Lee-Won Chong, Chao-Hung Hung, Te Sheng Chang, Jee-Fu Huang, Chi-Chieh Yang, Jui-Ting Hu, Chih-Wen Lin, Chia-Chi Wang, Wei-Wen Su, Tsai-Yuan Hsieh, Chih-Lin Lin, Wei-Lun Tsai, Tzong-Hsi Lee, Guei-Ying Chen, Szu-Jen Wang, Chun-Chao Chang, Sheng-Shun Yang, Wen-Chih Wu, Chia-Sheng Huang, Kwok-Hsiung Chou, Chien-Neng Kao, Pei-Chien Tsai, Mei-Hsuan Lee, Chien-Yu Cheng, Ming-Chang Tsai, Chun-Jen Liu, Chia-Yen Dai, Han-Chieh Lin, Wan-Long Chuang): Nothing to disclose. Funding Information: The authors would also like to thank the Taiwan Association for the Study of the Liver (TASL), the TASL Foundation, and Taiwan Liver Research Foundation for grant support and the TACR study group for data collection. We also thank the Center for Medical Informatics and Statistics of Kaohsiung Medical University for providing administrative and funding support. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2022",

month = feb,

doi = "10.1007/s40121-021-00576-7",

language = "English",

volume = "11",

pages = "485--500",

journal = "Infectious Diseases and Therapy",

issn = "2193-8229",

publisher = "Springer Healthcare",

number = "1",

}

TY - JOUR

T1 - Sofosbuvir/Velpatasvir for Hepatitis C Virus Infection

T2 - Real-World Effectiveness and Safety from a Nationwide Registry in Taiwan

AU - TACR investigators

AU - Cheng, Pin Nan

AU - Mo, Lein Ray

AU - Chen, Chun Ting

AU - Chen, Chi Yi

AU - Huang, Chung Feng

AU - Kuo, Hsing Tao

AU - Lo, Ching Chu

AU - Tseng, Kuo Chih

AU - Huang, Yi Hsiang

AU - Tai, Chi Ming

AU - Peng, Cheng Yuan

AU - Bair, Ming Jong

AU - Chen, Chien Hung

AU - Yeh, Ming Lun

AU - Lin, Chih Lang

AU - Lin, Chun Yen

AU - Lee, Pei Lun

AU - Chong, Lee Won

AU - Hung, Chao Hung

AU - Chang, Te Sheng

AU - Huang, Jee Fu

AU - Yang, Chi Chieh

AU - Hu, Jui Ting

AU - Lin, Chih Wen

AU - Wang, Chia Chi

AU - Su, Wei Wen

AU - Hsieh, Tsai Yuan

AU - Lin, Chih Lin

AU - Tsai, Wei Lun

AU - Lee, Tzong Hsi

AU - Chen, Guei Ying

AU - Wang, Szu Jen

AU - Chang, Chun Chao

AU - Yang, Sheng Shun

AU - Wu, Wen Chih

AU - Huang, Chia Sheng

AU - Chou, Kwok Hsiung

AU - Kao, Chien Neng

AU - Tsai, Pei Chien

AU - Liu, Chen Hua

AU - Lee, Mei Hsuan

AU - Cheng, Chien Yu

AU - Tsai, Ming Chang

AU - Liu, Chun Jen

AU - Dai, Chia Yen

AU - Lin, Han Chieh

AU - Kao, Jia Horng

AU - Chuang, Wan Long

AU - Yu, Ming Lung

N1 - Funding Information: The study was partly supported by grants from Kaohsiung Medical University (MOST 109-2314-B-037-044, KMU-K1110002, MOST 108-2314-B-037-066-MY3, KMU-TC108B06 [Center for Liquid Biopsy], KMU-TC108B07 & KMU-DK109002 [Cohort Research Center], 105KMUOR08 [Center for Cancer Research KMU Global Networking Talent Plan Grant], and KMU-TC109B05 [Center for Liquid Biopsy and Cohort Research]) and Kaohsiung Medical University Hospital (KMUH109-9R06, KMUH109-9R05, MOHW109-TDU-B-212-114006 and KMUH-IIT-109-2-05). The journal’s Rapid Service Fee is funded by Gilead Sciences Hong Kong Ltd. Funding Information: Medical writing assistance was provided by Ridda Jabbar and Julia Heagerty from Elements Communications Ltd, United Kingdom, funded by Gilead Sciences Hong Kong Ltd. Gilead had no control over the final content of this manuscript. Funding Information: Pin-Nan Cheng: Advisory board for AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Speaker for Abbott, AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Research grants from Gilead Sciences and Merck Sharp & Dohme. Jia-Horng Kao: Speaker, consultant and/or advisory board member for AbbVie, Arbutus Biopharma, Bristol Myers Squibb, Fujirebio, Gilead Sciences, Johnson & Johnson, MSD, Polaris, Sysmex and Roche. Ming-Lung Yu: Research support (grant) from Abbott, BMS, Gilead Sciences and Merck Sharp & Dohme. Consultant of AbbVie, Abbott, BMS, Gilead Sciences, Merck Sharp & Dohme, and Roche Diagnostics. Speaker for AbbVie, Abbott, BMS, Gilead Sciences, IPSEN, Merck Sharp & Dohme and Roche. Chung-Feng Huang: Speaker for AbbVie, BMS, Gilead Sciences, Merck Sharp & Dohme, and Roche. Chen-Hua Liu: Advisory board for AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Speaker for Abbott, AbbVie, Gilead Sciences, and Merck Sharp & Dohme. Research grants from AbbVie, Gilead Sciences, and Merck Sharp & Dohme. All other authors (Lein-Ray Mo, Chun-Ting Chen, Chi-Yi Chen, Hsing-Tao Kuo, Ching-Chu Lo, Kuo-Chih Tseng, Yi-Hsiang Huang, Chi-Ming Tai, Cheng-Yuan Peng, Ming-Jong Bair, Chien-Hung Chen, Ming-Lun Yeh, Chih-Lang Lin, Chun-Yen Lin, Pei-Lun Lee, Lee-Won Chong, Chao-Hung Hung, Te Sheng Chang, Jee-Fu Huang, Chi-Chieh Yang, Jui-Ting Hu, Chih-Wen Lin, Chia-Chi Wang, Wei-Wen Su, Tsai-Yuan Hsieh, Chih-Lin Lin, Wei-Lun Tsai, Tzong-Hsi Lee, Guei-Ying Chen, Szu-Jen Wang, Chun-Chao Chang, Sheng-Shun Yang, Wen-Chih Wu, Chia-Sheng Huang, Kwok-Hsiung Chou, Chien-Neng Kao, Pei-Chien Tsai, Mei-Hsuan Lee, Chien-Yu Cheng, Ming-Chang Tsai, Chun-Jen Liu, Chia-Yen Dai, Han-Chieh Lin, Wan-Long Chuang): Nothing to disclose. Funding Information: The authors would also like to thank the Taiwan Association for the Study of the Liver (TASL), the TASL Foundation, and Taiwan Liver Research Foundation for grant support and the TACR study group for data collection. We also thank the Center for Medical Informatics and Statistics of Kaohsiung Medical University for providing administrative and funding support. Publisher Copyright: © 2021, The Author(s).

PY - 2022/2

Y1 - 2022/2

N2 - Introduction: Pangenotypic direct-acting antivirals are expected to cure hepatitis C virus (HCV) in more than 95% of treated patients. However, data on the effectiveness and safety of sofosbuvir/velpatasvir (SOF/VEL) in Taiwan are limited. This study aims to characterize the patient population in the nationwide Taiwan Association for the Study of the Liver (TASL) HCV Registry and evaluate treatment outcome in Taiwanese patients receiving SOF/VEL. Methods: This study was a retrospective-prospective, observational, multicenter, real-world analysis. Adults with chronic hepatitis C were treated with SOF/VEL 400/100 mg ± ribavirin for 12 weeks. The primary outcome was sustained virologic response 12 weeks after end of therapy (SVR12). Factors associated with not achieving SVR12 were evaluated using logistic regression and covariate analysis. Safety was also assessed. Results: In total, 3480 patients were included: 86.8% genotype 1/2, 2.8% genotype 3, 0.1% genotype 4/5, 9.6% genotype 6; unclassified, 0.8%; 12.2% compensated cirrhosis; 3.3% decompensated cirrhosis; and 15.8% chronic kidney disease. Overall SVR12 rate was 99.4% (genotype 1, 99.5%; genotype 2, 99.4%; genotype 3, 96.9%; genotype 4, 100%; genotype 6, 99.7%). SVR12 rates among patients with compensated cirrhosis, decompensated cirrhosis, and chronic kidney disease stages 4–5 were 99.5%, 100%, and 100%, respectively. There were 21 patients (0.6%) who did not achieve SVR12. Factors associated with failure were treatment adherence below 60%, high viral load, and genotype 3 (p < 0.001, p = 0.028, and p = 0.001, respectively). Adverse events occurred in 10% of patients; 0.6% were serious and one was related to treatment. Treatment discontinuation occurred in 0.3% of patients; none were treatment related. The estimated glomerular filtration rate remained stable throughout treatment and follow-up, regardless of baseline values and cirrhosis status. Conclusion: SOF/VEL was highly effective and well tolerated in Taiwanese patients, irrespective of viral genotype, liver disease severity, and comorbidities.

AB - Introduction: Pangenotypic direct-acting antivirals are expected to cure hepatitis C virus (HCV) in more than 95% of treated patients. However, data on the effectiveness and safety of sofosbuvir/velpatasvir (SOF/VEL) in Taiwan are limited. This study aims to characterize the patient population in the nationwide Taiwan Association for the Study of the Liver (TASL) HCV Registry and evaluate treatment outcome in Taiwanese patients receiving SOF/VEL. Methods: This study was a retrospective-prospective, observational, multicenter, real-world analysis. Adults with chronic hepatitis C were treated with SOF/VEL 400/100 mg ± ribavirin for 12 weeks. The primary outcome was sustained virologic response 12 weeks after end of therapy (SVR12). Factors associated with not achieving SVR12 were evaluated using logistic regression and covariate analysis. Safety was also assessed. Results: In total, 3480 patients were included: 86.8% genotype 1/2, 2.8% genotype 3, 0.1% genotype 4/5, 9.6% genotype 6; unclassified, 0.8%; 12.2% compensated cirrhosis; 3.3% decompensated cirrhosis; and 15.8% chronic kidney disease. Overall SVR12 rate was 99.4% (genotype 1, 99.5%; genotype 2, 99.4%; genotype 3, 96.9%; genotype 4, 100%; genotype 6, 99.7%). SVR12 rates among patients with compensated cirrhosis, decompensated cirrhosis, and chronic kidney disease stages 4–5 were 99.5%, 100%, and 100%, respectively. There were 21 patients (0.6%) who did not achieve SVR12. Factors associated with failure were treatment adherence below 60%, high viral load, and genotype 3 (p < 0.001, p = 0.028, and p = 0.001, respectively). Adverse events occurred in 10% of patients; 0.6% were serious and one was related to treatment. Treatment discontinuation occurred in 0.3% of patients; none were treatment related. The estimated glomerular filtration rate remained stable throughout treatment and follow-up, regardless of baseline values and cirrhosis status. Conclusion: SOF/VEL was highly effective and well tolerated in Taiwanese patients, irrespective of viral genotype, liver disease severity, and comorbidities.

KW - Direct-acting antivirals

KW - Hepatitis C

KW - Real-world

KW - Sofosbuvir

KW - Taiwan

KW - Velpatasvir

UR - http://www.scopus.com/inward/record.url?scp=85122256113&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85122256113&partnerID=8YFLogxK

U2 - 10.1007/s40121-021-00576-7

DO - 10.1007/s40121-021-00576-7

M3 - Article

AN - SCOPUS:85122256113

SN - 2193-8229

VL - 11

SP - 485

EP - 500

JO - Infectious Diseases and Therapy

JF - Infectious Diseases and Therapy

IS - 1

ER -