Razavi, Homie A and Waked, Imam and Qureshi, Huma and Kondili, Loreta A and Duberg, Ann-Sofi and Aleman, Soo and Tanaka, Junko and Lazarus, Jeffrey V and Low-Beer, Daniel and Abbas, Zaigham and Rached, Antoine Abou and Aghemo, Alessio and Aho, Inka and Akarca, Ulus S and Al-Busafi, Said A and Al-Hamoudi, Waleed K and Al-Naamani, Khalid and Alaama, Ahmed Sabry and Aldar, Manahil M and Alghamdi, Mohammed and Gonzalez, Monica Alonso and Alserehi, Haleema and Anand, Anil C and Asselah, Tarik and Assiri, Abdullah M and Athanasakis, Kostas and Atugonza, Rita and Ben-Ari, Ziv and Berg, Thomas and Brandão-Mello, Carlos E and Brown, Ashley S M and Brown, Kimberly A and Brown, Robert S and Bruggmann, Philip and Brunetto, Maurizia R and Buti, Maria and Cheinquer, Hugo and Christensen, Peer Brehm and Chulanov, Vladimir and Cisneros Garza, Laura E and Coffin, Carla S and Coppola, Nicola and Craxi, Antonio and Crespo, Javier and Cui, Fuqiang and Dalgard, Olav and De La Torre, Alethse and De Ledinghen, Victor and Dieterich, Douglas and Drazilova, Sylvia and Dufour, Jean-François and El-Kassas, Mohamed and Elbadri, Mohammed and Esmat, Gamal and Mur, Rafael Esteban and Eurich, Brandon and Faini, Diana and Ferreira, Paulo R A and Flisiak, Robert and Frankova, Sona and Gaeta, Giovanni B and Gamkrelidze, Ivane and Gane, Edward J and Garcia, Virginia and García-Samaniego, Javier and Gemilyan, Manik and Gottfredsson, Magnus and Gschwantler, Michael and Gurski, Ana P M and Hajarizadeh, Behzad and Hamid, Saeed S and Hatzakis, Angelos and Hercun, Julian and Hockicková, Ivana and Huang, Jee-Fu and Hunyady, Bela and Hutchinson, Sharon J and Ishikawa, Naoko and Izumi, Kiyohiko and Izzi, Antonio and Janicko, Martin and Jarcuska, Peter and Jeruma, Agita and Johannessen, Asgeir and Kaliaskarova, Kulpash S and Kao, Jia-Horng and Kielland, Knut B and Kodjoh, Nicolas and Kottilil, Shyamasundaran and Kristian, Pavol and Kwo, Paul Y and Lagging, Martin and Lam, Hilton and Lázaro, Pablo and Lee, Mei-Hsuan and Lens, Sabela and Liakina, Valentina and Lim, Young-Suk and Makara, Michael and Manns, Michael and Murphy, Niamh and et al, . (2025) Number of people treated for hepatitis C virus infection in 2014-2023 and applicable lessons for new HBV and HDV therapies. Journal of Hepatology, Early online, DOI: 10.1016/j.jhep.2025.01.013.
External website: https://www.journal-of-hepatology.eu/article/S0168...
BACKGROUND AND AIMS: The year 2023 marked the 10-year anniversary of the launch of direct-acting antivirals (DAAs) for the treatment of the hepatitis C virus (HCV). HCV treatment trends by country, region, and globally are important to monitor progress toward the World Health Organization's 2030 elimination targets. Additionally, the historical patterns can help predict the treatment uptake for future therapies for other liver diseases.
METHODS: The number of people living with HCV (PLHCV) treated between 2014-2023 across 119 countries was estimated using national HCV registries, reported DAA sales data, pharmaceutical companies' reports, and estimates provided by national experts. For the countries with no available data, the average estimate of the corresponding Global Burden of Disease region was used.
RESULTS: An estimated 13,816,000 (95% uncertainty intervals (UI): 13,221,000-16,415,000) PLHCV were treated, of whom 12,748,000 (12,226,000-15,231,000) were treated with DAAs, of which 11,081,000 (10,542,000-13,338,000) were sofosbuvir-based DAA regimens. Country-level data accounted for 97% of these estimates. In high-income countries, there was a 41% drop in treatment from its peak, and reimbursement was a large predictor of treatment. In low- and middle-income countries, price played an important role in expanding treatment access through the public and private markets, and treatment continues to increase slowly after a sharp drop at the end of the Egyptian national program.
CONCLUSIONS: In the last 10 years, 21% of all HCV infections were treated with DAAs. Regional and temporal variations highlight the importance of active screening strategies. Without program enhancements, the number of treated PLHCV stalled in every country/region which may not reflect a lower prevalence but may instead reflect the diminishing returns of the existing strategies.
IMPACT AND IMPLICATIONS: Long-term hepatitis C virus (HCV) infection can lead to cirrhosis and liver cancer. Since 2014, these infections can be effectively treated with 8-12 weeks of oral therapies. In 2015, the World Health Organization (WHO) established targets to eliminate HCV by 2030, which included treatment targets for member countries. The current study examines HCV treatment patterns across 119 countries and regions from 2014 to 2023 to assess the impact of national programs. This study can assist physicians and policymakers in understanding treatment patterns within similar regions or income groups and in utilizing historical data to refine their strategies in the future.
G Health and disease > Disease by cause (Aetiology) > Communicable / infectious disease > Hepatitis A (HAV) / D (HDV) / E (HEV)
G Health and disease > Disease by cause (Aetiology) > Communicable / infectious disease > Hepatitis B (HBV)
G Health and disease > Disease by cause (Aetiology) > Communicable / infectious disease > Hepatitis C (HCV)
J Health care, prevention, harm reduction and treatment > Harm reduction > Substance use harm reduction
T Demographic characteristics > Person who injects drugs (Intravenous / injecting)
VA Geographic area > International
VA Geographic area > Europe > Ireland
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