Diagnosis, treatment, and follow-up of hepatitis C virus related liver disease.National consensus guideline in Hungary

Author:

Hunyady Béla12,Gerlei Zsuzsanna3,Gervain Judit4,Horváth Gábor5,Lengyel Gabriella6,Pár Alajos2,Rókusz László7,Szalay Ferenc8,†Telegdy László9,Tornai István10,Werling Klára6,Makara Mihály9

Affiliation:

1. Somogy Megyei Kaposi Mór Oktató Kórház Belgyógyászati Osztály Kaposvár Tallián Gy. u. 20–32. 7400

2. Pécsi Tudományegyetem, Általános Orvostudományi Kar I. Belgyógyászati Klinika Pécs

3. Semmelweis Egyetem, Általános Orvostudományi Kar Transzplantációs és Sebészeti Klinika Budapest

4. Szent György Egyetemi Oktató Kórház I. Belgyógyászat és Molekuláris Diagnosztikai Laboratórium Székesfehérvár

5. Szent János Kórház és Észak-budai Egyesített Kórházak Hepatológiai Szakrendelés Budapest

6. Semmelweis Egyetem, Általános Orvostudományi Kar II. Belgyógyászati Klinika Budapest

7. MH Egészségügyi Központ Honvédkórház I. Belgyógyászati Osztály Budapest

8. Semmelweis Egyetem, Általános Orvostudományi Kar I. Belgyógyászati Klinika Budapest

9. Egyesített Szent István és Szent László Kórház Budapest

10. Debreceni Egyetem, Általános Orvostudományi Kar, Orvos- és Egészségtudományi Centrum Belgyógyászati Intézet Debrecen

Abstract

Approximately 70,000 people are infected with hepatitis C virus in Hungary, and more than half of them are not aware of their infection. From the point of infected individuals early recognition and effective treatment of related liver injury may prevent consequent advanced liver diseases and complications (liver cirrhosis, liver failure and liver cancer) and can increase work productivity and life expectancy. Furthermore, these could from prevent further spread of the virus as well as reduce substantially long term financial burden of related morbidity, as a socioeconomic aspect. Pegylated interferon + ribavirin dual therapy, which is available in Hungary since 2003, can clear the virus in 40–45% of previously not treated (naïve), and in 5–21% of previous treatment-failure patients. Addition of a direct acting first generation protease inhibitor drug (boceprevir or telaprevir) to the dual therapy increases the chance of sustained viral response to 63–75% and 59–66%, respectively. These two protease inhibitors are available and financed for a segment of Hungarian patients since May 2013. Between 2013 and February 2015, other direct acting antivirals and interferon-free combination therapies have been registered for the treatment of chronic hepatitis C with a potential efficacy over 90% and typically with a short duration of 8–12 weeks. Indication of therapy includes exclusion of contraindications to the drugs and demonstration of viral replication with consequent liver injury, i.e., inflammation and/or fibrosis in the liver. Non-invasive methods (elastography and biochemical methods) are accepted and preferred for staging liver damage (fibrosis). For initiation of treatment accurate and timely molecular biology tests are mandatory. Eligibility for treatment is a subject of individual central medical review. Due to budget limitations therapy is covered only for a proportion of patients by the National Health Insurance Fund. Priority is given to those with urgent need based on a Hungarian Priority Index system reflecting primarily the stage of liver disease, and considering also additional factors, i.e., activity and progression of liver disease, predictive factors of treatment and other special issues. Approved treatments are restricted to the most cost-effective combinations based on the cost per sustained viral response value in different patient categories with consensus between professional organizations, National Health Insurance Fund and patient organizations. More expensive therapies might be available upon co-financing by the patient or a third party. Interferon-free treatments and shorter therapy durations preferred as much as financially feasible. A separate budget is allocated to cover interferon-free treatments for the most-in-need interferon ineligible/intolerant patients, and for those who have no more interferon-based therapy option. Orv. Hetil., 2015, 156(9), 343–351.

Publisher

Akademiai Kiado Zrt.

Subject

General Medicine

Reference24 articles.

1. Barna, T. K., Ozsvár, Z., Szendrényi, V., et al.: Hepatitis C virus antibody in the serum of blood donors. [Hepatitis C-vírus ellenanyag előfordulása véradók szérumában.] Orv. Hetil., 1996, 137(10), 507–511. [Hungarian]

2. Gervain, J., Simon, G. Jr., Papp, I., et al.: Analysing the type and subtype of hepatitis virus C of chronic viral hepatitis patients in Hungary. [A magyarországi krónikus “C” vírushepatitises betegek vírustípus- és szubtípus-meghatározása.] Orv. Hetil., 2001, 142(25), 1315–1319. [Hungarian]

3. Van der Meer, A. J., Veldt, B. J., Feld, J. J., et al.: Association between sustained virological response and all-cause mortality among patients with chronic hepatitis C and advanced hepatic fibrosis. JAMA, 2012, 308(24), 2584–2593.

4. Makara, M., Horváth, G., Szalay, F., et al.: Organizational characteristics of treatment for chronic hepatitis in Hungary: Hepatitis Registry and Priority Index. [A krónikus vírushepatitisek hazai ellátási rendszerének sajátosságai: Hepatitis Regiszter és a Prioritási Index.] Orv. Hetil., 2013, 154(29), 1151–1155. [Hungarian]

5. European Medicines Agency: Pegasys. Instructions for use. [Pegasys. Alkalmazási előírás.] http://www.ema.europa.eu/docs/hu_HU/document_library/EPAR_-_Product_Information/human/000395/WC500039195.pdf

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