HEPATOCELLULAR CARCINOMA AFTER DIRECT ANTIVIRAL AGENTS FOR HEPATITIS C IN PATIENTS WITH DECOMPENSATED CIRRHOSIS

Higuera-de-la-Tijera, F-; Flores-García, N.C.; Kershenobich, D.; Cerda-Reyes, E.; González-Huezo, M.S.; Pérez-Hernández, J.L.; Méndez-Sánchez, N.; Morales-Gutiérrez, O.; Lira-Vera, J.E.; Alagón-Fernández-del-Campo, P.; Vargas-Durán, F.Y.; Soto-Martínez, K.; Guerrero-Avendaño, G.M.L.; Servín-Caamaño, A.; Gándara-Calderón, J.G.; García-Domínguez, D.; Díaz-Orozco, L.E.; García-Casarreal, N.; Mejía-Loza, S.; Lázaro-Pacheco, I.B.; Rodríguez-Fuentes, E.

doi:10.1016/j.aohep.2021.100607

ISSN: 1665-2681

Annals of Hepatology (AoH) is an international, open access journal published bi-monthly with funds from the Fundación Clínica Médica Sur. It is the official journal of the Mexican Association of Hepatology (AMH), the Latin American Association for the Study of the Liver (ALEH), the Canadian Association for the Study of the Liver (CASL) and the Czech Society of Hepatology (CSH). AoH publishes editorials, opinions, concise reviews, original articles, brief reports, letters to the editor, news from affiliated associations, clinical practice guidelines and summaries of congresses in the field of Hepatology.

Topics covered by AoH include alcoholic liver disease, autoimmune hepatitis, biliary diseases, drug-induced liver injury, genetic liver diseases, NAFLD/NASH and viral hepatitis (HAV, HBV, HCV, HDV, HEV). Our journal seeks to publish articles on basic clinical care and translational research focused on preventing rather than treating the complications of end-stage liver disease.

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F- Higuera-de-la-Tijera1N.C. Flores-García2D. Kershenobich2E. Cerda-Reyes3M.S. González-Huezo4J.L. Pérez-Hernández1,5N. Méndez-Sánchez6O. Morales-Gutiérrez1J.E. Lira-Vera1P. Alagón-Fernández-del-Campo1F.Y. Vargas-Durán1K. Soto-Martínez1G.M.L. Guerrero-Avendaño1A. Servín-Caamaño1J.G. Gándara-Calderón3D. García-Domínguez4L.E. Díaz-Orozco6N. García-Casarreal7S. Mejía-Loza8I.B. Lázaro-Pacheco9E. Rodríguez-Fuentes1

1 Hospital General de México "Dr. Eduardo Liceaga". Ciudad de México, México

2 Instituto Nacional de Ciencias Médicas y Nutrición “Salvador Zubirán”. Ciudad de México, México

3 Hospital central militar. Ciudad de México, México

4 Centro Médico ISSEMyM Metepec, Edo. de México, México

5 Hospital Central Sur, PEMEX. Ciudad de México, México

6 Fundación Clínica Médica Sur. Ciudad de México, México

7 Hospital Regional 1° de Octubre, ISSSTE. Ciudad de México, México

8 Hospital Juárez de México. Ciudad de México, México

9 ISSSTE Oaxaca. Oaxaca, México

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Table 1. Risk factors related to the development of HCC after DAA in decompensated cirrhosis with hepatitis C infection

Special issue

This article is part of special issue:

Vol. 27. Issue S2

Oral presentations at the XVI National Congress of the Mexican Association of Hepatology

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Introduction and Objectives

If direct antiviral agents (DAA) are related to the development of HCC is controversial; therefore, exploring risk factors are crucial. We aimed to determine factors related to the development of hepatocellular carcinoma (HCC) in patients with hepatitis c (HCV) and decompensated cirrhosis (DC) treated with DAA.

Materials and Methods

A multicenter real-world cohort study including patients with HCV + DC treated with sofosbuvir (SOF) based on regimens free of inhibitors of protease (IPs).

Results

222 patients, 118 (53.2%) were women, mean age 57.2 ±11.5-year-old, 209 (94.1%) achieved sustained virological response (SVR). According to Child-Pugh 44(19.8%) were A with history of any clinical decompensation event, 147(66.2%) B, and 31 (14%) C. After DAA, 134 (60.4%) improve in MELD, 45 (20.3%) had no change, and 43 (19.4%) worse, this worse in MELD was related to non-SVR [SVR 37/209 (17.7%) vs. non-SVR 6/13 (46.2%); OR=2.6, 95%CI:1.4-5.0, p=0.02]. Nineteen (8.6%) developed HCC during the follow-up after therapy with DAA; however, when we compared basal laboratory values between those who developed HCC and those who did not only alfa-fetoprotein (AFP) levels were different (without HCC 14.3 [mean 95%CI: 10.6-18.1] ng/mL vs. HCC 55.7 [mean 95%CI: 28.4-83.0] ng/mL; p<0.006). Univariate and multivariate analyses are shown in Table 1.

Discussion

Our study confirms that rather than DAA therapy, the most critical factors related to the development of HCC in DC patients with HCV treated with DAA, are non-achieve SVR and, most important basal AFP levels > 20ng/mL, it is essential to note that patients in this cohort had no any suspicious lesion in ultrasonography (USG) previous to start DAA therapy in their semestral screening as most of the guidelines recommend. AASLD, for example, recommends semestral HCC screening with USG with or without AFP, giving more weight to the imagen study. However, based on our results, we recommend always determining AFP levels as a compliment to USG.

Conclusions

In HCV patients with DC treated with DAA and with a negative basal screening USG for suspicious malignant lesions, basal AFP > 20ng/mL are the most critical factor related to the development of HCC and should be determined complementary to the USG study.

The authors declare that there is no conflict of interest.

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