External validation of models to predict hepatocellular carcinoma in Hepatitis C Virus cured F3-F4 patients

Ângela Carvalho-Gomes; Tsveta Vladi Valcheva Valcheva; Iván Sahuco; Enrique Vidal; Laura Martínez-Arenas; Carmen Vinaixa; Victoria Aguilera; Sónia García García; Marina Berenguer

doi:10.1002/ueg2.12571

External validation of models to predict hepatocellular carcinoma in Hepatitis C Virus cured F3-F4 patients

United European Gastroenterol J. 2024 May 8. doi: 10.1002/ueg2.12571. Online ahead of print.

Authors

Ângela Carvalho-Gomes^{1

2}, Tsveta Vladi Valcheva Valcheva^{1

3}, Iván Sahuco¹, Enrique Vidal^{4

5}, Laura Martínez-Arenas^{1

2

6}, Carmen Vinaixa^{1

2

7}, Victoria Aguilera^{1

2

7}, Sónia García García⁷, Marina Berenguer^{1

2

3

7}

Affiliations

¹ Hepatology, Hepatobiliopancreatic Surgery and Transplant Group, La Fe Health Research Institute (IIS La Fe), Valencia, Spain.
² National Institute for the Study of Liver and Gastrointestinal Diseases, CIBEREHD, Instituto de Salud Carlos III (ISCIII), Madrid, Spain.
³ Medicine Department, University of Valencia, Valencia, Spain.
⁴ Laboratory of Cellular and Molecular Biology, Health Research Institute Hospital La Fe, Valencia, Spain.
⁵ Clinical and Translational Research in Cancer, Health Research Institute Hospital La Fe, Valencia, Spain.
⁶ Department of Biotechnology, Universitat Politècnica de València, Valencia, Spain.
⁷ Department of Gastroenterology, Hepatology Unit, La Fe University Hospital, Valencia, Spain.

PMID: 38720450
DOI: 10.1002/ueg2.12571

Abstract

Background & aims: Several hepatocellular carcinoma (HCC) risk-models have been developed to individualise patient surveillance following sustained viral response (SVR) in Hepatitis C Virus patients. Validation of these models in different cohorts is an important step to incorporate a more personalised risk assessment in clinical practice. We aimed at applying these models to stratify the risk in our patients and potentially determine cost-saving associated with individualised HCC risk-stratification screening strategy.

Methods: Patients with baseline F3-4 fibrosis treated with new oral direct-acting antivirals who had reached a SVR were regularly followed as part of the HCC surveillance strategy. Six models were applied: Pons, aMAP, Ioannou, HCC risk, Alonso and Semmler. Validation of the models was performed based on sensitivity and the proportion of patients labelled as "high risk".

Results: After excluding 557 with less than 3 fibrosis, 12 without SVR, 18 with a follow up (FU) <1 year, 17 transplant recipients, 16 lost to FU and 31 with HCC at time of antiviral therapy, our cohort consisted of 349 F3-4 SVR patients. Twenty-three patients (6.6%) developed HCC after a median FU of 5.12 years. The sensitivity of the different models varied between 0.17 (Semmler7noalcohol) and 1 (Alonso A and aMAP). The lowest proportion of high-risk patients corresponded to the Semmler-noalcohol model (5%). Sixty-three and 90% of the Alonso A and aMAP patients, respectively were labelled as high risk. The most reliable HCC risk-model applied to our cohort to predict HCC development is the Alonso model (based on fibrosis stage assessed by liver stiffness measurements or Fibrosis-4 index (FIB-4) at baseline and after 1 year, and albumin levels at 1 year) with a-100% sensitivity in detecting HCC among those at high risk and 63% labelled as high risk. The application of the model would have saved the cost of 1290 ultrasound no longer being performed in the 37% low-risk group.

Conclusion: In our cohort, the Alonso A model allows the most reliable reduction in HCC screening resulting in safely stopping life-long monitoring in about a third of F3-F4 patients achieving SVR with DAAs.

Keywords: HCC‐models; Hepatitis C Virus; hepatocellular carcinoma; patient monitoring; sustained viral response.

Abstract

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