No evidence of association between inherited thrombophilia and increased risk of liver fibrosis

Author:

Ezcurra Iranzu1,Puente Ángela1,Cuadrado Antonio1,Tamayo Ibai2,Iruzubieta Paula1,Arias‐Loste María Teresa1,González Francisco José3,Pellón Raúl3,Sánchez Sara3,Crespo Juan3,Acebo Mercedes3,López‐Hoyos Marcos4,Pérez Rocío5,Cuesta Amalia5,Antón Ángela1,Echavarría Víctor1,Fábrega Emilio1ORCID,Crespo Javier1,Fortea Jose Ignacio1ORCID

Affiliation:

1. Gastroenterology and Hepatology Department Clinical and Translational Research in Digestive Diseases Valdecilla Research Institute (IDIVAL) Marqués de Valdecilla University Hospital Santander Spain

2. Navarrabiomed Health Research Institute Pamplona Spain

3. Radiology Department Hospital Universitario Marqués de Valdecilla Santander Spain

4. Inmunology Department Hospital Universitario Marqués de Valdecilla IDIVAL Santander Spain

5. Hematology Department Hospital Universitario Marqués de Valdecilla Santander Spain

Abstract

AbstractBackgroundPreliminary evidence suggests that inherited hypercoagulable disorders can lead to an increased risk of significant liver fibrosis.ObjectiveWe aimed to investigate the prevalence of significant fibrosis in patients with inherited thrombophilia, assessed by using liver stiffness (LS), and to compare this prevalence to that found in a large population‐based cohort from the same region.MethodsThis was a single‐center, cross‐sectional study. A complete laboratory analysis for liver disease, LS by transient elastography and an abdominal ultrasound were performed in patients with inherited thrombophilia diagnosed between May 2013‐February 2017. These patients were propensity score matched (ratio 1:4) with a population‐based cohort from the same region (PREVHEP‐ETHON study; NCT02749864; N = 5988).ResultsOf 241 patients with inherited thrombophilia, eight patients (3.3%) had significant fibrosis (LS ≥8 kPa). All of them had risk factors for liver disease and met diagnostic criteria for different liver diseases. After matching 221 patients with thrombophilia with 884 patients of the PREVHEP‐ETHON cohort, the prevalence of significant fibrosis was similar between both cohorts (1.8% vs. 3.6%, p = 0.488). Multivariate analysis showed that age and liver disease risk factors, but not belonging to the thrombophilia cohort, were associated with the presence of significant fibrosis. The magnitude of the increased risk of significant fibrosis in patients with risk factors for liver disease was also similar in both cohorts.ConclusionsOur findings do not provide evidence supporting an association between inherited thrombophilia and an increased risk of significant liver fibrosis, independent of the presence of liver‐related causes of fibrosis.

Funder

Instituto de Salud Carlos III

Publisher

Wiley

Subject

Gastroenterology,Oncology

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