Abstract

Although long regarded as the gold standard for liver fibrosis staging in chronic hepatitis C (CHC), liver biopsy (LB) implies both the risk of an invasive procedure and significant variability. The aim of this study was to evaluate the diagnostic performance for transient elastography (TE) and aspartate aminotransferase to platelet index (APRI) used alone and in combination compared to liver biopsy and to analyze false positive/negative results. Patients with CHC, and no previous clinical diagnosis of cirrhosis were enrolled to undergo liver biopsy, TE and APRI. A total of 182 adult patients with a median age of 55 years and median body mass index of 26.71 kg/m2 were analyzed. On LB, 56% of patients had significant levels of fibrosis (METAVIR F≥2) and 28% had advanced fibrosis (F3/F4). The strongest performance for both tests was observed for exclusion of advanced fibrosis with good negative predictive values (89 and 86%, respectively). Low necroinflammatory activity on LB was associated with false negative TE. False positives were associated with NASH and smaller LB fragments. Correlation between APRI and Fibroscan for F≥2 was 100% and 84% for F≥3 and remained high in both false negative and false positive instances, correctly identifying F<2 in 71% of cases and F<3 in 78% (and potentially foregoing up to 84% of LB). We concluded that low individual performance indicators could be attributable to limitations of LB. Poorer differentiation of lower levels of fibrosis is a known issue for LB and remains so for noninvasive tests. Good predictability is possible, however, for advanced fibrosis.

Highlights

  • Liver fibrosis (LF) staging is an important component of chronic hepatitis C (CHC) management

  • We present a prospective cross-sectional study aimed to evaluate the performance of two noninvasive LF staging tests individually and combined, in an outpatient CHC population in Brazil comprising 30% of patients with advanced fibrosis

  • Among different technologies for noninvasive LF staging, liver stiffness (LS) determination using transient elastography (TE) has been extensively investigated in recent years [10,16,21] and was elected as one of the objects of our study

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Summary

Introduction

Liver fibrosis (LF) staging is an important component of chronic hepatitis C (CHC) management. In an attempt to overcome potential risks and expand access and eligibility in LF staging, several noninvasive approaches have been developed [5,6,7,8], some relying on analysis of physical changes associated with liver fibrosis, such as elastography, and others on biochemical markers and scoring systems ranging from isolated platelet counts [9] to more elaborate indexes, such as Fibrotests, Fibrometers, and Hepascores These indexes have variable diagnostic performances [10,11,12], usually with stronger predictability for advanced fibrosis and cirrhosis when

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