Metabolomics in liver diseases: A novel alternative for liver biopsy?

Author:

Tanaka Yasuo

Abstract

Hepatitis C virus (HCV) remains a significant public health problem as it can cause acute and chronic hepatitis. Chronic HCV infection is a major cause of liver fibrosis, and evaluation of liver fibrosis is essential because the prognosis of patients with chronic HCV infection is closely related to the stage of fibrosis. Liver fibrosis is traditionally evaluated based on pathological analysis of biopsy specimens, which is considered the gold standard. Nevertheless, liver biopsy is invasive and susceptible to sampling error and inter- and intraobserver variation in pathological interpretation; it is also costly. Therefore, noninvasive diagnostic investigations have been developed, including the use of fibrotic markers, scoring systems based on routine blood tests, and transient elastography with magnetic resonance imaging or ultrasonography. Recently, metabolomics, an emerging technology, has been used to detect the fibrosis stage. In this editorial, I comment on the article titled “Metabolomics in chronic hepatitis C: Decoding fibrosis grading and underlying pathways” by Ferrasi et al published in the recent issue of the World Journal of Hepatology . I discuss previous studies on the use of metabolome analysis for the diagnosis of HCV-related liver fibrosis and the potential development of biopsy-free diagnostic techniques.

Publisher

Baishideng Publishing Group Inc.

Subject

Hepatology

Reference20 articles.

1. World Health Organization. Global hepatitis report 2017. World Health Organization 2017; ISBN: 978-92-4-156545-5

2. Liver fibrosis

3. Liver cirrhosis

4. Hepatocellular carcinoma in cirrhosis: Incidence and risk factors

5. Liver biopsy: The best, not the gold standard

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