Fibulin‐4 as a potential extracellular vesicle marker of fibrosis in patients with cirrhosis

Author:

Kumagai Masaru1,Tsuchiya Atsunori12ORCID,Yang Yuan13,Takeda Nobutaka1,Natsui Kazuki1,Natusi Yui1,Tomiyoshi Kei1,Yamazaki Fusako1,Koseki Yohei1,Shinchi Hiroki4,Imawaka Naoko5,Ukekawa Ryo5,Nishibu Takahiro5,Abe Hiroyuki1,Sasaki Takako6,Ueda Koji4,Terai Shuji12ORCID

Affiliation:

1. Division of Gastroenterology and Hepatology, Graduate School of Medical and Dental Sciences Niigata University Japan

2. Future Medical Research Center for Exosome and Designer Cells (F‐DEC) Niigata University Japan

3. Department of Gastroenterology, Digestive Disease Hospital Affiliated Hospital of Zunyi Medical University China

4. Project for Realization of Personalized Cancer Medicine, Cancer Precision Medicine Center Japanese Foundation for Cancer Research Tokyo Japan

5. Biotechnology Center, R&D Marketing Operations FUJIFILM Wako Pure Chemical Corporation Amagasaki‐shi Japan

6. Department of Pharmacology, Faculty of Medicine Oita University Yufu Japan

Abstract

Chronic liver injury leads to decreased liver function and increased fibrosis. Fibrosis is not only associated with the development of portal hypertension and carcinogenesis, but with the occurrence of events and a poor prognosis, highlighting the importance of non‐invasive fibrosis assessment in patients. In the present study, we searched for markers related to liver fibrosis via proteomic analysis of small extracellular vesicles (sEVs). In the discovery cohort, proteomic analysis was carried out in the sEVs extracted from the sera of 5 patients with decompensated cirrhosis, 5 patients with compensated cirrhosis, and 5 controls without liver disease. Interestingly, in this cohort, fibulin‐4 was significantly associated with cirrhosis while in the validation cohort [formed by 191 patients: 7 patients without disease, 16 patients without liver disease (other diseases), 38 patients with chronic liver disease (CLD), 75 patients with cirrhosis of Child–Pugh class A (36 without hepatocellular carcinoma [HCC], 29 with HCC), and 65 patients with cirrhosis of Child–Pugh class B–C (39 without HCC, 26 with HCC)], fibulin‐4/CD9 levels increased with cirrhosis progression. Furthermore, the fibulin‐4/CD9 ratio was significantly higher in patients with varices. Immunostaining also revealed strong fibulin‐4 expression in cholangiocytes within the fibrous areas and mesothelial cells in liver tissue blood vessels. Taken together, our results suggest that fibulin‐4, essential for lysyl oxidase activation, might be a new liver fibrosis marker found in the sEVs of patients with cirrhosis.

Publisher

Wiley

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