Hepatology Communications (Aug 2021)

Cluster of Differentiation 44 Promotes Liver Fibrosis and Serves as a Biomarker in Congestive Hepatopathy

  • Yosuke Osawa,
  • Hironari Kawai,
  • Tomoyuki Tsunoda,
  • Haruki Komatsu,
  • Miku Okawara,
  • Yuriko Tsutsui,
  • Yuichi Yoshida,
  • Shiori Yoshikawa,
  • Taizo Mori,
  • Taiji Yamazoe,
  • Sachiyo Yoshio,
  • Takashi Oide,
  • Ayano Inui,
  • Tatsuya Kanto

DOI
https://doi.org/10.1002/hep4.1721
Journal volume & issue
Vol. 5, no. 8
pp. 1437 – 1447

Abstract

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Congestive hepatopathy (CH) with chronic passive congestion is characterized by the progression of liver fibrosis without prominent inflammation and hepatocellular damage. Currently, the lack of reliable biomarkers for liver fibrosis in CH often precludes the clinical management of patients with CH. To explore fibrosis biomarkers, we performed proteome analysis on serum exosomes isolated from patients with CH after the Fontan procedure. Exosomal cluster of differentiation (CD)44 levels were increased in patients with CH compared to healthy volunteers and was accompanied by increases in serum levels of soluble CD44 and CD44 expression in the liver. To address the roles of CD44 in CH, we established a mouse model of chronic liver congestion by partial inferior vena cava ligation (pIVCL) that mimics CH by fibrosis progression with less inflammation and cellular damage. In the pIVCL mice, enhanced CD44 expression in hepatic stellate cells (HSCs) and deposition of its ligand hyaluronan were observed in the liver. Blood levels of soluble CD44 were correlated with liver fibrosis. The blockade of CD44 with specific antibody inhibited liver fibrosis in pIVCL mice and was accompanied by a reduction in S100 calcium‐binding protein A4 expression following activation of HSCs. Conclusion: Chronic liver congestion promotes fibrosis through CD44. This identifies CD44 as a novel biomarker and therapeutic target of liver fibrosis in patients with CH.