Downregulation of Hepatic Stem Cell Factor by Vivo-Morpholino Treatment Inhibits Mast Cell Migration and Decreases Biliary Damage/senescence and Liver Fibrosis in Mdr2 Mice

Overview

Journal Biochim Biophys Acta Mol Basis Dis

Publisher Elsevier

Specialties Biochemistry
Biophysics
Genetics
Molecular Biology

Date 2019 Sep 16

PMID 31521820

Citations 23

Authors

Vik Meadows

Lindsey Kennedy

Laura Hargrove

Jennifer Demieville

Fanyin Meng

Shohaib Virani

Evan Reinhart

Konstantina Kyritsi

Pietro Invernizzi

Zhihong Yang

Nan Wu

Suthat Liangpunsakul

Gianfranco Alpini

Heather Francis

Affiliations

Soon will be listed here.

Abstract

Methods: FVB/NJ and Mdr2 mice were treated with Mismatch or SCF Vivo-Morpholinos. We measured (i) SCF expression and secretion; (ii) hepatic damage; (iii) MC migration/activation and histamine signaling; (iv) ductular reaction and biliary senescence; and (v) hepatic fibrosis. In human PSC patients, SCF expression and secretion were measured. In vitro, cholangiocytes were evaluated for SCF expression and secretion. Biliary proliferation/senescence was measured in cholangiocytes pretreated with 0.1% BSA or the SCF inhibitor, ISK03. Cultured HSCs were stimulated with cholangiocyte supernatant and activation measured. MC migration was determined with cholangiocytes pretreated with BSA or ISK03 loaded into the bottom of Boyden chambers and MCs into top chamber.

Results: Biliary SCF expression and SCF serum levels increase in human PSC. Cholangiocytes, but not hepatocytes, from SCF Mismatch Mdr2 mice have increased SCF expression and secretion. Inhibition of SCF in Mdr2 mice reduced (i) hepatic damage; (ii) MC migration; (iii) histamine and SCF serum levels; and (iv) ductular reaction/biliary senescence/hepatic fibrosis. In vitro, cholangiocytes express and secrete SCF. Blocking biliary SCF decreased MC migration, biliary proliferation/senescence, and HSC activation.

Conclusion: Cholangiocytes secrete increased levels of SCF inducing MC migration, contributing to biliary damage/hepatic fibrosis. Targeting MC infiltration may be an option to ameliorate PSC progression.

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