Pro-fibrotic compounds induce stellate cell activation, ECM-remodelling and Nrf2 activation in a human 3D-multicellular model of liver fibrosis

Prestigiacomo, Vincenzo; Weston, Anna; Messner, Simon; Lampart, Franziska; Suter-Dick, Laura

Pro-fibrotic compounds induce stellate cell activation, ECM-remodelling and Nrf2 activation in a human 3D-multicellular model of liver fibrosis

Dateien

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Autor:innen

Prestigiacomo, Vincenzo

Autor:in (Körperschaft)

Publikationsdatum

30.06.2017

Typ der Arbeit

Studiengang

Sammlung

Institut für Chemie und Bioanalytik

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Typ

01A - Beitrag in wissenschaftlicher Zeitschrift

Herausgeber:innen

Herausgeber:in (Körperschaft)

Betreuer:in

Übergeordnetes Werk

PLOS ONE

Themenheft

DOI der Originalpublikation

https://doi.org/10.1371/journal.pone.0179995

URI

https://irf.fhnw.ch/handle/11654/52242
https://doi.org/10.26041/fhnw-13250

Link

Reihe / Serie

Reihennummer

Jahrgang / Band

12

Ausgabe / Nummer

6

Seiten / Dauer

Patentnummer

Verlag / Herausgebende Institution

Public Library of Science

Verlagsort / Veranstaltungsort

Auflage

Version

Programmiersprache

Abtretungsempfänger:in

Praxispartner:in/Auftraggeber:in

Zusammenfassung

Background & Aims Currently most liver fibrosis research is performed in vivo, since suitable alternative in vitro systems which are able to recapitulate the cellular events leading to liver fibrosis are lacking. Here we aimed at generating a system containing cells representing the three key players of liver fibrosis (hepatocyte, Kupffer cells and stellate cells) and assess their response to pro-fibrotic compounds such as TGF-β1, methotrexate (MTX) and thioacetamide (TAA). Methods Human cell lines representing hepatocytes (HepaRG), Kupffer cell (THP-1 macrophages) and stellate cells (hTERT-HSC) were co-cultured using the InSphero hanging drop technology to generate scaffold-free 3D microtissues, that were treated with pro-fibrotic compounds (TGF-β1, MTX, TAA) for up to 14 days. The response of the microtissues was evaluated by determining the expression of cytokines (TNF-α, TGF-β1 and IL6), the deposition and secretion of ECM proteins and induction of gene expression of fibrosis biomarkers (e.g. αSMA). Induction of Nrf2 and Keap1, as key player of defence mechanism, was also evaluated. Results We could demonstrate that the multicellular 3D microtissue cultures could be maintained in a non-activated status, based on the low expression levels of activation markers. Macrophages were activated by stimulation with LPS and hTERT-HSC showed activation by TGF-β1. In addition, MTX and TAA elicited a fibrotic phenotype, as assessed by gene-expression and protein-deposition of ECM proteins such as collagens and fibronectin. An involvement of the antioxidant pathway upon stimulation with pro-fibrotic compounds was also observed. Conclusion Here, for the first time, we demonstrate the in vitro recapitulation of key molecular and cellular events leading to liver fibrosis: hepatocellular injury, antioxidant defence response, activation of Kupffer cells and activation of HSC leading to deposition of ECM.

Schlagwörter

Fachgebiet (DDC)

600 - Technik, Medizin, angewandte Wissenschaften

Projekt

Veranstaltung

Startdatum der Ausstellung

Enddatum der Ausstellung

Startdatum der Konferenz

Enddatum der Konferenz

Datum der letzten Prüfung

ISBN

ISSN

1932-6203

Sprache

Englisch

Während FHNW Zugehörigkeit erstellt

Ja

Zukunftsfelder FHNW

Publikationsstatus

Veröffentlicht

Begutachtung

Fachlektorat/Editorial Review

Open Access-Status

Gold

Lizenz

Zitation

Prestigiacomo, V., Weston, A., Messner, S., Lampart, F., & Suter-Dick, L. (2017). Pro-fibrotic compounds induce stellate cell activation, ECM-remodelling and Nrf2 activation in a human 3D-multicellular model of liver fibrosis. Plos One, 12(6). https://doi.org/10.1371/journal.pone.0179995

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