Bile salts regulate CYP7A1 expression and elicit a fibrotic response and abnormal lipid production in 3D liver microtissues

Messner, Catherine Jane; Mauch, Linda; Suter-Dick, Laura

Bile salts regulate CYP7A1 expression and elicit a fibrotic response and abnormal lipid production in 3D liver microtissues

Autor:innen

Messner, Catherine Jane

Mauch, Linda

Suter-Dick, Laura

Autor:in (Körperschaft)

Publikationsdatum

10.2019

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

Toxicology in Vitro

Themenheft

DOI der Originalpublikation

https://doi.org/10.1016/j.tiv.2019.06.002

URI

https://irf.fhnw.ch/handle/11654/51623

Link

Reihe / Serie

Reihennummer

Jahrgang / Band

60

Ausgabe / Nummer

Seiten / Dauer

261-271

Patentnummer

Verlag / Herausgebende Institution

Elsevier

Verlagsort / Veranstaltungsort

Auflage

Version

Programmiersprache

Abtretungsempfänger:in

Praxispartner:in/Auftraggeber:in

Zusammenfassung

Disrupted regulation and accumulation of bile salts (BS) in the liver can contribute towards progressive liver damage and fibrosis. Here, we investigated the role of BS in the progression of cholestatic injury and liver fibrosis using 3D scaffold-free multicellular human liver microtissues (MTs) comprising the cell lines HepaRG, THP-1 and hTERT-HSCs. This in vitro model has been shown to recapitulate cellular events leading to fibrosis including hepatocellular injury, inflammation and activation of HSCs, ultimately leading to increased deposition of extracellular matrix (ECM). In order to better differentiate the contribution of individual cells during cholestasis, the effects of BS were evaluated either on each of the three cell types individually or on the multicellular MTs. Our data corroborate the toxic effects of BS on HepaRG cells and indicate that BS exposure elicited a slight increase in cytokines without causing stellate cell activation. Contrarily, using the MTs, we could demonstrate that low concentrations of BS led to cellular damage and triggered a fibrotic response. This indicates that cellular interplay is required to achieve BS-triggered activation of HSC. Moreover, BS were capable of down-regulating CYP7A1 expression in MTs and elicited abnormal lipid production (accumulation) concordant with clinical cases where chronic cholestasis results in hypercholesterolemia.

Schlagwörter

Fachgebiet (DDC)

500 - Naturwissenschaften und Mathematik

Projekt

Veranstaltung

Startdatum der Ausstellung

Enddatum der Ausstellung

Startdatum der Konferenz

Enddatum der Konferenz

Datum der letzten Prüfung

ISBN

ISSN

0887-2333
1879-3177

Sprache

Englisch

Während FHNW Zugehörigkeit erstellt

Ja

Zukunftsfelder FHNW

Publikationsstatus

Veröffentlicht

Begutachtung

Peer-Review der ganzen Publikation

Open Access-Status

Closed

Lizenz

Zitation

Messner, C. J., Mauch, L., & Suter-Dick, L. (2019). Bile salts regulate CYP7A1 expression and elicit a fibrotic response and abnormal lipid production in 3D liver microtissues. Toxicology in Vitro, 60, 261–271. https://doi.org/10.1016/j.tiv.2019.06.002

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