Models and methods for in vitro testing of hepatic gap junctional communication

Michaël Maes, Sara Crespo Yanguas, Joost Willebrords, Mathieu Vinken

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11 Citations (Scopus)

Abstract

Inherent to their pivotal roles in controlling all aspects of the liver cell life cycle, hepatocellular gap junctions are frequently disrupted upon impairment of the homeostatic balance, as occurs during liver toxicity. Hepatic gap junctions, which are mainly built up by connexin32, are specifically targeted by tumor promoters and epigenetic carcinogens. This renders inhibition of gap junction functionality a suitable indicator for the in vitro detection of nongenotoxic hepatocarcinogenicity. The establishment of a reliable liver gap junction inhibition assay for routine in vitro testing purposes requires a cellular system in which gap junctions are expressed at an in vivo-like level as well as an appropriate technique to probe gap junction activity. Both these models and methods are discussed in the current paper, thereby focusing on connexin32-based gap junctions.
Original languageEnglish
Pages (from-to)569-577
JournalToxicology in Vitro
Volume30
Issue number1
Early online date26 Sep 2015
DOIs
Publication statusPublished - 1 Dec 2015

Keywords

  • gap junction
  • connexin
  • liver
  • in vitro model
  • nongenotoxic carcinogen
  • intercellular communication

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  • Connexins and pannexins in liver damage

    Crespo Yanguas, S., Willebrords, J., Maes, M., da Silva, T. C., Alves Pereira, I. V., Cogliati, B., Zaidan Dagli, M. L. & Vinken, M., 18 Feb 2016, In: EXCLI Journal. 15, p. 177-186 10 p.

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