Literature DB >> 24117459

Cadmium disorganises the scaffolding of gap and tight junction proteins in the hepatic cell line WIF B9.

Sylviane Boucherie1, Catherine Decaens, Jean-Marc Verbavatz, Brigitte Grosse, Marie Erard, Fabienne Merola, Doris Cassio, Laurent Combettes.   

Abstract

BACKGROUND INFORMATION: Hepatocytes, which perform the main functions of the liver, are particularly vulnerable to toxic agents such as cadmium, an environmental pollutant. To identify the molecular targets for cadmium in hepatocytes, we have studied the effects of CdCl2 on the hybrid cell line WIF-B9 that exhibits stable structural and functional hepatocytic polarity.
RESULTS: We showed that the toxicity of CdCl2 (1 µM, 24 h) resulted in a reduction in direct intercellular communication (via gap junctions) and in an increase in paracellular permeability (decrease in the sealing of tight junctions). These effects were not related to changes in the expression of the key proteins involved, Cx32 and claudin 2, the first being constitutive of gap junctions and the second of tight junctions in this cell line. Using immunofluorescence experiments, we observed a change in the location of Cx32 and claudin 2: these two proteins were less often found in the tight junction network that closes the bile canaliculi (BC). In control cells, 'Proximity Ligation Assay' (PLA Duolink®) has confirmed in situ that molecules of claudin 2 and Cx32 are very close to each other at the BC (probably less than 16 nm). This was no longer the case after treatment with CdCl2 . Localisation of occludin and Cx32 relative to each other was not modified by CdCl2 , but CdCl2 increased the PLA signal between molecules of JAM-A and Cx32. Finally, examination of freeze-fracture replicas obtained from cultures treated with CdCl2 showed the disruption of the network of tight junctions and the depletion or the disintegration of the junctional plaques associated with tight junctions.
CONCLUSIONS: This study demonstrates in situ the changes induced by cadmium on the organisation of cell-cell junctions and points out the importance of the association Cx32/claudin 2 for the maintenance of normal hepatocyte functions.
© 2013 Société Française des Microscopies and Société de Biologie Cellulaire de France. Published by John Wiley & Sons Ltd.

Entities:  

Keywords:  cadmium; claudins and connexins; gap and tight junctions; hepatocytes

Mesh:

Substances:

Year:  2013        PMID: 24117459     DOI: 10.1111/boc.201200092

Source DB:  PubMed          Journal:  Biol Cell        ISSN: 0248-4900            Impact factor:   4.458


  6 in total

1.  Different Routes of Administration Lead to Different Oxidative Damage and Tissue Disorganization Levels on the Subacute Cadmium Toxicity in the Liver.

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Review 2.  Freeze fracture: new avenues for the ultrastructural analysis of cells in vitro.

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Journal:  Histochem Cell Biol       Date:  2017-11-13       Impact factor: 4.304

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Authors:  Hui Zou; Xuezhong Liu; Tao Han; Di Hu; Yi Wang; Yan Yuan; Jianhong Gu; Jianchun Bian; Jiaqiao Zhu; Zong-ping Liu
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5.  Gap junction blockage promotes cadmium-induced apoptosis in BRL 3A derived from Buffalo rat liver cells.

Authors:  Di Hu; Hui Zou; Tao Han; Junze Xie; Nannan Dai; Liling Zhuo; Jianhong Gu; Jianchun Bian; Yan Yuan; Xuezhong Liu; Zongping Liu
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6.  Effects of Cadmium on ZO-1 Tight Junction Integrity of the Blood Brain Barrier.

Authors:  Jacopo Junio Valerio Branca; Mario Maresca; Gabriele Morucci; Tommaso Mello; Matteo Becatti; Luigia Pazzagli; Ilaria Colzi; Cristina Gonnelli; Donatello Carrino; Ferdinando Paternostro; Claudio Nicoletti; Carla Ghelardini; Massimo Gulisano; Lorenzo Di Cesare Mannelli; Alessandra Pacini
Journal:  Int J Mol Sci       Date:  2019-11-29       Impact factor: 5.923

  6 in total

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