Phosphatidylcholine Specific PLC-Induced Dysregulation of Gap Junctions, a Robust Cellular Response to Environmental Toxicants, and Prevention by Resveratrol in a Rat Liver Cell Model

Sovadinová, Iva; Babica, Pavel; Böke, Hatice; Kumar, Esha; Wilke, Andrew; Park, Joon Suk; Trosko, James E.; Upham, Brad L.

doi:10.1371/journal.pone.0124454

Cited by 30 publications

(73 citation statements)

References 55 publications

(84 reference statements)

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“…GJIC dysregulation by VIN has not been previously reported. Effective concentrations of VIN for inhibition of GJIC (30-min EC 50 ¼ 126 mM) are comparable with the chemicals like alachlor, perfluoroheptanoic acid, benzoylperoxide, or lipidic compounds, which required higher concentrations (>100 mM) to rapidly induce >50% inhibitory effect (Sovadinova et al, 2015;Upham et al, 1998Upham et al, , 2007. Also, endogenous or synthetic estrogens and androgens were found to affect GJIC and connexins not only via classical genomic mechanism (Ren et al, 2013), but also via rapid actions of non-genomic signaling (Iwase et al, 2006;Lyng et al, 2000;Pluciennik et al, 1996).…”

Section: Discussionmentioning

confidence: 84%

“…Also, endogenous or synthetic estrogens and androgens were found to affect GJIC and connexins not only via classical genomic mechanism (Ren et al, 2013), but also via rapid actions of non-genomic signaling (Iwase et al, 2006;Lyng et al, 2000;Pluciennik et al, 1996). GJIC thus represents a cellular event possibly altered by hormones and EDCs via different mechanisms, which might be chemical-, as well as cell type-specific (Osgood et al, 2013;Sovadinova et al, 2015). The immediate cell responses to MXC and VIN observed in this study, such as inhibition of GJIC and phosphorylation of MAPKs and Cx43, were most likely mediated by rapid mechanisms independent of ER or AR genomic signaling.…”

Section: Discussionmentioning

confidence: 99%

“…Cells were routinely cultured in 75 cm 2 tissue culture flasks (Costar, Cambridge, Massachusetts) in humidified 5% CO 2 atmosphere at 37 C, and routinely passaged every other day. (Ogawa et al, 2004;Sovadinova et al, 2015) and efficiency of these pretreatments was verified by positive controls with model chemicals known to dysregulate GJIC by a mechanism dependent on a given pathway: EGF was used as a positive control for U0126 (MEK1/2 inhibitor), anisomycin for SB202190 (p38 inhibitor), 1-MeA for D609 (PC-PLC inhibitor) and resveratrol. Pretreatments with ER agonist (E2, HPTE), ER antagonists (ICI 182 780), AR agonist (testosterone) and AR antagonists (flutamide, VIN M2) were done using concentrations ranging from 1 to 250 mM and 30 or 120 min incubation time.…”

Section: Methodsmentioning

confidence: 99%

“…Many EDCs, such as bisphenol A, DDT, lindane or phthalates, were found to induce rapid dysregulation of GJIC, with their effects shown to be structure-dependent and mediated via mechanisms including activation of specific kinases or phospholipases (Sovadinova et al, 2015;Vinken et al, 2009b). These data indicate that dysregulation of GJIC could be the key cellular process altered by EDCs via mechanisms independent on genomic signaling, which might contribute to their disruptive effects on epigenetic regulations, developmental programming, tissue development, and homeostasis.…”

mentioning

confidence: 99%

“…These effects, which are relevant for transcriptional and epigenetic control of gene expression and normal cell behavior (Trosko, 2011), were studied in a rat liver epithelial cell line WB-F344. This cell line is a well-established in vitro model for assessment of GJIC and mechanistic studies in responses to environmental contaminants (Sovadinova et al, 2015;Upham et al, 2007Upham et al, , 2008, which has been validated by in vivo studies (Sai et al, 2000;Upham et al, 2009) and matches the most extensively used rodent model system, F344 rats, in the National Toxicology Program. Both of these EDCs exhibited dose, time and mechanistic differences on GJIC, MAPKs, and phospholipase C, which were elicited by the parental compounds and occurred independently of ER-or AR-mediated genomic mechanisms.…”

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confidence: 99%

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Methoxychlor and Vinclozolin Induce Rapid Changes in Intercellular and Intracellular Signaling in Liver Progenitor Cells

et al. 2016

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Methoxychlor (MXC) and vinclozolin (VIN) are well-recognized endocrine disrupting chemicals known to alter epigenetic regulations and transgenerational inheritance; however, non-endocrine disruption endpoints are also important. Thus, we determined the effects of MXC and VIN on the dysregulation of gap junctional intercellular communication (GJIC) and activation of mitogen-activated protein kinases (MAPKs) in WB-F344 rat liver epithelial cells. Both chemicals induced a rapid dysregulation of GJIC at non-cytotoxic doses, with 30 min EC 50 values for GJIC inhibition being 10 mM for MXC and 126 mM for VIN. MXC inhibited GJIC for at least 24 h, while VIN effects were transient and GJIC recovered after 4 h. VIN induced rapid hyperphosphorylation and internalization of gap junction protein connexin43, and both chemicals also activated MAPK ERK1/2 and p38. Effects on GJIC were not prevented by MEK1/2 inhibitor, but by an inhibitor of phosphatidylcholine-specific phospholipase C (PC-PLC), resveratrol, and in the case of VIN, also, by a p38 inhibitor. Estrogen (ER) and androgen receptor (AR) modulators (estradiol, ICI 182,780, HPTE, testosterone, flutamide, VIN M2) did not attenuate MXC or VIN effects on GJIC. Our data also indicate that the effects were elicited by the parental compounds of MXC and VIN. Our study provides new evidence that MXC and VIN dysregulate GJIC via mechanisms involving rapid activation of PC-PLC occurring independently of ER-or AR-dependent genomic signaling. Such alterations of rapid intercellular and intracellular signaling events involved in regulations of gene expression, tissue development, function and homeostasis, could also contribute to transgenerational epigenetic effects of endocrine disruptors.

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Section: Discussionmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Methoxychlor and Vinclozolin Induce Rapid Changes in Intercellular and Intracellular Signaling in Liver Progenitor Cells

et al. 2016

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Cell membrane‐related toxic responses and disruption of intercellular communication in PCB mechanisms of toxicity: A review

Murati

Miletić

Pleadin

et al. 2020

J of Applied Toxicology

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An understanding of polychlorinated biphenyl (PCB) congener‐specific effects on cell membrane and intercellular communication is important within the studies of PCB absorption, organ‐related PCB accumulation and exertion of toxic responses. Toxic potential of PCBs is linked to various deleterious effects on human health, including neurotoxicity, immunotoxicity, reproductive toxicity and genotoxicity and, recently in 2016 International Agency for Research on Cancer (IARC) has upgraded the classification of PCBs to Group 1 “Carcinogenic to humans.” Proposed mechanisms of aforementioned PCBs adverse effects at cellular membrane level are: (i) downregulation of gap junction intercellular communication and/or connexins; (ii) compromised membrane integrity; and (iii) altered tight junction barrier function. This study, based on an extensive literature survey, shows the progress in scientific research of each of these three levels with the aim of pointing out the earliest toxic events of PCBs, which can result in serious cell/tissue/organ damage.

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Scrape Loading/Dye Transfer Assay

Babica

Sovadinová

Upham

2016

Methods in Molecular Biology

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The scrape loading/dye transfer (SL/DT) technique is a simple functional assay for the simultaneous assessment of gap junctional intercellular communication (GJIC) in a large population of cells. The equipment needs are minimal and are typically met in standard cell biology labs, and SL/DT is the simplest and quickest of all the assays that measure GJIC. This assay has also been adapted for in vivo studies. The SL/DT assay is also conducive to a high-throughput setup with automated fluorescence microscopy imaging and analysis to elucidate more samples in shorter time, and hence can serve a broad range of in vitro pharmacological and toxicological needs.

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Phosphatidylcholine Specific PLC-Induced Dysregulation of Gap Junctions, a Robust Cellular Response to Environmental Toxicants, and Prevention by Resveratrol in a Rat Liver Cell Model

Cited by 30 publications

References 55 publications

Methoxychlor and Vinclozolin Induce Rapid Changes in Intercellular and Intracellular Signaling in Liver Progenitor Cells

Methoxychlor and Vinclozolin Induce Rapid Changes in Intercellular and Intracellular Signaling in Liver Progenitor Cells

Cell membrane‐related toxic responses and disruption of intercellular communication in PCB mechanisms of toxicity: A review

Scrape Loading/Dye Transfer Assay

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