Dioxin-dependent activation of murine Cyp1a-1 gene transcription requires protein kinase C-dependent phosphorylation.

Carrier, F.; Owens, Roland A.; Nebert, Daniel W.; Puga, Alvaro

doi:10.1128/mcb.12.4.1856

Cited by 146 publications

(75 citation statements)

References 72 publications

(75 reference statements)

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“…This effect has been observed in multiple liver cell types [Puga et al, 1992;Enan et al, 1998b;Ashida et al, 2000], but not in all [Gohl et al, 1996]. In other cells, such as LPS-activated B cells, TCDD downregulates AP-1 expression [Suh et al, 2002], suggesting a cell type-dependent effect of AHR ligands on immediate-early protooncogene induction.…”

Section: Ahr Agonists Activate Immediate-early Response Genesmentioning

confidence: 86%

“…Exposure of multiple rodent cell lines to TCDD results in an essentially immediate increase in protein kinase C levels and activity in cellular membranes [Bombick et al, 1985Madhukar et al, 1988;Carrier et al, 1992]. TCDD specifically activates tyrosine kinases associated with the EGFR [Madhukar et al, 1984[Madhukar et al, , 1988 and induces the association of adaptor proteins such as SHC, GRB2, and SOS with EGFR [Park et al, 1998].…”

Section: Ahr Ligand-dependent Activation Of Signal Transduction Pathwaysmentioning

confidence: 99%

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Aryl hydrocarbon receptor, cell cycle regulation, toxicity, and tumorigenesis

Marlowe

Puga

2005

J of Cellular Biochemistry

280

201

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Most effects of exposure to halogenated and polycyclic aromatic hydrocarbons are mediated by the aryl hydrocarbon receptor (AHR). It has long been recognized that the AHR is a ligand-activated transcription factor that plays a central role in the induction of drug-metabolizing enzymes and hence in xenobiotic detoxification. Of late, it has become evident that outside this well-characterized role, the AHR also functions as a modulator of cellular signaling pathways. In this Prospect, we discuss the involvement of the AHR in pathways critical to cell cycle regulation, mitogen-activated protein kinase cascades, immediate-early gene induction, and the functions of the RB protein. Ultimately, the toxicity of AHR xenobiotic ligands may be intrinsically connected with the perturbation of these pathways and depend on the many critical signaling pathways and effectors with which the AHR itself interacts. J. Cell. Biochem. 96: 1174Biochem. 96: -1184Biochem. 96: , 2005. Key words: Ah receptor; xenobiotic ligands; signal transduction; retinoblastoma protein; apoptosis Exposure to halogenated aromatic hydrocarbons (HAHs) and PAHs results in a wide range of toxic and carcinogenic responses in animals and in humans. It is widely accepted that most of these exposure effects are mediated by the aryl hydrocarbon receptor (AHR), a cytosolic ligand-activated transcription factor that upon ligand binding translocates to the nucleus, where it complexes with ARNT (a.k.a. HIF1b). AHR/ARNT heterodimers bind to specific consensus DNA sites in the regulatory domains of genes coding for many Phase I and Phase II drug-metabolizing enzymes and activate the transcription of these genes [Hankinson, 1995]. During the last 8-10 years, it has also become evident that the AHR has a second function, involving promotion of cell cycle progression, and that this function is accomplished in the absence of an exogenous ligand. In contrast, activation of the Ah receptor by high-affinity HAH or PAH ligands such as TCDD and B[a]P has been known for many years to result in a wide range of cell cycle perturbations, including G 0 /G 1 and G 2 /M arrest, diminished capacity for DNA replication, and inhibition of cell proliferation [reviewed in Puga et al., 2002]. These two outcomes are diametrically opposed and raise questions for which we do not have satisfactory answers at present. For example, how does the unliganded cytosolic Ah receptor influence a nuclear function such as cell cycle progression? Does this effect involve nuclear translocation? If so, do liganded and unliganded nuclear translocation events have different molecular outcomes? What makes dioxin carcinogenic? In these and similar questions, we need to bear in mind that it is only our current ß 2005 Wiley-Liss, Inc.

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Section: Ahr Agonists Activate Immediate-early Response Genesmentioning

confidence: 86%

Section: Ahr Ligand-dependent Activation Of Signal Transduction Pathwaysmentioning

confidence: 99%

Aryl hydrocarbon receptor, cell cycle regulation, toxicity, and tumorigenesis

Marlowe

Puga

2005

J of Cellular Biochemistry

280

201

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“…Recently, a number of in vivo and in vitro studies have been focused on the effects of protein kinase activation on the specific signal transduction pathways in the control of cyp1A1 gene expression. Notably, protein kinase C-mediated phosphorylation (15,16) appears to be a determinant in the regulation of PAHinducible cyp1A1 gene expression. Our past experiments suggested that PKC-dependent phosphorylation of AhR appears to be required for PAH induction of all of the xenobiotic metabolizing enzymes in the Ah gene battery, not just for cyp1A1 (17).…”

Section: Discussionmentioning

confidence: 99%

“…Carrier et al (15) and Reiners et al (16) have provided evidence that some step in transactivation by the AhR is dependent upon phosphorylation by PKC. Our studies (17) with cultured rat hepatocytes demonstrated that the PKC inhibitors H7 and staurosporine concomitantly inhibited PAH induction of all five genes we tested, including aldh3, cyp1A1, gst1, qor, and ugt1.…”

mentioning

confidence: 99%

cAMP-dependent Negative Regulation of Rat Aldehyde Dehydrogenase Class 3 Gene Expression

Xiao

Falkner

Xie

et al. 1997

Journal of Biological Chemistry

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We investigated the inhibitory effects of intracellular cyclic adenosine monophosphate (cAMP) levels in regulating class 3 aldehyde dehydrogenase (aldh3) gene expression using cultures of primary rat hepatocytes and transient transfection experiments with HepG2 cells. In addition to regulation by an Ah receptor-dependent mechanism, expression of many members of the Ah gene battery have been shown to be negatively regulated. As was seen for the cytochrome P450 (cyp1A1) gene, aldh3 is transcriptionally inducible by polycyclic aromatic hydrocarbons (PAH), and this induction involving function of the arylhydrocarbon (Ah) receptor is inhibited by the protein kinase C (PKC) inhibitors, 1-(5-isoquinolinesulfonyl)-2-methylpiperazine di-HCl (H7) and staurosporine. However, PAH induction of ALDH-3 activity, protein, and mRNA was potentiated 2-4-fold by addition of the protein kinase A (PKA) inhibitors, N-(2-(methylamino)ethyl)-5-isoquinolinesulfonamide di-HCl (H8) and N-(2-guanidinoethyl)-5-isoquinolinesulfonamide HCl (HA1004). These PKA inhibitors had no effect on the PAH induction of the cyp1A1. Protein kinase A activity of cultured hepatocytes was specifically inhibited by H8 and HA1004 in a concentration-dependent manner, but not by H7, and there was an inverse correlation observed between potentiation of PAH-induced aldh3 gene expression and inhibition of specific PKA activity by the PKA inhibitors. The cAMP analog dibutyryl cAMP, the adenylate cyclase activator forskolin, and the protein phosphatase 1 and 2A inhibitor okadaic acid all dramatically inhibited both PAH induction and H8 potentiation of PAH induction of aldh3 expression but had no effect on induction of cyp1A1 expression in cultured hepatocytes.Both basal and PAH-dependent expression of a chloramphenicol acetyltransferase expression plasmid containing approximately 3.5 kilobase pairs of the 5-flanking region of aldh3 (pALDH3.5CAT) were enhanced 3-4-fold by the PKA inhibitor H8 but not by the PKC inhibitor H7 (>20 M). cAMP analogs, activators of PKA activity, or protein phosphatase inhibitors diminished expression of the reporter gene in a manner identical to the native gene in cultured rat hepatocytes. Using deletion analysis of the pALDH3.5CAT construct, we demonstrated the existence of a negative regulatory region in the 5-flanking region between ؊1057 and ؊991 base pairs which appears to be responsible for the cAMP-dependent regulation of this gene under both basal and PAH-induced conditions. At least two apparently independent mechanisms which involve protein phosphorylation regulate aldh3 expression. One involves function of the Ah receptor which requires PKC protein phosphorylation to positively regulate both aldh3 and cyp1A1 gene expression and the other a cAMP-responsive process which allows PKA activity to negatively regulate expression of aldh3 under either basal or inducible conditions.The aldehyde dehydrogenases (ALDH, 1 aldehyde NAD(P) ϩ oxidoreductase EC 1.2.1.3) are a family of NAD(P) ϩ -dependent enzymes that oxidize a broad class of alde...

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“…The activated AhR complex then binds promoter regions of target genes at specific DNA-binding sites (aryl hydrocarbon response elements (AhREs)), thereby modulating gene transcription (Okey et al, 1994;Hankinson, 1995;Porter et al, 2001). A common outcome of AhR activation is the induction of genes such as those encoding the cytochrome P-4501A1, 1A2, and 1B1 monooxygenases (Poland et al, 1974;Whitlock, 1990;Carrier et al, 1992;Larsen et al, 1997). AhR-dependent upregulation of these enzymes results in increased metabolism of some AhR ligands such as PAH and the production of carcinogenic intermediates (Buters et al, 1999;Dertinger et al, 2001).…”

Section: Introductionmentioning

confidence: 99%