Cyclic AMP-dependent Protein Kinase Signaling Modulates Pregnane x Receptor Activity in a Species-specific Manner

Lichti-Kaiser, Kristin; Xu, Chenshu; Staudinger, Jeff

doi:10.1074/jbc.m807426200

Cited by 52 publications

(82 citation statements)

References 34 publications

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“…PKA and PKC are known to contribute to the cell signaling involved in ligand-inducible PXR activation; PKC and PKA cell signaling represses the transcriptional activity of PXR by increasing the strength of the interaction between PXR and the nuclear receptor corepressor protein NCoR, and the human PXR protein can serve as an effective substrate for catalytically active PKA (Ding and Staudinger, 2005a,b;Lichti-Kaiser et al, 2009b). We demonstrated here for the first time that CaMKII directly phosphorylated the threonine-290 of hPXR in vitro, while PKA and PKC, two activitydependent kinases with similar consensus sequences to CaMKII, could also phosphorylate serines/threonines, except for the threonine-290 of hPXR (Fig.…”

Section: Threonine-290 Regulates Human Pxr Nuclear Translocationmentioning

confidence: 99%

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

et al. 2014

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The human pregnane X receptor (hPXR) is recognized as a xenobioticsensing nuclear receptor that transcriptionally regulates the gene expression of drug-metabolizing enzymes and transporters. Our study elucidates the mechanism by which the localization of hPXR is regulated through threonine-290. A phosphomimetic mutation at threonine-290 (T290D) retained hPXR in the cytoplasm of HepG2, HuH6, and SW480 cells in vitro and the mouse liver in vivo even after treatment with rifampicin, and a phosphodeficient mutation (T290A) translocated from the cytoplasm to the nucleus as the wild-type hPXR. The amount of the unphosphorylated wild-type yellow fluorescent protein-hPXR fusion protein but not the T290A mutant increased on Phos-tag gels in response to stimulations with rifampicin and cyclin-dependent kinase 2 inhibitor roscovitine, and a marked increase was observed in the unphosphorylated levels of the T290A mutant in nontreated cells. The Ca CaMKII directly phosphorylated the threonine-290 of hPXR, and the T290A mutant conferred resistance to CaMKII. The protein phosphatase (PP) inhibitor okadaic acid (100 nM) and transfection with anti-PP1 siRNA but not anti-PP2A siRNA led to reduced expression of CYP3A4 mRNA. After the rifampicin and roscovitine stimulations, PP1 was recruited to the wild-type hPXR but not the T290A mutant. These results suggest that phosphorylation at threonine-290 by CaMKII may impair the function of hPXR by repressing its translocation to the nucleus, and dephosphorylation by PP1 is necessary for the xenobiotic-dependent nuclear translocation of hPXR.

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Section: Threonine-290 Regulates Human Pxr Nuclear Translocationmentioning

confidence: 99%

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

et al. 2014

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“…The negative regulation of PXR by the cell-cycle-regulated Cdk2 suggests that PXR is subject to cell cycle regulation. PXR was also reported to be a substrate in in vitro kinase assays for a panel of kinases; protein kinase C (PKC) (Ding and Staudinger 2005b), 70 kDa ribosomal S6 kinase (p70S6K), glycogen synthase kinase 3 (GSK3), and casein kinase II (CK2) (Lichti-Kaiser et al 2009b), further suggesting that PXR may be modulated by a wide range of protein kinases. However, to this end, in vivo phosphorylation of PXR remains undetectable.…”

Section: 3mentioning

confidence: 99%

“…Treatment of primary rat and human hepatocytes with protein kinase A (PKA) activator leads to the attenuation of Cyp3A1 (Cyp3A1 is the rat ortholog of human CYP3A4) and CYP3A4 mRNA levels, respectively. This can be attributed, in part, to the phosphorylation of PXR by PKA (Ding & Staudinger 2005a;Lichti-Kaiser et al 2009b). However, a similar treatment of mouse hepatocytes resulted in an increase in Cyp3a11 mRNA levels, suggesting species specificity within PXR (Lichti-Kaiser et al 2009b).…”

Section: 3mentioning

confidence: 99%

“…This can be attributed, in part, to the phosphorylation of PXR by PKA (Ding & Staudinger 2005a;Lichti-Kaiser et al 2009b). However, a similar treatment of mouse hepatocytes resulted in an increase in Cyp3a11 mRNA levels, suggesting species specificity within PXR (Lichti-Kaiser et al 2009b). Work from our laboratory demonstrated that the treatment of HepG2 cells with flavonoids leads to an increase in CYP expression through modulating the activity of cyclin-dependent kinase 5 (Cdk5).…”

Section: 3mentioning

confidence: 99%

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Pregnane X Receptor in Drug Development

Ong¹,

Wang²,

Chai³

et al. 2011

Drug Development - A Case Study Based Insight Into Modern Strategies

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“…Kinases such as protein kinase A (Ding and Staudinger, 2005a;Lichti-Kaiser et al, 2009), protein kinase C (Ding and Staudinger, 2005b), cyclin-dependent kinase (CDK)2 (Lin et al, 2008), and p70 ribosomal S6 kinase (Pondugula et al, 2009b) phosphorylate PXR and regulate PXR-mediated CYP gene expression. Furthermore, CDK1, casein kinase II, and glycogen synthase kinase 3 also phosphorylate PXR (Lichti-Kaiser et al, 2009), although the functional significance of these phosphorylations is unknown.…”

Section: Introductionmentioning

confidence: 99%

Protein Phosphatase 2Cβl Regulates Human Pregnane X Receptor-Mediated CYP3A4 Gene Expression in HepG2 Liver Carcinoma Cells

Pondugula

Tong²,

Wu³

et al. 2010

Drug Metab Dispos

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ABSTRACT:The human pregnane X receptor (hPXR) regulates the expression of CYP3A4, which plays a vital role in hepatic drug metabolism and has considerably reduced expression levels in proliferating hepatocytes. We have recently shown that cyclin-dependent kinase 2 (CDK2) negatively regulates hPXR-mediated CYP3A4 gene expression. CDK2 can be dephosphorylated and inactivated by protein phosphatase type 2C beta isoform long (PP2C␤l), a unique phosphatase that was originally cloned from human liver. In this study, we sought to determine whether PP2C␤l is involved in regulating hPXR's transactivation activity and whether PP2C␤l affects CDK2 regulation of this activity in HepG2 liver carcinoma cells. In transactivation assays, transiently coexpressed PP2C␤l significantly enhanced the hPXR-mediated CYP3A4 promoter activity and decreased the inhibitory effect of CDK2 on hPXR transactivation activity. In addition, shRNA-mediated down-regulation of endogenous PP2C␤l promoted cell proliferation, inhibited the interaction of hPXR with steroid receptor coactivator-1, and attenuated the hPXR transcriptional activity. The levels of PP2C␤l did not affect hPXR expression. Our results show for the first time that PP2C␤l is essential for hPXR activity and can positively regulate this activity by counteracting the inhibitory effect of CDK2. Our results implicate a novel and important role for PP2C␤l in regulating hPXR activity and CYP3A4 expression by inhibiting or desensitizing signaling pathways that negatively regulate the function of pregnane X receptor in liver cells and are consistent with the notion that both the activity of hPXR and the expression of CYP3A4 are regulated in a cell cycle-dependent and cell proliferation-dependent manner.

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Cyclic AMP-dependent Protein Kinase Signaling Modulates Pregnane x Receptor Activity in a Species-specific Manner

Cited by 52 publications

References 34 publications

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

Pregnane X Receptor in Drug Development

Protein Phosphatase 2Cβl Regulates Human Pregnane X Receptor-Mediated CYP3A4 Gene Expression in HepG2 Liver Carcinoma Cells

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Cyclic AMP-dependent Protein Kinase Signaling Modulates Pregnane x Receptor Activity in a Species-specific Manner

Cited by 52 publications

References 34 publications

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca2+/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca2+/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

Pregnane X Receptor in Drug Development

Protein Phosphatase 2Cβl Regulates Human Pregnane X Receptor-Mediated CYP3A4 Gene Expression in HepG2 Liver Carcinoma Cells

Contact Info

Product

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Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1

Threonine-290 Regulates Nuclear Translocation of the Human Pregnane X Receptor through Its Phosphorylation/Dephosphorylation by Ca²⁺/Calmodulin-Dependent Protein Kinase II and Protein Phosphatase 1