Dimerization with Retinoid X Receptors Promotes Nuclear Localization and Subnuclear Targeting of Vitamin D Receptors

Prüfer, Kirsten; Rácz, Attila; Lin, Grace C.; Bársony, Julia

doi:10.1074/jbc.m003791200

Cited by 130 publications

(105 citation statements)

References 45 publications

(27 reference statements)

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“…Next, we tested the effect of ligands on intranuclear localization of LXR a and LXR b. We and others showed previously that fluorescent chimeras of nuclear receptors bound to ligand accumulate in nuclear foci [Htun et al, 1996Lim et al, 1999;Prufer et al, 2000;Stenoien et al, 2000;Baumann et al, 2001;Prufer and Barsony, 2002]. We treated 293LXRa and 293LXRb cells with either vehicle (DMSO), agonist (a combination of 10 mM 22-(R) hydroxycholesterol and 100 nM 9-cis retinoic acid), or antagonist (1 mM geranyl geranyl pyrophosphate).…”

Section: Results Lxr a And Lxr B Are Nuclear With And Without Ligandmentioning

confidence: 99%

“…YFP, YFP-LXR a, and YFP-LXR b were stably expressed in HEK293 cells (293YFP, 293LXRa, and 293LXRb cells, respectively) and selected using geneticin as described previously [Prufer et al, 2000]. Expression of YFP-LXR a and YFP-LXR b at the expected molecular weight in each three clones was confirmed using Western blot analysis (not shown).…”

Section: Cells and Expression Constructsmentioning

confidence: 99%

“…Transcriptionally active YFP-RXR (RXR a) was generated as described earlier [Prufer et al, 2000]. We received LXR a and LXR b in the pDNR vector from the Harvard Institute of Proteomics.…”

Section: Cells and Expression Constructsmentioning

confidence: 99%

“…HEK293, and F9 cells were obtained from ATCC (Manassas, VA) and grown as described previously [Racz and Barsony, 1999;Prufer et al, 2000]. Briefly, cell cultures were maintained in DMEM (Invitrogen, Carlsbad, CA) supplemented with 10% FBS (Hyclone, Logan, UT), 2 mM glutamine (Invitrogen), and 0.1 mg/ml gentamicin (Invitrogen …”

Section: Cells and Expression Constructsmentioning

confidence: 99%

“…Unliganded androgen receptor (AR) [Tyagi et al, 2000], glucocorticoid receptor (GR) [Picard and Yamamoto, 1987], and vitamin D receptor (VDR) [Barsony et al, 1997] localize at least partially in the cytoplasm but translocate into the nucleus after ligand binding. In contrast, progesterone receptor [GuiochonMantel et al, 1991], thyroid hormone receptor (TR) [Bunn et al, 2001], estrogen receptor (ER) , RXR [Prufer et al, 2000], LXR a [Watanabe et al, 2003], and LXR b [Mo et al, 2002] are primarily located in the nuclei with or without bound ligand. However, nucleocytoplasmic trafficking has been shown for both types of nuclear receptors [Dauvois et al, 1993;Guiochon-Mantel et al, 1994;Hache et al, 1999;Baumann et al, 2001;Bunn et al, 2001;Prufer and Barsony, 2002].…”

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confidence: 99%

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Nuclear localization of liver X receptor α and β is differentially regulated

Prüfer

Boudreaux

2006

J of Cellular Biochemistry

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Activity of nuclear receptors is regulated by their nuclear localization. Liver X receptors (LXR) a and b are nuclear receptors that regulate transcription of genes for cholesterol metabolism, cholesterol transport, and lipogenesis. While LXR a and b are very similar in structure and exhibit similar ligand binding properties, their physiological roles are quite different. Since the LXRs fall into a class of receptors that move between the nucleus and cytoplasm, experiments were conducted to determine whether LXR a and LXR b show differences in their nuclear localization pattern. To determine the location of each receptor, cell lines stably expressing yellow fluorescent protein (YFP) chimeras with either LXR a or LXR b were examined. Retention in the nucleus of the chimeric proteins in the presence or absence of ligands was assessed using fluorescence microscopy coupled with digitonin permeabilization assays. Surprisingly, differences were found between LXR a and LXR b. Whereas unliganded LXR a was retained in the nucleus, unliganded LXR b was partially exported. Mutations were then introduced into putative nuclear localization sequences (NLS) to determine which sequences are important for nuclear localization and function. Mutation in one such sequence abolished nuclear localization of LXR a, whereas the analogous change in LXR b had a much less dramatic effect. Mutations in analogous putative NLS also differentially affected transcriptional activation by LXR a and LXR b. These data demonstrate for the first time that nuclear retention and localization as well as function of LXR a and LXR b are differentially regulated.

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Section: Results Lxr a And Lxr B Are Nuclear With And Without Ligandmentioning

confidence: 99%

Section: Cells and Expression Constructsmentioning

confidence: 99%

“…Transcriptionally active YFP-RXR (RXR a) was generated as described earlier [Prufer et al, 2000]. We received LXR a and LXR b in the pDNR vector from the Harvard Institute of Proteomics.…”

Section: Cells and Expression Constructsmentioning

confidence: 99%

Section: Cells and Expression Constructsmentioning

confidence: 99%

mentioning

confidence: 99%

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Nuclear localization of liver X receptor α and β is differentially regulated

Prüfer

Boudreaux

2006

J of Cellular Biochemistry

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Ligand binding is without effect on complex formation of the ligand binding domain of the ecdysone receptor (EcR)

Greb‐Markiewicz

Fauth

Spindler-Barth

2005

Arch. Insect Biochem. Physiol.

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The ligand-binding domain (LBD) encompassing the C-terminal parts of the D- and the complete E-domains of the ecdysteroid receptor (EcR) fused to Gal4(AD) is present in two high molecular weight complexes (600 and 150 kDa) in yeast extracts according to size exclusion chromatography (Superdex 200 HR 10/30). Hormone binding is mainly associated with 150-kDa complexes. Complex formation is not influenced by hormone, but the ligand stabilizes the complexes at elevated salt concentrations. Mutational analysis of Gal4(AD)-EcR(LBD) revealed that formation of 600-kDa, but not 150-kDa, complexes depends on dimerization mediated by the EcR(LBD). Deletion of helix 12 is without effect. Mutation of K497 in helix 4, known to be essential for comodulator binding, abolishes 600-KDa complexes, but does not interfere with the formation of 150-kDa complexes. In contrast, the DE-domains of USP fused to Gal4(DBD) elute as monomer after elimination of the dimerization capacity of the ligand-binding domains by mutation of P463 in helix 10. The data presented here reveal that the complex formation of ligand-binding domains EcR and USP ligand is different.

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Phosphate: Known and potential roles during development and regeneration of teeth and supporting structures

Foster

Tompkins

Rutherford

et al. 2008

Birth Defects Research Pt C

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Inorganic phosphate (Pi) is abundant in cells and tissues as an important component of nucleic acids and phospholipids, a source of high-energy bonds in nucleoside triphosphates, a substrate for kinases and phosphatases, and a regulator of intracellular signaling. The majority of the body’s Pi exists in the mineralized matrix of bones and teeth. Systemic Pi metabolism is regulated by a cast of hormones, phosphatonins, and other factors via the bone-kidney-intestine axis. Mineralization in bones and teeth is in turn affected by homeostasis of Pi and inorganic pyrophosphate (PPi), with further regulation of the Pi/PPi ratio by cellular enzymes and transporters. Much has been learned by analyzing the molecular basis for changes in mineralized tissue development in mutant and knock-out mice with altered Pi metabolism. This review focuses on factors regulating systemic and local Pi homeostasis and their known and putative effects on the hard tissues of the oral cavity. By understanding the role of Pi metabolism in the development and maintenance of the oral mineralized tissues, it will be possible to develop improved regenerative approaches.

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Dimerization with Retinoid X Receptors Promotes Nuclear Localization and Subnuclear Targeting of Vitamin D Receptors

Cited by 130 publications

References 45 publications

Nuclear localization of liver X receptor α and β is differentially regulated

Nuclear localization of liver X receptor α and β is differentially regulated

Ligand binding is without effect on complex formation of the ligand binding domain of the ecdysone receptor (EcR)

Phosphate: Known and potential roles during development and regeneration of teeth and supporting structures

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