Specific protein-DNA interactions at a xenobiotic-responsive element: copurification of dioxin receptor and DNA-binding activity.

Hapgood, Janet P.; Cuthill, Scott; Denis, Marc G.; Poellinger, Lorenz; Gustafsson, Jan‐Åke

doi:10.1073/pnas.86.1.60

Cited by 98 publications

(60 citation statements)

References 24 publications

(25 reference statements)

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“…After diffusing into a cell, BaP binds with AhR and translocates into the nuclei, where BaP-AhR heterodimers form complexes with Ah receptor nuclear translocator (Arnt) proteins (2). The BaP-AhR-Arnt complexes then transactivate the CYP1A1 gene via interaction with its xenobiotic responsive element in the promoter region (37). In addition to the inhibition of BPDE-DNA adduct formation, our results show that GNMT is capable of reducing CYP1A1 enzyme activity induced by BaP (Fig.…”

Section: Discussionmentioning

confidence: 73%

See 1 more Smart Citation

Glycine N -Methyltransferase Tumor Susceptibility Gene in the Benzo( a )pyrene-Detoxification Pathway

Chen¹,

Lin

Darbha

et al. 2004

Cancer Research

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Section: Discussionmentioning

confidence: 73%

“…The low (Ϫ9.10 kcal/mol) binding energy between the dimeric form of GNMT and BaP suggests that BaP may displace (Table 2). Accordingly, several GNMT amino acid residues (including Thr 37 (Fig. 5C).…”

Section: Gnmt Nuclear Translocation Was Induced By Bap In Bothmentioning

confidence: 99%

Glycine N -Methyltransferase Tumor Susceptibility Gene in the Benzo( a )pyrene-Detoxification Pathway

Chen¹,

Lin

Darbha

et al. 2004

Cancer Research

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“…Besides the hepatocytespecific transcription factor HNFB3A and a CAAT enhancer, an Ah/ARNT binding domain [57][58][59][60] and a barbiturate recognition box 61 was found at a perfect distance to form a complex on the cDNA. This binding site for barbiturates seems to have a negative regulatory function, because the application of phenobarbital to rats at a dose of 100 mg/kg 36 hours before the isolation of hepatocytes leads to a marked decrease of methotrexate transport, whereas the uptake of cholate is not altered (Fig.…”

Section: Resultsmentioning

confidence: 99%

Cloning and functional characterization of the bile acid-sensitive methotrexate carrier from rat liver cells

Honscha¹,

Dötsch²,

Thomsen³

et al. 2000

Hepatology

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The antifolates methotrexate and trimetrexate are potent inhibitors of the dihydrofolate reductase, an enzyme that delivers by the metabolism of folate and its reduced forms the C1-groups for the synthesis of nucleotides and amino acids. Methotrexate, which has a comparatively moderate toxicity is one of the most important clinically used chemotherapeutics for the treatment of leukemias, such as acute lymphoblastic leukemia of children. It is also used in breast cancer, squamous tumors of the head and neck, lymphomas, and choriocarcinomas. 1,2 Uptake studies of methotrexate and the natural folic acid derivatives in different tumor and normal cells have shown that at least two different carrier systems mediate the uptake of these compounds. The 40 kd folate binding protein has a high affinity for folic acid but a low affinity for reduced folates. [3][4][5][6][7][8][9][10] The corresponding complementary DNAs (cDNAs) as well as genomic clones have been isolated from various sources, 11-19 but a detailed characterization of the transporter function is still missing.Different cDNAs and genomic clones for the reduced folate carrier, which has a high affinity for the reduced folates 5-methyltetrahydrofolate, 5-formyltetrahydrofolate, and methotrexate, but a low affinity for folate [20][21][22][23][24] have been also isolated from different immortal cell lines 25-31 but the clones were not characterized in detail.The expression and the abundance of the two carriers varied in different tumor and normal cells. From uptake studies it became evident that, first, in some cell systems both transport systems work in tandem 32 whereas two independently operating carrier systems were also described. 33,34 Second, tumor cells differ from normal cells in their transport properties. [35][36][37][38][39] Results from Chello et al. 40 showed, for example, a 30-fold higher affinity for methotrexate in the mouse leukemia cell line L1210 than in freshly isolated murine intestinal cells.Hepatocytes are exceptional with respect to folate transport. In contrast to most other cells, hepatocytes express a separate carrier system for 5-methyltetrahydrofolate, which is different from the reduced folate transporter. 41,42 We recently characterized the uptake of methotrexate into freshly isolated hepatocytes 43 and showed that this chemotherapeutic is taken up by a sodium-dependent active transport system, which is inhibited by the reduced folates, dihydrofolate, and tetrahydrofolate but not by folate itself. Moreover, substrates of two well-known organic anion transport systems in the liver, the Ntcp1 44,45 and the oatp1, 46 like the bile acids taurocholate and cholate as well as xenobiotics such as bromosulfophthalein, the loop diuretic bumetanide, and the mycotoxin ochratoxin A are potent inhibitors of the hepatocellular methotrexate carrier. Because some substrates were Abbreviations: cDNA, complementary DNA; RL-Mtx, rat liver methotrexate transporter; RACE-PCR, rapid amplification of cDNA ends polymerase chain reaction; DMEM, Dulbecco modi...

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“…This is in agreement with the deviation from the published consensus sequence 5Ј-T G/C G/T CACGC N C/A-3Ј (14), which is three base pair for DRE I, but only two for DRE II and DRE III (see Table II). Still, the core sequence, to which the AHR/ARNT/TCDD complex makes physical contact (14,28), is unchanged in all three DREs. Note that DRE I binds to proteins of an unknown nature, albeit this complex is not shifted by TCDD treatment.…”

Section: The Tcdd-activated Ahr Binds To the Dres In The Il-2 Distal mentioning

confidence: 99%

The MurineIL-2Promoter Contains Distal Regulatory Elements Responsive to the Ah Receptor, a Member of the Evolutionarily Conserved bHLH-PAS Transcription Factor Family

Jeon¹,

Esser²

2000

The Journal of Immunology

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Signaling through the TCR and costimulatory signals primarily control transcription of the IL-2 gene in naive T cells. The minimal promoter necessary for this expression lies proximal, between −300 and the transcription start site. We had previously shown that activation of the arylhydrocarbon receptor (AHR), a member of the bHLH-PAS family of transcription factors, leads to increased mRNA expression of IL-2 in murine fetal thymocytes. The AHR is abundant in the thymus and may play a role for the development of the immune system. Moreover, its overactivation by chemicals such as dioxins leads to immunosuppression and thymic involution. Binding motifs for the liganded AHR can be identified in the distal region −1300 to −800 of the mouse IL-2 promoter. We show here that these DNA motifs, the so-called dioxin response elements, after binding to the liganded AHR are sufficient to transactivate luciferase expression in a reporter gene system. The IL-2 gene can be induced by the AHR also in thymocytes in vivo after injection of 2,3,7,8-tetrachlorodibenzo-p-dioxin, a potent ligand of the AHR. The AHR mediates the IL-2 induction as shown with AHR-deficient mice. However, in spleen cells in vitro costimulation via the TCR is necessary for optimal IL-2 gene induction. Thus, the IL-2 promoter region contains novel distal regulatory elements that can be addressed by the AHR to induce IL-2 and can cooperate with the proximal promoter in this.

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Specific protein-DNA interactions at a xenobiotic-responsive element: copurification of dioxin receptor and DNA-binding activity.

Cited by 98 publications

References 24 publications

Glycine N -Methyltransferase Tumor Susceptibility Gene in the Benzo( a )pyrene-Detoxification Pathway

Glycine N -Methyltransferase Tumor Susceptibility Gene in the Benzo( a )pyrene-Detoxification Pathway

Cloning and functional characterization of the bile acid-sensitive methotrexate carrier from rat liver cells

The MurineIL-2Promoter Contains Distal Regulatory Elements Responsive to the Ah Receptor, a Member of the Evolutionarily Conserved bHLH-PAS Transcription Factor Family

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