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Regulation of mouse CYP1A1 gene expression by dioxin: requirement of two cis-acting elements during induction. 总被引:19,自引:12,他引:7 下载免费PDF全文
L A Neuhold Y Shirayoshi K Ozato J E Jones D W Nebert 《Molecular and cellular biology》1989,9(6):2378-2386
The mouse cytochrome P1450 (CYP1A1) gene is responsible for the metabolism of numerous carcinogens and toxic chemicals. Induction by the environmental contaminant tetrachlorodibenzo-p-dioxin (TCDD) requires a functional aromatic hydrocarbon (Ah) receptor. We examined the 5'-flanking region of the CYP1A1 gene in mouse hepatoma Hepa-1 wild-type cells and a mutant line having a defect in chromatin binding of the TCDD-receptor complex. We identified two cis-acting elements (distal, -1071 to -901 region; proximal, -245 to -50 region) required for constitutive and TCDD-inducible CYP1A1 gene expression. Three classes of DNA-protein complexes binding to the distal element were identified: class I, found only in the presence of TCDD and a functional Ah receptor, that was heat labile and not competed against by simian virus 40 (SV40) early promoter DNA; class II, consisting of at least three constitutive complexes that were heat stable and bound to SV40 DNA; and class III, composed of at least three constitutive complexes that were thermolabile and were not competed against by SV40 DNA. Essential contacts for these proteins were centered at -993 to -990 for the class I complex, -987, -986, or both for the class II complexes, and -938 to -927 for the class III complexes. The proximal element was absolutely essential for both constitutive and TCDD-inducible CYP1A1 gene expression, and at least two constitutive complexes bound to this region. These data are consistent with the proximal element that binds proteins being necessary but not sufficient for inducible gene expression; interaction of these proteins with those at the distal element was found to be required for full CYP1A1 induction by TCDD. 相似文献
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The functional human dihydrofolate reductase gene 总被引:54,自引:0,他引:54
M J Chen T Shimada A D Moulton A Cline R K Humphries J Maizel A W Nienhuis 《The Journal of biological chemistry》1984,259(6):3933-3943
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T Okazaki J D Zajac T Igarashi E Ogata H M Kronenberg 《The Journal of biological chemistry》1991,266(32):21903-21910
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D A Wiginton D J Kaplan J C States A L Akeson C M Perme I J Bilyk A J Vaughn D L Lattier J J Hutton 《Biochemistry》1986,25(25):8234-8244
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Ma Q 《Archives of biochemistry and biophysics》2002,404(2):309-316
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Complete nucleotide sequence of the human corticotropin-beta-lipotropin precursor gene. 总被引:11,自引:2,他引:9 下载免费PDF全文
H Takahashi Y Hakamata Y Watanabe R Kikuno T Miyata S Numa 《Nucleic acids research》1983,11(19):6847-6858
The nucleotide sequence of an 8658-base-pair human genomic DNA segment containing the entire corticotropin-beta-lipotropin precursor gene has been determined, and some sequence features of the gene and its flanking regions have been analysed. The gene is composed of 7665 base pairs including two introns of 3708 and 2886 base pairs. Comparison of the 5'-flanking sequences of the human, bovine and mouse corticotropin-beta-lipotropin precursor genes reveals the presence of a highly conserved region, which contains sequences of 14-15 base pairs homologous with sequences located upstream of the mRNA start site of other glucocorticoid-regulated genes. 相似文献
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B K Chow V Ting F Tufaro R T MacGillivray 《The Journal of biological chemistry》1991,266(28):18927-18933