Transcriptional regulation of the human reduced folate carrier promoter C: synergistic transactivation by Sp1 and C/EBP beta and identification of a downstream repressor

Payton SG; Whetstine JR; Ge YB; Matherly LH

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Transcriptional regulation of the human reduced folate carrier promoter C: synergistic transactivation by Sp1 and C/EBP beta and identification of a downstream repressor

机译：人类减少的叶酸载体启动子C的转录调控：Sp1和C / EBP beta的协同反式激活和下游阻遏物的鉴定

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The human reduced folate carrier (hRFC) is ubiquitously but differentially expressed in human tissues and its levels are regulated by up to six alternatively spliced non-coding regions (designated A1/A2, A, B, C, D, and E) and by at least four promoters. By transient transfections of HepG2 human hepatoma cells.with 5' and 3' deletion constructs spanning 2883 bp of upstream sequence, a transcriptionally important region was localized to within 177 bp flanking the transcriptional start sites for exon C. By gel shift and chromatin immunoprecipitation assays, Sp1 and C/EBP beta transcription factors were found to bind consensus elements (GC-box, CCAAT-box) within this region. The functional importance of these elements was confirmed by transient tranfections of HepG2 cells with hRFC-C reporter constructs in which these elements were mutated, and by co-transfections of Drosophila SL-2 cells with wild-type hRFC-C promoter and expression constructs for Sp I and C/EBP beta, Whereas both Sp I and C/EBP beta transactivated hRFC-C promoter activity, C/EBP alpha and gamma were transcriptionally inert. Sp1 combined with C/EBP beta resulted in a synergistic transactivation. In HepG2 cells, transfections with Sp1 and C/EBP beta both increased endogenous levels of hRFC-C transcripts. By 3' deletion analysis, a repressor sequence was localized to within 71 bp flanking the minimal promoter. On gel shifts, a novel transcriptional repressor was localized to within 30 bp. Collectively, these results identify transcriptionally important regions in the hRFC-C minimal promoter that include a GC-box and CCAAT-box, and suggest that cooperative interactions between Sp1 and C/EBP beta are essential for hRFC-C transactivation. Another possible factor in the tissue-specific regulation of the hRFC-C region involves the downstream repressor flanking the minimal promoter. (C) 2004 Elsevier B.V. All rights reserved.

机译：人类减少的叶酸载体（hRFC）在人体组织中普遍存在但差异表达，其水平受多达六个交替剪接的非编码区（称为A1 / A2，A，B，C，D和E）和至少四个启动子。通过瞬时转染HepG2人肝癌细胞，具有跨上游序列2883 bp的5'和3'缺失构建体，转录重要区域位于外显子C转录起始位点两侧177 bp之内。通过凝胶迁移和染色质免疫沉淀测定，发现Sp1和C / EBP beta转录因子结合了该区域内的共有元件（GC-box，CCAAT-box）。这些元件的功能重要性已通过用hRFC-C报告基因构建体瞬时转染HepG2细胞（其中这些元素发生了突变）以及果蝇SL-2细胞与野生型hRFC-C启动子及其表达构建体的共转染得到了证实。 Sp I和C / EBP beta，而Sp I和C / EBP beta均可激活hRFC-C启动子活性，而C / EBP alpha和γ在转录上是惰性的。 Sp1与C / EBP beta结合导致协同反式激活。在HepG2细胞中，用Sp1和C / EBP beta转染均可增加hRFC-C转录本的内源性水平。通过3'缺失分析，阻遏物序列位于最小启动子侧翼的71bp内。在凝胶移位时，新型转录阻遏物定位在30 bp以内。总的来说，这些结果确定了hRFC-C最小启动子中的转录重要区域，包括GC-box和CCAAT-box，并暗示Sp1和C / EBP beta之间的协同相互作用对于hRFC-C反式激活至关重要。 hRFC-C区的组织特异性调节的另一个可能因素涉及最小启动子侧翼的下游阻遏物。（C）2004 Elsevier B.V.保留所有权利。

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《Biochimica et biophysica acta. Gene structure and expression》 |2005年第1期|共13页
作者
Payton SG; Whetstine JR; Ge YB; Matherly LH;
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正文语种 eng
中图分类生物化学;
关键词
reduced folate carrier; methotrexate; Sp1; C/EBP; transcription; ACUTE LYMPHOBLASTIC-LEUKEMIA; GAMMA-GLUTAMATE SYNTHETASE; MESSENGER-RNA; METHOTREXATE RESISTANCE; CELLULAR PHARMACOLOGY; BINDING PROTEINS; GENE-EXPRESSION; ORGANIZATION; STABILITY; SEQUENCES;

机译：还原叶酸载体;甲氨蝶呤;Sp1;C / EBP;转录;急性淋巴母细胞白血病;γ-谷氨酸合成酶;信使RNA;甲氨蝶呤抗性;细胞药理学;结合蛋白;基因表达;结构;组织;
入库时间 2022-08-18 09:01:37

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1. Transcriptional regulation of the human reduced folate carrier promoter C: synergistic transactivation by Sp1 and C/EBP beta and identification of a downstream repressor [J] . Payton SG, Whetstine JR, Ge YB, Biochimica et biophysica acta. Gene structure and expression . 2005,第1期

机译：人类减少的叶酸载体启动子C的转录调控：Sp1和C / EBP beta的协同反式激活和下游阻遏物的鉴定
2. Transcriptional regulation of the human cystathionine beta-synthase -1b basal promoter: synergistic transactivation by transcription factors NF-Y and Sp1/Sp3. [J] . Ge Y, Konrad MA, Matherly LH, The Biochemical Journal . 2001,第Pta1期

机译：人类胱硫醚β-合酶-1b基础启动子的转录调控：转录因子NF-Y和Sp1 / Sp3的协同反式激活。
3. Transcriptional regulation of the human cystathionine β-synthase ?1b basal promoter: synergistic transactivation by transcription factors NF-Y and Sp1/Sp3 [J] . Jeffrey W. TAUB, Larry H. MATHERLY, Mark A. KONRAD, The biochemical journal . 2001,第1期

机译：人胱硫醚β-合酶β1b基础启动子的转录调控：转录因子NF-Y和Sp1 / Sp3的协同反式激活
4. Transcriptional Regulation of The Human Leukotriene Q Synthase Promoter [C] . Ji-liang Zhao, K. Frank Austen, Bing K. Lam International Stereotactic Radiosurgery Society . 2000

机译：人白三烯Q合酶启动子的转录调节
5. Transcriptional regulation of the human aryl hydrocarbon receptor: Identification of multiple transactivation sub-domains and role of coactivators in modulating transactivation potential. [D] . Kumar, Mohan Basavaraju. 2000

机译：人类芳烃受体的转录调控：多个反式激活子域的识别和共激活剂在调节反式激活潜力中的作用。
6. Transcriptional regulation of the human cystathionine beta-synthase -1b basal promoter: synergistic transactivation by transcription factors NF-Y and Sp1/Sp3. [O] . Y Ge, M A Konrad, L H Matherly, 2001

机译：人胱硫醚β-合酶-1b基础启动子的转录调控：转录因子NF-Y和Sp1 / Sp3的协同反式激活。
7. Roles of USF, Ikaros and Sp proteins in the transcriptional regulation of the human reduced folate carrier B promoter [O] . Liu, Mingjun, Whetstine, Johnathan R., Payton, Scott G., 2004

机译：USF，Ikaros和Sp蛋白在人类还原型叶酸载体B启动子的转录调控中的作用

Transcriptional regulation of the human reduced folate carrier promoter C: synergistic transactivation by Sp1 and C/EBP beta and identification of a downstream repressor

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