Overlapping antioxidant response element and PMA responseelement sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene.

Wild AC; Gipp JJ; Mulcahy T

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Overlapping antioxidant response element and PMA responseelement sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene.

机译：重叠的抗氧化剂应答元件和PMA应答元件序列介导了基础和β-萘黄酮诱导的人γ-谷氨酰半胱氨酸合成酶催化亚基基因的表达。

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gamma-Glutamylcysteine synthetase (GCS), the rate-limiting enzyme in the de novo synthesis of GSH, is a heterodimer, consisting of a catalytic (GCSh) and a regulatory subunit (GCSl). We previously demonstrated that the constitutive and beta-naphthoflavone (beta-NF)-induced expression of the GCSh gene is mediated by a distal antioxidant response element (ARE), ARE4, located 3.1 kb upstream of the transcriptional start site [Mulcahy, Wartman, Bailey and Gipp (1997) J. Biol. Chem. 272, 7445-7454]. ARE4 consists of a consensus ARE sequence (5'-GTGACTCAGCG-3') containing an embedded PMA-responsive element (TRE, underlined). The relative significance of the two overlapping response elements to constitutive and beta-NF-induced expression of the GCSh gene was determined by mutational analyses. The internal activator protein-1 (AP-1)-binding sequence mediated constitutive expression of promoter/reporter transgenes, but was not required for beta-NF responsiveness. In gel-shift experiments, the TRE was necessary for binding of proteins from nuclear extracts prepared from untreated HepG2 cells. In contrast, induction by beta-NF was dependent on an intact ARE sequence, particularly the terminal GC box of ARE4. The GC box of ARE4 was shown to be essential for both basal and beta-NF-induced expression of reporter constructs. This element also influenced binding of nuclear proteins to ARE4, specifically in extracts isolated from beta-NF-treated HepG2 cells. Because previous studies indicated that ARE4 may co-operate with a separate putative ARE, the role of the neighbouring sequence (ARE3), located 34 bases downstream of ARE4, was also evaluated. Mutation of this element within a GCSh promoter/reporter did not modify the basal or beta-NF-induced expression of the transgene, demonstrating that ARE3 does not influence the constitutive or beta-NF-induced expression of the GCSh gene.

机译：γ-谷氨酰半胱氨酸合成酶（GCS）是GSH从头合成的限速酶，是一种异二聚体，由催化（GCSh）和调节亚基（GCS1）组成。我们先前证明，组成型和β-萘黄酮（β-NF）诱导的GCSh基因表达是由远端抗氧化反应元件（ARE）ARE4介导的，ARE4位于转录起始位点上游3.1 kb [Mulcahy，Wartman， Bailey和Gipp（1997）J.Biol。化学272，7445-7454]。 ARE4由一个共有的ARE序列（5'-GTGACTCAGCG-3'）组成，该序列包含一个嵌入的PMA响应元件（带下划线的TRE）。通过突变分析确定了两个重叠的响应元件对组成型和β-NF诱导的GCSh基因表达的相对重要性。内部激活蛋白-1（AP-1）绑定序列介导启动子/报告基因转基因的组成型表达，但不是β-NF反应性所必需的。在凝胶迁移实验中，TRE对于结合未经处理的HepG2细胞制备的核提取物中的蛋白质是必需的。相反，β-NF的诱导取决于完整的ARE序列，尤其是ARE4的末端GC盒。已证明ARE4的GC盒对于基础构建物和β-NF诱导的报告基因表达都至关重要。该元素还影响了核蛋白与ARE4的结合，特别是从β-NF处理过的HepG2细胞分离的提取物中。由于先前的研究表明ARE4可能与单独的推定ARE协同工作，因此还评估了位于ARE4下游34个碱基处的邻近序列（ARE3）的作用。 GCSh启动子/报告子中此元素的突变不会改变转基因的基础表达或β-NF诱导的表达，表明ARE3不会影响GCSh基因的组成性表达或β-NF诱导的表达。

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《The Biochemical Journal》 |1998年第2期|共9页
作者
Wild AC; Gipp JJ; Mulcahy T;
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正文语种 eng
中图分类生物化学;
关键词
beta-Naphthoflavone; Antioxidants; Gene Expression Regulation; Glutamate Cysteine Ligase genetics; β萘黄酮; 抗氧化药; 基因表达调控;

机译：beta-Naphthoflavone;Antioxidants;Gene Expression Regulation;Glutamate Cysteine Ligase genetics;β萘黄酮;抗氧化药;基因表达调控;

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1. Overlapping antioxidant response element and PMA responseelement sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene. [J] . Wild AC, Gipp JJ, Mulcahy T The Biochemical Journal . 1998,第Pta2期

机译：重叠的抗氧化剂应答元件和PMA应答元件序列介导了基础和β-萘黄酮诱导的人γ-谷氨酰半胱氨酸合成酶催化亚基基因的表达。
2. Overlapping antioxidant response element and PMA response element sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene [J] . Wild AC., Mulcahy RT., Gipp JJ. The Biochemical Journal . 1998,第Pta2期

机译：重叠的抗氧化剂应答元件和PMA应答元件序列介导基础和β-萘黄酮诱导的人γ-谷氨酰半胱氨酸合成酶催化亚基基因的表达
3. Overlapping antioxidant response element and PMA responseelement sequences mediate basal and β-naphthoflavone-induced expression of the human γ-glutamylcysteine synthetase catalytic subunit gene [J] . Angela C. WILD, Jerry J. GIPP, R. Timothy MULCAHY The biochemical journal . 1998,第2期

机译：重叠的抗氧化剂反应元件和PMA反应元件序列介导基础和β-萘黄酮诱导的人γ-谷氨酰半胱氨酸合成酶催化亚基基因的表达
4. Overlapping antioxidant response element and PMA response element sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene. [O] . A C Wild, J J Gipp, T Mulcahy 1998

机译：重叠的抗氧化剂反应元件和PMA反应元件序列介导了人γ-谷氨酰半胱氨酸合成酶催化亚基的基础和β-萘黄酮诱导的表达。
5. Constitutive and β-Naphthoflavone-induced Expression of the Human γ-Glutamylcysteine Synthetase Heavy Subunit Gene Is Regulated by a Distal Antioxidant Response Element/TRE Sequence [O] . R. Timothy Mulcahy, Marybeth A. Wartman, Howard H. Bailey, 1997

机译：本构和β-萘酚诱导的人γ-戊酰琥珀酰基合成酶重亚基基因的表达由远端抗氧化反应元素/ TRE序列调节

Overlapping antioxidant response element and PMA responseelement sequences mediate basal and beta-naphthoflavone-induced expression of the human gamma-glutamylcysteine synthetase catalytic subunit gene.

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