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编码PKI(1 - 31)(一种环磷酸腺苷(cAMP)刺激的基因表达的特异性抑制剂)的质粒,抑制JEG - 3细胞中部分而非全部cAMP调节的DNA反应元件的基础转录活性。

Plasmids encoding PKI(1-31), a specific inhibitor of cAMP-stimulated gene expression, inhibit the basal transcriptional activity of some but not all cAMP-regulated DNA response elements in JEG-3 cells.

作者信息

Grove J R, Deutsch P J, Price D J, Habener J F, Avruch J

机构信息

Howard Hughes Medical Institute Laboratory, Harvard Medical School, Boston, Massachusetts.

出版信息

J Biol Chem. 1989 Nov 25;264(33):19506-13.

PMID:2479635
Abstract

Plasmids that encode a bioactive amino-terminal fragment of the heat-stable inhibitor of the cAMP-dependent protein kinase, PKI(1-31), were employed to characterize the role of this protein kinase in the control of transcriptional activity mediated by three DNA regulatory elements in the JEG-3 human placental cell line. The 5'-flanking sequence of the human collagenase gene contains the heptameric sequence, 5'-TGAGTCA-3', previously identified as a "phorbol ester" response element. Reporter genes containing either the intact 1.2-kilobase 5'-flanking sequence from the human collagenase gene or just the 7-base pair (bp) response element, when coupled to an enhancerless promoter, each exhibit both cAMP and phorbol ester-stimulated expression in JEG-3 cells. Cotransfection of either construct with plasmids encoding PKI(1-31) inhibits cAMP-stimulated but not basal- or phorbol ester-stimulated expression. Pretreatment of cells with phorbol ester for 1 or 2 days abrogates completely the response to rechallenge with phorbol ester but does not alter the basal expression of either construct; cAMP-stimulated expression, while modestly inhibited, remains vigorous. The 5'-flanking sequence of the human chorionic gonadotropin-alpha subunit (HCG alpha) gene has two copies of the sequence, 5'-TGACGTCA-3', contained in directly adjacent identical 18-bp segments, previously identified as a cAMP-response element. Reporter genes containing either the intact 1.5 kilobase of 5'-flanking sequence from the HCG alpha gene, or just the 36-bp tandem repeat cAMP response element, when coupled to an enhancerless promoter, both exhibit a vigorous cAMP stimulation of expression but no response to phorbol ester in JEG-3 cells. Cotransfection with plasmids encoding PKI(1-31) inhibits both basal and cAMP-stimulated expression in a parallel fashion. The 5'-flanking sequence of the human enkephalin gene mediates cAMP-stimulated expression of reporter genes in both JEG-3 and CV-1 cells. Plasmids encoding PKI(1-31) inhibit the expression that is stimulated by the addition of cAMP analogs in both cell lines; basal expression, however, is inhibited by PKI(1-31) only in the JEG-3 cell line and not in the CV-1 cells. These observations indicate that, in JEG-3 cells, PKI(1-31) is a specific inhibitor of kinase A-mediated gene transcription, but it does not modify kinase C-directed transcription.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

编码环磷酸腺苷(cAMP)依赖性蛋白激酶热稳定抑制剂PKI(1 - 31)生物活性氨基末端片段的质粒,被用于在JEG - 3人胎盘细胞系中表征该蛋白激酶在由三个DNA调控元件介导的转录活性控制中的作用。人胶原酶基因的5'侧翼序列包含七聚体序列5'-TGAGTCA-3',该序列先前被鉴定为“佛波酯”反应元件。当与无增强子启动子偶联时,含有来自人胶原酶基因完整的1.2千碱基5'侧翼序列或仅7碱基对(bp)反应元件的报告基因,在JEG - 3细胞中均表现出cAMP和佛波酯刺激的表达。用编码PKI(1 - 31)的质粒与任一构建体共转染可抑制cAMP刺激的表达,但不抑制基础表达或佛波酯刺激的表达。用佛波酯预处理细胞1或2天可完全消除对再次用佛波酯刺激的反应,但不改变任一构建体的基础表达;cAMP刺激的表达虽略有抑制,但仍很活跃。人绒毛膜促性腺激素α亚基(HCGα)基因的5'侧翼序列在直接相邻的相同18 bp片段中含有两个5'-TGACGTCA-3'序列拷贝,该序列先前被鉴定为cAMP反应元件。当与无增强子启动子偶联时,含有来自HCGα基因完整的1.5千碱基5'侧翼序列或仅36 bp串联重复cAMP反应元件的报告基因,在JEG - 3细胞中均表现出强烈的cAMP刺激的表达,但对佛波酯无反应。用编码PKI(1 - 31)的质粒共转染以平行方式抑制基础表达和cAMP刺激的表达。人脑啡肽基因的5'侧翼序列在JEG - 3和CV - 1细胞中介导报告基因的cAMP刺激的表达。编码PKI(1 - 31)的质粒在两种细胞系中均抑制由添加cAMP类似物刺激的表达;然而,基础表达仅在JEG - 3细胞系中被PKI(1 - 31)抑制,而在CV - 1细胞中未被抑制。这些观察结果表明,在JEG - 3细胞中,PKI(1 - 31)是激酶A介导的基因转录的特异性抑制剂,但它不改变激酶C指导的转录。(摘要截短至400字)

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