首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Characterization of the cocaine- and amphetamine-regulated transcript (CART) peptide gene promoter and its activation by a cyclic AMP-dependent signaling pathway in GH3 cells.
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Characterization of the cocaine- and amphetamine-regulated transcript (CART) peptide gene promoter and its activation by a cyclic AMP-dependent signaling pathway in GH3 cells.

机译:可卡因和苯丙胺调节的转录物(CART)肽基因启动子的表征及其在GH3细胞中的依赖于环AMP依赖的信号通路的激活。

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摘要

Cocaine- and amphetamine-regulated transcript (CART) peptides are regulated neuropeptides that play a role in a variety of physiological processes. CART mRNA is also highly regulated as its levels change in response to psychostimulant drugs and leptin. To understand the mechanisms involved in regulating CART mRNA levels, the mouse CART 5'-flanking regulatory region was studied. The sequence of 3.4 kb of the mouse CART 5'-flanking region revealed a proximal promoter that contains a cluster of transcription factor binding sites, including an overlapping STAT/CRE/AP1 site. In addition, the 5'-most 320 bp of the CART promoter shares 83% nucleotide identity between mouse and human. Three luciferase expressing constructs containing varying amounts of CART 5' upstream sequence were generated and tested for promoter activity. Transient transfection of GH3 cells with constructs containing 641 and 3451 bp of upstream sequence displayed strong promoter activity, producing 29-fold and 51-fold stimulation, respectively, while, a construct containing 102 bp of upstream sequence displayed a 5.4-fold increase in activity. A construct containing the composite STAT/CRE/AP1 site was responsive to cyclic AMP induction by forskolin in GH3 cells. Forskolin treatment also resulted in a 4.5-fold increase in CART mRNA levels after 6 h and the addition of H89, an inhibitor of protein kinase A, reduced the levels by 50%. These studies indicate that the CART proximal promoter lies within the 5'-most 641 bp and that in GH3 cells the CART gene is regulated via a cyclic AMP-dependent pathway.
机译:可卡因和苯丙胺调节的转录物(CART)肽是在多种生理过程中起作用的受调节的神经肽。由于CART mRNA的水平随着对精神刺激药和瘦素的反应而变化,因此也受到高度调节。为了了解调节CART mRNA水平的机制,研究了小鼠CART 5'侧翼调控区。小鼠CART 5'侧翼区的3.4 kb序列揭示了一个近端启动子,其中包含转录因子结合位点簇,包括一个重叠的STAT / CRE / AP1位点。此外,CART启动子的5'-最远320 bp在小鼠和人之间共有83%的核苷酸同一性。产生了三种含有不同量的CART 5'上游序列的表达荧光素酶的构建体,并测试了其启动子活性。用含有641和3451 bp上游序列的构建体瞬时转染GH3细胞表现出强大的启动子活性,分别产生29倍和51倍的刺激,而含有102 bp上游序列的构建体显示出5.4倍的活性增加。包含复合STAT / CRE / AP1位点的构建体对GH3细胞中毛喉素对环AMP的诱导有反应。 Forskolin处理还导致6小时后CART mRNA水平增加4.5倍,并且添加H89(蛋白激酶A抑制剂)可使水平降低50%。这些研究表明,CART近端启动子位于5'-最上端641 bp之内,并且在GH3细胞中,CART基因是通过环状AMP依赖性途径调控的。

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