环磷酸腺苷反应元件结合蛋白的磷酸化是促肾上腺皮质激素释放激素转录激活所必需的,但并不充分。
Cyclic adenosine 3',5'-monophosphate responsive element binding protein phosphorylation is required but not sufficient for activation of corticotropin-releasing hormone transcription.
作者信息
Liu Ying, Kamitakahara Anna, Kim Alice Joohee, Aguilera Greti
机构信息
Section on Endocrine Physiology, Developmental Endocrinology Branch, National Institute of Child Health and Human Development, National Institutes of Health,10 Center Drive, Bethesda, MD 20892, USA.
出版信息
Endocrinology. 2008 Jul;149(7):3512-20. doi: 10.1210/en.2008-0052. Epub 2008 Mar 27.
cAMP is a major regulator of CRH transcription. However, receptors activating CRH neurons (alpha-adrenergic and glutamatergic) do not signal through cAMP, suggesting that calcium phospholipid-dependent signaling synergizes with small elevations of intracellular cAMP. To test this hypothesis, we examined the relationship between activation of CRH transcription, cAMP production, and cAMP response element binding protein (CREB) phosphorylation in neuronal cultures treated with the adenylyl cyclase stimulator, forskolin, the phorbol ester, phorbol-12-myristate-13-acetate (PMA), or their combination. Forskolin, at threshold concentrations for cAMP production and CREB phosphorylation, induced CRH promoter-driven luciferase activity in 4B cells (EC(50) = 0.7 microm) and CRH primary transcript in hypothalamic neurons (EC(50) = 0.6 microm). PMA alone failed to activate CRH transcription despite being as effective as forskolin in phosphorylating CREB (Ser133 and Ser121). Although PMA potentiated the effect of low forskolin concentrations on CRH transcription and CREB phosphorylation, there was no correlation between phosphorylated CREB levels and activation of CRH transcription. Similarly, the calcium/calmodulin-dependent kinase inhibitor, KN-93, enhanced PMA plus forskolin-stimulated CREB phosphorylation and inhibited CRH transcription. Suppression of CREB phosphorylation by the protein kinase A inhibitor, H89, or the CREB dominant negative, A-CREB, did not affect basal but blocked forskolin-stimulated transcription. This study shows that calcium phospholipid-dependent pathways potentiate the ability of small elevations of intracellular cAMP to activate CRH transcription, providing a mechanism by which non-cAMP-dependent regulators induce CRH gene expression. In addition, the data indicate that phosphorylated CREB is essential but not sufficient for activation of CRH transcription, suggesting that full promoter stimulation requires the interaction of phosphorylated CREB with a coactivator.
环磷酸腺苷(cAMP)是促肾上腺皮质激素释放激素(CRH)转录的主要调节因子。然而,激活CRH神经元的受体(α-肾上腺素能和谷氨酸能受体)并不通过cAMP进行信号传导,这表明钙磷脂依赖性信号传导与细胞内cAMP的小幅升高协同作用。为了验证这一假设,我们研究了在用腺苷酸环化酶刺激剂福斯可林、佛波酯、佛波醇-12-肉豆蔻酸酯-13-乙酸酯(PMA)或它们的组合处理的神经元培养物中,CRH转录激活、cAMP产生和cAMP反应元件结合蛋白(CREB)磷酸化之间的关系。福斯可林在产生cAMP和使CREB磷酸化的阈值浓度下,诱导4B细胞中CRH启动子驱动的荧光素酶活性(半数有效浓度[EC50]=0.7微摩尔)以及下丘脑神经元中的CRH初级转录本(EC50=0.6微摩尔)。单独的PMA尽管在使CREB(Ser133和Ser121)磷酸化方面与福斯可林一样有效,但未能激活CRH转录。尽管PMA增强了低浓度福斯可林对CRH转录和CREB磷酸化的作用,但磷酸化的CREB水平与CRH转录激活之间没有相关性。同样,钙/钙调蛋白依赖性激酶抑制剂KN-93增强了PMA加福斯可林刺激的CREB磷酸化,并抑制了CRH转录。蛋白激酶A抑制剂H89或CREB显性阴性突变体A-CREB对CREB磷酸化的抑制并不影响基础状态,但阻断了福斯可林刺激的转录。这项研究表明,钙磷脂依赖性途径增强了细胞内cAMP小幅升高激活CRH转录的能力,提供了一种非cAMP依赖性调节因子诱导CRH基因表达的机制。此外,数据表明磷酸化的CREB对于激活CRH转录是必不可少的,但并不充分,这表明完整的启动子刺激需要磷酸化的CREB与共激活因子相互作用。
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