cAMP 类似物及其代谢产物可增强肾上腺皮质细胞中 TREK-1 mRNA 和 K+ 电流的表达。
cAMP analogs and their metabolites enhance TREK-1 mRNA and K+ current expression in adrenocortical cells.
机构信息
Department of Neuroscience, The Ohio State University, College of Medicine and Public Health, 5196 Graves Hall, 333 West 10th Avenue, Columbus, OH 43210-1239, USA.
出版信息
Mol Pharmacol. 2010 Mar;77(3):469-82. doi: 10.1124/mol.109.061861. Epub 2009 Dec 22.
bTREK-1 K(+) channels set the resting membrane potential of bovine adrenal zona fasciculata (AZF) cells and function pivotally in the physiology of cortisol secretion. Adrenocorticotropic hormone controls the function and expression of bTREK-1 channels through signaling mechanisms that may involve cAMP and downstream effectors including protein kinase A (PKA) and exchange protein 2 directly activated by cAMP (Epac2). Using patch-clamp and Northern blot analysis, we explored the regulation of bTREK-1 mRNA and K(+) current expression by cAMP analogs and several of their putative metabolites in bovine AZF cells. At concentrations sufficient to activate both PKA and Epac2, 8-bromoadenosine-cAMP enhanced the expression of both bTREK-1 mRNA and K(+) current. N(6)-Benzoyladenosine-cAMP, which activates PKA but not Epac, also enhanced the expression of bTREK-1 mRNA and K(+) current measured at times from 24 to 96 h. An Epac-selective cAMP analog, 8-(4-chlorophenylthio)-2'-O-methyl-cAMP (8CPT-2'-OMe-cAMP), potently stimulated bTREK-1 mRNA and K(+) current expression, whereas the nonhydrolyzable Epac activator 8-(4-chlorophenylthio)-2'-O-methyl-cAMP, Sp-isomer was ineffective. Metabolites of 8CPT-2'-OMe-cAMP, including 8-(4-chlorophenylthio)-2'-O-methyladenosine-5'-O-monophosphate and 8CPT-2'-OMe-adenosine, promoted the expression of bTREK-1 transcripts and ion current with a temporal pattern, potency, and effectiveness resembling that of the parent compound. Likewise, at low concentrations, 8-(4-chlorophenylthio)-cAMP (8CPT-cAMP; 30 microM) but not its nonhydrolyzable analog 8-(4-chlorophenylthio)-cAMP, Sp-isomer, enhanced the expression of bTREK-1 mRNA and current. 8CPT-cAMP metabolites, including 8CPT-adenosine and 8CPT-adenine, also increased bTREK-1 expression. These results indicate that cAMP increases the expression of bTREK-1 mRNA and K(+) current through a cAMP-dependent but Epac2-independent mechanism. They further demonstrate that one or more metabolites of 8-(4-chlorophenylthio)-cAMP analogs potently stimulate bTREK-1 expression by activation of a novel cAMP-independent mechanism. These findings raise significant questions regarding the specificity of 8-(4-chlorophenylthio)-cAMP analogs as cAMP mimetics.
bTREK-1 K(+) 通道设定牛肾上腺束状带(AZF)细胞的静息膜电位,并在皮质醇分泌的生理学中起着关键作用。促肾上腺皮质激素通过可能涉及环磷酸腺苷(cAMP)和下游效应物(包括蛋白激酶 A(PKA)和直接由 cAMP 激活的交换蛋白 2(Epac2))的信号机制来控制 bTREK-1 通道的功能和表达。使用膜片钳和 Northern blot 分析,我们研究了 cAMP 类似物及其几种假定代谢物对牛 AZF 细胞中 bTREK-1 mRNA 和 K(+) 电流表达的调节。在足以激活 PKA 和 Epac2 的浓度下,8-溴腺苷-cAMP 增强了 bTREK-1 mRNA 和 K(+) 电流的表达。N(6)-苯甲酰基腺苷-cAMP 虽然激活了 PKA,但不激活 Epac,也增强了 bTREK-1 mRNA 和 K(+) 电流的表达,在 24 至 96 小时的时间内测量。Epac 选择性 cAMP 类似物 8-(4-氯苯基硫代)-2'-O-甲基-cAMP(8CPT-2'-OMe-cAMP)强烈刺激 bTREK-1 mRNA 和 K(+) 电流表达,而非水解的 Epac 激活剂 8-(4-氯苯基硫代)-2'-O-甲基-cAMP,Sp-异构体则无效。8CPT-2'-OMe-cAMP 的代谢物,包括 8-(4-氯苯基硫代)-2'-O-甲基腺苷-5'-O-单磷酸和 8CPT-2'-OMe-腺苷,以类似于母体化合物的时间模式、效力和有效性促进 bTREK-1 转录物和离子电流的表达。同样,在低浓度下,8-(4-氯苯基硫代)-cAMP(8CPT-cAMP;30 μM)但不是其非水解类似物 8-(4-氯苯基硫代)-cAMP,Sp-异构体增强了 bTREK-1 mRNA 和电流的表达。8CPT-cAMP 的代谢物,包括 8CPT-腺苷和 8CPT-腺嘌呤,也增加了 bTREK-1 的表达。这些结果表明,cAMP 通过 cAMP 依赖性但 Epac2 独立的机制增加 bTREK-1 mRNA 和 K(+) 电流的表达。它们进一步表明,8-(4-氯苯基硫代)-cAMP 类似物的一种或多种代谢物通过激活一种新的 cAMP 非依赖性机制强烈刺激 bTREK-1 的表达。这些发现引发了关于 8-(4-氯苯基硫代)-cAMP 类似物作为 cAMP 模拟物的特异性的重大问题。
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