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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Cyclic AMP potentiates substance P-induced amylase secretion by augmenting the effect of calcium in the rat parotid acinar cells
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Cyclic AMP potentiates substance P-induced amylase secretion by augmenting the effect of calcium in the rat parotid acinar cells

机译:环状AMP通过增强大鼠腮腺腺泡细胞中钙的作用来增强P诱导的淀粉酶分泌

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Potentiation of amylase secretion by the combination of isoproterenol and substance P was examined in perfused rat parotid acinar cells. Combined additions of substance P and isoproterenol evoked biphasic changes in amylase secretion, an initial large peak and the following sustained plateau: the magnitudes of the both responses were higher than the sum of the responses induced by each agonist along. Isoproterenol also increased the maximum response and the apparent affinity (EC_(50)) for substance P to evoke the initial peak response; the EC_(50) values were about 20 and 0.8 nM, respectively, in the absence and the presence of isoproterenol. On the other hand, 1 nM substance P was sufficient for evoking the maximum potentiation of the sustained plateau response. Substance P did not change the EC_(50) for isoproterenol. The effect of isoproterenol was mimicked with dibutyryl cyclic AMP and agonists that increase parotid cyclic AMP. Omission of Ca~(2+) or addition of 5 mM nickel chloride almost completely abolished the potentiation of the sustained plateau, but little decreased that of the initial peak. Depletion of Ca~(2+) in InsP_3-sensitive intracellular stores with thapsigargin, on the other hand, decreased the initial peak response, but not the sustained plateau, to substance P. The potentiation was also observed between isoproterenol and Ca~(2+) ionophores. Switching to the solutions containing higher concentrations of Ca~(2+) during the continuous stimulation with isoproterenol or IBMX evoked a large, but transient, response of amylase secretion. Time course of changes in amylase secretion induced by isoproterenol and substance P in combination was very similar to that of substance P, but not of isoproterenol. Isoproterenol did not enhance the effect of substance p on [Ca~(2+)]_i. These results show that the potentiation is mainly, if not totally, caused by cyclic AMP-induced enhancement of the potency and the efficacy in the pathway regulated by Ca~(2+).
机译:在灌流的大鼠腮腺腺泡细胞中检查了异丙肾上腺素和P物质的组合对淀粉酶分泌的增强作用。物质P和异丙肾上腺素的组合添加引起淀粉酶分泌的双相变化,一个初始大峰和以下持续的平稳期:这两个反应的幅度都高于每个激动剂诱导的反应总和。异丙肾上腺素还增加了物质P的最大响应和表观亲和力(EC_(50)),以引起初始峰值响应。在不存在和存在异丙肾上腺素的情况下,EC_(50)值分别约为20和0.8 nM。另一方面,1 nM物质P足以引起持续高原反应的最大增强。 P物质未改变异丙肾上腺素的EC_(50)。异丙基肾上腺素的效果与二丁酰环AMP和增加腮腺环AMP的激动剂相似。省略Ca〜(2+)或添加5 mM氯化镍几乎完全消除了持续高原的增强作用,但几乎没有降低初始峰的增强作用。另一方面,用毒胡萝卜素使InsP_3敏感的细胞内存储中Ca〜(2+)的减少降低了对P物质的初始峰响应,但并没有持续的平台期。还观察到异丙肾上腺素和Ca〜(2)之间的增强作用。 +)离子载体。在用异丙肾上腺素或IBMX连续刺激过程中,切换到含有较高浓度Ca〜(2+)的溶液引起了淀粉酶分泌的大而短暂的反应。异丙肾上腺素和P物质联合引起的淀粉酶分泌变化的时间过程与P物质非常相似,但与异丙肾上腺素的变化却非常相似。异丙肾上腺素不会增强p物质对[Ca〜(2 +)] _ i的作用。这些结果表明,增强作用主要是(如果不是全部)由循环AMP诱导的效能增强以及Ca〜(2+)调节的途径中的功效引起。

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