McKinney M, Stenstrom S, Richelson E
Mol Pharmacol. 1985 Feb;27(2):223-35.
Murine neuroblastoma cells (clone N1E-115) possess muscarinic receptors that mediate multiple responses, including the elevation of cyclic GMP levels and the inhibition of receptor-mediated increases in cyclic AMP. Evidence is presented showing that two muscarinic agonist-receptor conformations in N1E-115 cells each separately mediate a cyclic nucleotide response. Pirenzepine inhibited the [3H]cyclic GMP response to carbachol with a KD value of approximately 6 nM, whereas it inhibited the ability of carbachol to reduce prostaglandin E1-mediated elevations in [3H]cyclic AMP levels with a KD value of 93 nM, thus differentiating between two classes of receptors involved in these responses. Ten muscarinic agonists were studied for their ability to mediate the two cyclic nucleotide responses. Six were as effective as acetylcholine in the reduction of [3H]cyclic AMP levels, but only two were as effective as acetylcholine in elevating [3H]cyclic GMP levels. Four agonists (arecoline, pilocarpine, oxotremorine, and McN-A343) were ineffective in increasing [3H]cyclic GMP levels. These four agonists and bethanecol, which could increase [3H]cyclic GMP levels only 18% as well as acetylcholine, behaved as competitive antagonists in this response to carbachol. These partial agonists, in contrast to carbachol, bound to only one class of muscarinic sites in N1E-115 cells with equilibrium dissociation constants determined by competition binding assays which agreed well with their respective EC50 values for their effect on [3H]cyclic AMP levels. The equilibrium dissociation constants for the partial agonists determined by their inhibition of carbachol in the [3H] cyclic GMP response also agreed well with their respective EC50 values for mediating the [3H]cyclic AMP response. Thus, the partial agonists bound to the same receptors at which carbachol mediated [3H]cyclic GMP formation, but with KD values about the same as their respective EC50 values for inhibition of prostaglandin E1-mediated [3H]cyclic AMP increases. The full agonists acetylcholine and methacholine, like carbachol, bound to two sites in N1E-115 cells. For the six agonists able to stimulate both responses at least to some degree, the ratio of their potencies at each response correlated with their respective efficacies at each response but with much more dependence in the [3H]cyclic GMP response.(ABSTRACT TRUNCATED AT 400 WORDS)
小鼠神经母细胞瘤细胞(克隆N1E - 115)拥有介导多种反应的毒蕈碱受体,包括环鸟苷酸水平的升高以及对受体介导的环磷酸腺苷增加的抑制。有证据表明,N1E - 115细胞中的两种毒蕈碱激动剂 - 受体构象各自分别介导一种环核苷酸反应。哌仑西平抑制卡巴胆碱引起的[3H]环鸟苷酸反应,其KD值约为6 nM,而它抑制卡巴胆碱降低前列腺素E1介导的[3H]环磷酸腺苷水平升高的能力,KD值为93 nM,从而区分了参与这些反应的两类受体。研究了十种毒蕈碱激动剂介导两种环核苷酸反应的能力。六种在降低[3H]环磷酸腺苷水平方面与乙酰胆碱效果相同,但只有两种在升高[3H]环鸟苷酸水平方面与乙酰胆碱效果相同。四种激动剂(槟榔碱、毛果芸香碱、氧化震颤素和McN - A343)在升高[3H]环鸟苷酸水平方面无效。这四种激动剂以及仅能将[3H]环鸟苷酸水平升高至乙酰胆碱18%的氨甲酰甲胆碱,在对卡巴胆碱的这种反应中表现为竞争性拮抗剂。与卡巴胆碱不同,这些部分激动剂在N1E - 115细胞中仅与一类毒蕈碱位点结合,通过竞争结合测定确定的平衡解离常数与它们对[3H]环磷酸腺苷水平影响的各自EC50值非常吻合。由它们在[3H]环鸟苷酸反应中抑制卡巴胆碱所确定的部分激动剂的平衡解离常数也与它们介导[3H]环磷酸腺苷反应的各自EC50值非常吻合。因此,部分激动剂与卡巴胆碱介导[3H]环鸟苷酸形成的相同受体结合,但其KD值与它们抑制前列腺素E1介导的[3H]环磷酸腺苷增加的各自EC50值大致相同。完全激动剂乙酰胆碱和醋甲胆碱与卡巴胆碱一样,在N1E - 115细胞中与两个位点结合。对于能够至少在一定程度上刺激两种反应的六种激动剂,它们在每种反应中的效价之比与它们在每种反应中的各自效能相关,但在[3H]环鸟苷酸反应中的依赖性更强。(摘要截短至400字)
