六甲铵在体外与毒蕈碱受体亚型的相互作用。

The interaction of hexamethonium with muscarinic receptor subtypes in vitro.

作者信息

Eglen R M, Michel A D, Cornett C M, Kunysz E A, Whiting R L

机构信息

Institute of Pharmacology, Syntex Research, Palo Alto, CA 94303.

出版信息

Br J Pharmacol. 1989 Oct;98(2):499-506. doi: 10.1111/j.1476-5381.1989.tb12623.x.

DOI:10.1111/j.1476-5381.1989.tb12623.x

PMID:2819331

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1854706/

Abstract

The action of hexamethonium has been studied at a range of muscarinic receptors in vitro by use of both functional and radioligand binding studies. 2. In functional studies, hexamethonium exhibited little or no significant (P less than 0.05) antagonism of contractile responses to carbachol at muscarinic receptors in the guinea-pig ileum, oesophageal muscularis mucosae, urinary bladder and trachea. However, antagonism was observed at muscarinic receptors in the guinea-pig left atria mediating negative inotropic responses and the calculated pKB value was 3.80. Hexamethonium also antagonized contractile responses to carbachol in the canine saphenous vein. The pKB value at these receptors was 3.75. 3. In the presence of 3.2 mM hexamethonium, the pA2 value for methoctramine at atrial muscarinic receptors was reduced by approximately 10 fold (control pA2 value was 7.81 +/- 0.05; pA2 value in hexamethonium was 6.73 +/- 0.04). In contrast at tracheal muscarinic receptors, the pA2 values for methoctramine were unaffected in the presence of 3.2 mM hexamethonium (control pA2 = 5.58 +/- 0.07; pA2 value in hexamethonium was 5.63 +/- 0.12). All values quoted are mean +/- s.e. mean, n = 8. 4. In competition radioligand binding studies, hexamethonium exhibited a higher affinity for cardiac M2 receptors (pKi = 3.68) than for cerebrocortical M1 receptors (pKi = 3.28) or for submaxillary gland M3 receptors (pKi = 2.61). At M2 receptors hexamethonium at concentrations of 0.1-10 mM, increased the half life of the dissociation rate of [3H]-N-methylscopolamine 1.6-4.3 fold. This was observed at M3 receptors only at 10 mM, when the half life was increased 1.7 fold. 5. We conclude that hexamethonium, in addition to its well characterized nicotinic antagonist properties, can act as a weak muscarinic antagonist and differentiates between cardiac M2 receptors and glandular/smooth muscle M3 receptors. However, hexamethonium differentiates less clearly between M1 and M2 receptors. The selectivity between M2 and M3 receptors observed in the present study with hexamethonium is comparable to other M2 selective antagonists such as AF-DX 116 and himbacine. 6. Caution should be exercised with regard to the inclusion of hexamethonium in functionsal studies of M2 muscarinic receptor subtypes at concentrations of 0.1 mm and above.

摘要

已通过功能研究和放射性配体结合研究，在一系列毒蕈碱受体上对六甲铵的作用进行了体外研究。2. 在功能研究中，六甲铵对豚鼠回肠、食管肌层黏膜、膀胱和气管中毒蕈碱受体介导的卡巴胆碱收缩反应几乎没有或没有显著（P<0.05）拮抗作用。然而，在豚鼠左心房介导负性变力反应的毒蕈碱受体上观察到了拮抗作用，计算得到的pKB值为3.80。六甲铵还拮抗了犬隐静脉对卡巴胆碱的收缩反应。这些受体处的pKB值为3.75。3. 在存在3.2 mM六甲铵的情况下，心房毒蕈碱受体上甲氧基氨的pA2值降低了约10倍（对照pA2值为7.81±0.05；六甲铵存在时的pA2值为6.73±0.04）。相比之下，在气管毒蕈碱受体处，3.2 mM六甲铵存在时甲氧基氨的pA2值未受影响（对照pA2 = 5.58±0.07；六甲铵存在时的pA2值为5.63±0.12）。所有引用值均为平均值±标准误，n = 8。4. 在竞争性放射性配体结合研究中，六甲铵对心脏M2受体（pKi = 3.68）的亲和力高于对大脑皮质M1受体（pKi = 3.28）或颌下腺M3受体（pKi = 2.61）的亲和力。在M2受体处，浓度为0.1 - 10 mM的六甲铵使[3H]-N-甲基东莨菪碱解离速率的半衰期增加了1.6 - 4.3倍。仅在10 mM时在M3受体处观察到这种情况，此时半衰期增加了1.7倍。5. 我们得出结论，六甲铵除了具有其已充分表征的烟碱拮抗剂特性外，还可作为一种弱毒蕈碱拮抗剂，并且能区分心脏M2受体和腺体/平滑肌M3受体。然而，六甲铵在M1和M2受体之间的区分不太明显。本研究中观察到的六甲铵对M2和M3受体的选择性与其他M2选择性拮抗剂如AF-DX 116和辛巴因相当。6. 在M2毒蕈碱受体亚型的功能研究中，当浓度为0.1 mM及以上时，应谨慎使用六甲铵。