在非洲爪蟾卵母细胞中表达的重组人神经元烟碱型乙酰胆碱受体hα2β2、hα2β4、hα3β2、hα3β4、hα4β2、hα4β4和hα7的药理学特性
Pharmacological characterization of recombinant human neuronal nicotinic acetylcholine receptors h alpha 2 beta 2, h alpha 2 beta 4, h alpha 3 beta 2, h alpha 3 beta 4, h alpha 4 beta 2, h alpha 4 beta 4 and h alpha 7 expressed in Xenopus oocytes.
作者信息
Chavez-Noriega L E, Crona J H, Washburn M S, Urrutia A, Elliott K J, Johnson E C
机构信息
SIBIA Neurosciences, Inc., La Jolla, California, USA.
出版信息
J Pharmacol Exp Ther. 1997 Jan;280(1):346-56.
Human neuronal nicotinic acetylcholine receptors (nAChRs) h alpha 2 beta 2, h alpha 2 beta 4, h alpha 3 beta 2, h alpha 3 beta 4, h alpha 4 beta 2, h alpha 4 beta 4 and h alpha 7 were expressed in Xenopus oocytes and tested for their sensitivities to the nicotinic agonists acetylcholine (ACh), nicotine, cytisine (CYT) and 1,1-dimethyl-4-phenylpiperazinium (DMPP) and the nAChR. antagonists mecamylamine (MEC), d-tubocurarine and dihydro-beta-erythroidine. CYT was the least efficacious agonist at hnAChRs containing beta 2 subunits, but it displayed significant activity at h alpha 2 beta 4, h alpha 3 beta 4, h alpha 4 beta 4 and h alpha 7 nAChRs. ACh was one of the most efficacious agonists at all hnAChRs, except at h alpha 3 beta 2, where DMPP was markedly more efficacious than ACh. ACh was among the least potent agonists at all hnAChRs. The rank order of potency displayed by h alpha 3 beta 2 and h alpha 3 beta 4 nAChRs (DMPP approximately CYT approximately nicotine > ACh and DMPP > CYT approximately nicotine > ACh, respectively), differs from that reported for their rat homologs (Luetje and Patrick, 1991; Covernton et al., 1994). The agonist profile observed in h alpha 7 also differs from that reported for its rat homolog (Seguela et al., 1993). Human alpha 4 beta 2 and h alpha 4 beta 4 nAChRs were more sensitive to dihydro-beta-erythroidine than d-tubocurarine, whereas h alpha 7 and h alpha 3 beta 4 were more sensitive to d-tubocurarine than dihydro-beta-erythroidine. These antagonists were equipotent at h alpha 2 beta 2, h alpha 3 beta 2 and h alpha 2 beta 4 nAChRs. MEC (3 microM) inhibited h alpha 2 beta 4 and h alpha 4 beta 4 nAChRs by > 80%, whereas h alpha 2 beta 2, h alpha 4 beta 2 and h alpha 7 nAChRs were inhibited by approximately 50%. Taken together, the differential sensitivities observed at various recombinant hnAChR subtypes indicate that both alpha and beta subunits contribute to the pharmacology of these ligand-gated channels. The unique selectivity profiles displayed by human nAChRs constitute a valuable tool for the development of selective nicotinic analogs as potential therapeutic drugs.
人类神经元烟碱型乙酰胆碱受体(nAChRs)hα2β2、hα2β4、hα3β2、hα3β4、hα4β2、hα4β4和hα7在非洲爪蟾卵母细胞中表达,并测试它们对烟碱型激动剂乙酰胆碱(ACh)、尼古丁、金雀花碱(CYT)和1,1 - 二甲基 - 4 - 苯基哌嗪鎓(DMPP)以及nAChR拮抗剂美加明(MEC)、d - 筒箭毒碱和二氢β - 刺桐啶的敏感性。CYT是对含有β2亚基的hnAChRs作用最弱的激动剂,但它在hα2β4、hα3β4、hα4β4和hα7 nAChRs上显示出显著活性。ACh是除hα3β2外所有hnAChRs中最有效的激动剂之一,在hα3β2中DMPP比ACh明显更有效。ACh是所有hnAChRs中效力最弱的激动剂之一。hα3β2和hα3β4 nAChRs显示的效力顺序(分别为DMPP≈CYT≈尼古丁>ACh和DMPP>CYT≈尼古丁>ACh)与它们大鼠同源物报道的顺序不同(Luetje和Patrick,1991;Covernton等人,1994)。在hα7中观察到的激动剂特征也与其大鼠同源物报道的不同(Seguela等人,1993)。人类α4β2和hα4β4 nAChRs对二氢β - 刺桐啶比对d - 筒箭毒碱更敏感,而hα7和hα3β4对d - 筒箭毒碱比对二氢β - 刺桐啶更敏感。这些拮抗剂在hα2β2、hα3β2和hα2β4 nAChRs上效力相当。MEC(3μM)对hα2β4和hα4β4 nAChRs的抑制率>80%,而hα2β2、hα4β2和hα7 nAChRs的抑制率约为50%。综上所述,在各种重组hnAChR亚型中观察到的不同敏感性表明α和β亚基都对这些配体门控通道的药理学有贡献。人类nAChRs显示的独特选择性特征构成了开发选择性烟碱类似物作为潜在治疗药物的有价值工具。
Zotero 插件