介导大鼠主动脉对去甲肾上腺素收缩反应的α1D肾上腺素能受体的特性研究
Characterization of an alpha 1D-adrenoceptor mediating the contractile response of rat aorta to noradrenaline.
作者信息
Kenny B A, Chalmers D H, Philpott P C, Naylor A M
机构信息
Department of Discovery Biology, Pfizer Central Research, Sandwich, Kent.
出版信息
Br J Pharmacol. 1995 Jul;115(6):981-6. doi: 10.1111/j.1476-5381.1995.tb15907.x.
Abstract
- The affinities of a number of alpha 1-adrenoceptor antagonists were determined by displacement of [3H]-prazosin binding from cloned human alpha 1A-adrenoceptors (previously designated cloned alpha 1c subtype), alpha 1B alpha 1D and rat alpha 1D-adrenoceptors, stably expressed in rat-1 fibroblasts. Functional affinity estimates for these compounds were also determined from noradrenaline-mediated contractions of rat aorta. 2. BMY 7378 displayed high affinity for cloned human alpha 1D-adrenoceptors (pKi = 8.2 +/- 0.10) and was selective over alpha 1A (pKi = 6.2 +/- 0.10) and alpha 1B subtypes (6.7 +/- 0.11). WB 4101, benoxathian and phentolamine displayed high affinity for alpha 1A and alpha 1D adrenoceptors compared to the alpha 1B subtype. Spiperone displayed high affinity and selectivity for alpha 1B adrenoceptors (pKi 8.8 +/- 0.16). 5-Methyl-urapidil was selective for cloned alpha 1A adrenoceptors. 3. Comparative binding affinities (pKi) for compounds at cloned human and rat1D adrenoceptors were almost identical (r = 0.99, slope = 1.08). 4. Prazosin, doxazosin and 5-methyl-urapidil were potent, competitive antagonists of noradrenaline-mediated contractions of rat aorta (pA2 values of 9.8, 8.8 and 7.8 respectively). The selective alpha 1D antagonist BMY 7378 was also a potent antagonist on rat aorta (pKB = 8.3 +/- 0.1) but the interaction of this compound was not consistent with competitive antagonism at a single population of receptors. 5. Functional affinities for compounds determined against noradrenaline-mediated contractions of rat aorta correlated well with binding affinities at cloned alpha 1D-adrenoceptors (r = 0.96), but not with alpha 1A (r = 0.61) or alpha 1B (r = 0.46) subtypes. 6. Noradrenaline-mediated contractions of rat aorta were sensitive to the alkylating effects of chlorethylclonidine (CEC). CEC (10 microM) caused a small rightward shift in the noradrenaline concentration-response curve. CEC at 100 microM caused a further shift and suppression of the maximum response to noradrenaline.7. The results of this study suggest that noradrenaline predominantly, but not exclusively, mediates contraction of rat aorta through the activation of an alphalD-adrenoceptor.
摘要
- 通过[3H]-哌唑嗪与克隆的人α1A-肾上腺素能受体(先前称为克隆的α1c亚型)、α1B、α1D以及在大鼠-1成纤维细胞中稳定表达的大鼠α1D-肾上腺素能受体的结合置换,测定了多种α1-肾上腺素能受体拮抗剂的亲和力。还通过去甲肾上腺素介导的大鼠主动脉收缩来确定这些化合物的功能亲和力估计值。2. BMY 7378对克隆的人α1D-肾上腺素能受体表现出高亲和力(pKi = 8.2±0.10),并且对α1A(pKi = 6.2±0.10)和α1B亚型(6.7±0.11)具有选择性。与α1B亚型相比,WB 4101、贝诺噻嗪和酚妥拉明对α1A和α1D肾上腺素能受体表现出高亲和力。螺哌隆对α1B肾上腺素能受体表现出高亲和力和选择性(pKi 8.8±0.16)。5-甲基-乌拉地尔对克隆的α1A肾上腺素能受体具有选择性。3. 化合物在克隆的人α1D和大鼠α1D肾上腺素能受体上的比较结合亲和力(pKi)几乎相同(r = 0.99,斜率 = 1.08)。4. 哌唑嗪、多沙唑嗪和5-甲基-乌拉地尔是去甲肾上腺素介导的大鼠主动脉收缩的强效竞争性拮抗剂(pA2值分别为9.8、8.8和7.8)。选择性α1D拮抗剂BMY 7378对大鼠主动脉也是一种强效拮抗剂(pKB = 8.3±0.1),但该化合物的相互作用与在单一受体群体上的竞争性拮抗作用不一致。5. 针对去甲肾上腺素介导的大鼠主动脉收缩测定的化合物功能亲和力与在克隆的α1D-肾上腺素能受体上的结合亲和力相关性良好(r = 0.96),但与α1A(r = 0.61)或α1B(r = 0.46)亚型无关。6. 去甲肾上腺素介导的大鼠主动脉收缩对氯乙可乐定(CEC)的烷基化作用敏感。CEC(10μM)使去甲肾上腺素浓度-反应曲线出现小的右移。100μM的CEC导致进一步右移并抑制对去甲肾上腺素的最大反应。7. 本研究结果表明,去甲肾上腺素主要但并非唯一地通过激活α1D-肾上腺素能受体介导大鼠主动脉收缩。
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