(-)-地散胺,一种从青藤仔中分离得到的选择性α1D肾上腺素能受体拮抗剂。
(-)-Discretamine, a selective alpha 1D-adrenoceptor antagonist, isolated from Fissistigma glaucescens.
作者信息
Ko F N, Guh J H, Yu S M, Hou Y S, Wu Y C, Teng C M
机构信息
Pharmacological Institute, College of Medicine, National Taiwan University, Taipei.
出版信息
Br J Pharmacol. 1994 Aug;112(4):1174-80. doi: 10.1111/j.1476-5381.1994.tb13207.x.
Abstract
- The selectivity of (-)-discretamine for alpha 1-adrenoceptor subtypes was investigated by use of functional and binding studies in rat vas deferens, spleen and aorta, and in cultured DDT1MF-2 and A10 cells. 2. In prostatic portions of rat vas deferens, the competitive antagonists (-)-discretamine, 5-methylurapidil (5-MU) and prazosin inhibited contractions to noradrenaline (NA) with pA2 values of 6.21, 8.71 and 9.27, respectively. The irreversible antagonist, chloroethylclonidine (CEC, 100 microM) failed to affect contractions to NA while nifedipine (1 microM) blocked them almost completely. 3. In rat spleen, the competitive antagonists (-)-discretamine, 5-MU and prazosin inhibited contractions to phenylephrine with pA2 values of 6.44, 7.19 and 9.45, respectively. CEC (100 microM) significantly reduced the maximum contraction to phenylephrine while nifedipine (1 microM) did not affect it. 4. In rat aorta, the competitive antagonists (-)-discretamine, 5-MU and prazosin inhibited contractions to NA with pA2 values of 7.60, 8.00 and 9.40, respectively. CEC also antagonized the contractions to NA in a competitive manner with a pA2 value of 6.10. 5. The specific binding of [3H]-prazosin to DDT1MF-2 and A10 cells was concentration-dependent and saturated at 3-5 nM with KD values of 0.24 +/- 0.02 and 0.20 +/- 0.02 nM, respectively. (-)-Discretamine,5-MU, CEC and prazosin inhibited specific [3H]-prazosin binding to DDTIMF-2 and AlO cells in a concentration-dependent manner with ICso values of 390.8 +/- 20.6, 43.6 +/- 3.9, 200.0 +/- 30.0 and 0.8 +/- 0.1 nM, respectively in DDTIMF-2 cells, and 25.0 +/- 3.2, 8.6 +/- 1.4, 1000.0 +/- 30.8 and 0.52 +/- 0.03 nM, respectively in AlO cells.6. Pretreatment of Al0 cells with CEC (10 MicroM) for 30 min and then washed out thoroughly, reduced specific [3H]-prazosin binding by 30%. The CEC-insensitive [3H]-prazosin binding was inhibited by(-)-discretamine with an IC50 value of 7.0 +/- 0.3 nM.7. 5-MU (100 nM), CEC (1 MicroM) and prazosin (10 nM) markedly inhibited NA (3 MicroM)-induced [3H]-inositol monophosphate formation in DDTIMF-2 and A1O cells, while (-)-discretamine (100 nM)inhibited NA-induced [3H]-inositol monophosphate formation only in AlO cells.8. In conclusion, (-)-discretamine is a selective alpha lD-adrenoceptor antagonist in vascular smooth muscle.Its selectivity among various al-adrenoceptor subtypes is alpha 1A: alpha1B: alpha1D =0.04:0.07:1.0.
摘要
- 通过在大鼠输精管、脾脏和主动脉以及培养的DDT1MF - 2和A10细胞中进行功能和结合研究,考察了(-)-离散胺对α1 - 肾上腺素能受体亚型的选择性。2. 在大鼠输精管的前列腺部分,竞争性拮抗剂(-)-离散胺、5 - 甲基尿嘧啶(5 - MU)和哌唑嗪抑制去甲肾上腺素(NA)引起的收缩,其pA2值分别为6.21、8.71和9.27。不可逆拮抗剂氯乙可乐定(CEC,100μM)未能影响NA引起的收缩,而硝苯地平(1μM)几乎完全阻断了这些收缩。3. 在大鼠脾脏中,竞争性拮抗剂(-)-离散胺、5 - MU和哌唑嗪抑制去氧肾上腺素引起的收缩,其pA2值分别为6.44、7.19和9.45。CEC(100μM)显著降低了对去氧肾上腺素的最大收缩反应,而硝苯地平(1μM)对此无影响。4. 在大鼠主动脉中,竞争性拮抗剂(-)-离散胺、5 - MU和哌唑嗪抑制NA引起的收缩,其pA2值分别为7.60、8.00和9.40。CEC也以竞争性方式拮抗NA引起的收缩,pA2值为6.10。5. [3H] - 哌唑嗪与DDT1MF - 2和A10细胞的特异性结合呈浓度依赖性,在3 - 5 nM时达到饱和,KD值分别为0.24±0.02和0.20±0.02 nM。(-)-离散胺、5 - MU、CEC和哌唑嗪以浓度依赖性方式抑制[3H] - 哌唑嗪与DDTIMF - 2和AlO细胞的特异性结合,在DDTIMF - 2细胞中的IC50值分别为390.8±20.6、43.6±3.9、200.0±30.0和0.8±0.1 nM,在AlO细胞中的IC50值分别为25.0±3.2、8.6±1.4、1000.0±30.8和0.52±0.03 nM。6. 用CEC(10μM)预处理Al0细胞30分钟,然后彻底洗脱,使[3H] - 哌唑嗪的特异性结合减少30%。CEC不敏感的[3H] - 哌唑嗪结合被(-)-离散胺抑制,IC50值为7.0±0.3 nM。7. 5 - MU(100 nM)、CEC(1μM)和哌唑嗪(10 nM)显著抑制NA(3μM)诱导的DDTIMF - 2和A1O细胞中[3H] - 肌醇单磷酸的形成,而(-)-离散胺(100 nM)仅在AlO细胞中抑制NA诱导的[3H] - 肌醇单磷酸的形成。8. 总之,(-)-离散胺是血管平滑肌中的一种选择性α1D - 肾上腺素能受体拮抗剂。其在各种α1 - 肾上腺素能受体亚型中的选择性为α1A:α1B:α1D = 0.04:0.07:1.0。
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