匹维溴铵(一种季铵化合物)与大鼠回肠平滑肌中1,4-二氢吡啶结合位点的相互作用。
Interaction of pinaverium (a quaternary ammonium compound) with 1,4-dihydropyridine binding sites in rat ileum smooth muscle.
作者信息
Feron O, Wibo M, Christen M O, Godfraind T
机构信息
Laboratoire de Pharmacologie, Université Catholique de Louvain, Bruxelles, Belgium.
出版信息
Br J Pharmacol. 1992 Feb;105(2):480-4. doi: 10.1111/j.1476-5381.1992.tb14279.x.
Abstract
- The interaction of pinaverium bromide, a quaternary ammonium compound, with binding sites for (L-type) calcium channel blockers was investigated in rat ileum smooth muscle. 2. Pinaverium inhibited [3H]-(+)-PN200-110 ([3H]-(+)-isradipine) specific binding to tissue homogenates incompletely (Ki 0.38 microM; maximal inhibition 80%). In contrast, binding to single cell preparations (obtained by collagenase treatment) and to saponin-treated homogenates was completely inhibited. These data are compatible with the view that, in untreated homogenates, 20% of [3H]-(+)-isradipine binding sites are not accessible to pinaverium because it is associated with sealed inside-out vesicles. 3. Pinaverium bromide increased the apparent KD of [3H]-(+)-isradipine binding to saponin-treated homogenates but did not significantly affect the Bmax value. Moreover, the dissociation rate constant of [3H]-(+)-isradipine binding was not changed by pinaverium. These data suggest that pinaverium interacts with the dihydropyridine binding site in a competitive manner. However, in contrast to uncharged dihydropyridine calcium antagonists, pinaverium inhibited, rather than stimulated, [3H]-diltiazem binding to rat brain membranes (at 30-37 degrees C). 4. Although Bmax values of [3H]-(+)-isradipine were similar in homogenates prepared from tissue and cells (collagenase-treated), the KD value was significantly higher in cell homogenates (166 vs 95 pM). Similarly, the Ki value of pinaverium was higher in cell preparations than in tissue homogenates (0.77 vs 0.38 microM). Thus, collagenase can significantly modify the dihydropyridine recognition site.5. The competitive interaction of pinaverium, a permanently charged drug, with [3H]-(+)-isradipine bound to intact cells and its absence of interaction with [3H]-(+)-isradipine bound to sealed inside-out vesicles imply that the dihydropyridine receptor lies near the external surface of the plasma membrane.
摘要
- 在大鼠回肠平滑肌中研究了季铵化合物匹维溴铵与(L型)钙通道阻滞剂结合位点的相互作用。2. 匹维溴铵对组织匀浆中[3H]-(+)-PN200-110([3H]-(+)-伊拉地平)的特异性结合抑制不完全(Ki为0.38微摩尔;最大抑制率80%)。相比之下,对单细胞制剂(通过胶原酶处理获得)和皂素处理的匀浆的结合则被完全抑制。这些数据与以下观点相符:在未处理的匀浆中,20%的[3H]-(+)-伊拉地平结合位点对匹维溴铵不可达,因为它与封闭的内翻囊泡相关。3. 匹维溴铵增加了[3H]-(+)-伊拉地平与皂素处理的匀浆结合的表观解离常数(KD),但对最大结合容量(Bmax)值无显著影响。此外,匹维溴铵未改变[3H]-(+)-伊拉地平结合的解离速率常数。这些数据表明匹维溴铵以竞争性方式与二氢吡啶结合位点相互作用。然而,与不带电荷的二氢吡啶类钙拮抗剂不同,匹维溴铵在30 - 37℃时抑制而非刺激[3H]-地尔硫䓬与大鼠脑膜的结合。4. 尽管从组织和细胞(胶原酶处理)制备的匀浆中[3H]-(+)-伊拉地平的Bmax值相似,但细胞匀浆中的KD值显著更高(166对95皮摩尔)。同样,匹维溴铵在细胞制剂中的Ki值高于组织匀浆中的Ki值(0.77对0.38微摩尔)。因此,胶原酶可显著改变二氢吡啶识别位点。5. 永久带电药物匹维溴铵与结合在完整细胞上的[3H]-(+)-伊拉地平的竞争性相互作用以及其与结合在封闭的内翻囊泡上的[3H]-(+)-伊拉地平缺乏相互作用,意味着二氢吡啶受体位于质膜外表面附近。
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本文引用的文献
1
Protein measurement with the Folin phenol reagent.使用福林酚试剂进行蛋白质测定。
J Biol Chem. 1951 Nov;193(1):265-75.
2
Effect of pinaverium bromide on electrical and mechanical activity of smooth muscle cells.溴化匹那维铵对平滑肌细胞电活动和机械活动的影响。
Naunyn Schmiedebergs Arch Pharmacol. 1983 Jun;323(1):72-7. doi: 10.1007/BF00498831.
3
A unitary mechanism of calcium antagonist drug action.钙拮抗剂药物作用的单一机制。
Proc Natl Acad Sci U S A. 1983 Feb;80(3):860-4. doi: 10.1073/pnas.80.3.860.
4
Heterogeneity of ouabain specific binding sites and (Na+ + K+)-ATPase inhibition in microsomes from rat heart.哇巴因特异性结合位点的异质性以及大鼠心脏微粒体中(钠 + 钾)-ATP酶的抑制作用
Biochem Pharmacol. 1984 Jan 1;33(1):47-53. doi: 10.1016/0006-2952(84)90369-1.
5
Ligand: a versatile computerized approach for characterization of ligand-binding systems.配体:一种用于表征配体结合系统的通用计算机化方法。
Anal Biochem. 1980 Sep 1;107(1):220-39. doi: 10.1016/0003-2697(80)90515-1.
6
Effects of pinaverium bromide and verapamil on the motility of the rat isolated colon.溴丙胺太林和维拉帕米对大鼠离体结肠运动的影响。
Br J Pharmacol. 1985 Sep;86(1):89-94. doi: 10.1111/j.1476-5381.1985.tb09438.x.
7
Interactions of muscarinic drugs with their receptors in single cells of guinea-pig taenia caecum.毒蕈碱类药物与豚鼠盲肠带单个细胞中其受体的相互作用。
J Pharm Pharmacol. 1986 Jun;38(6):476-8. doi: 10.1111/j.2042-7158.1986.tb04615.x.
8
Measurement of whole-cell calcium current in voltage-clamped vascular muscle cells.电压钳制血管平滑肌细胞全细胞钙电流的测量。
Mol Cell Biochem. 1988 Mar-Apr;80(1-2):87-93. doi: 10.1007/BF00231007.
9
Pharmacologic relevance of dihydropyridine binding sites in membranes from rat aorta: kinetic and equilibrium studies.大鼠主动脉膜中二氢吡啶结合位点的药理学相关性:动力学和平衡研究。
Circ Res. 1988 Jan;62(1):91-6. doi: 10.1161/01.res.62.1.91.
10
Calcium antagonism and calcium entry blockade.钙拮抗作用与钙内流阻断
Pharmacol Rev. 1986 Dec;38(4):321-416.
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