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Pharmacological analysis of ecto-ATPase inhibition: evidence for combined enzyme inhibition and receptor antagonism in P2X-purinoceptor ligands.胞外ATP酶抑制的药理学分析:P2X嘌呤受体配体中酶抑制与受体拮抗联合作用的证据
Br J Pharmacol. 1994 Dec;113(4):1432-8. doi: 10.1111/j.1476-5381.1994.tb17157.x.
2
Pharmacological and biochemical analysis of FPL 67156, a novel, selective inhibitor of ecto-ATPase.新型胞外ATP酶选择性抑制剂FPL 67156的药理与生化分析
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3
FPL 66096: a novel, highly potent and selective antagonist at human platelet P2T-purinoceptors.FPL 66096:一种新型的、高效且具有选择性的人血小板P2T嘌呤受体拮抗剂。
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Br J Pharmacol. 1990 Mar;99(3):617-21. doi: 10.1111/j.1476-5381.1990.tb12979.x.
10
Pharmacological profile of the novel P2T-purinoceptor antagonist, FPL 67085 in vitro and in the anaesthetized rat in vivo.新型P2T嘌呤受体拮抗剂FPL 67085的体外和麻醉大鼠体内药理学特性
Br J Pharmacol. 1995 Jul;115(6):1110-6. doi: 10.1111/j.1476-5381.1995.tb15925.x.

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J Physiol Sci. 2012 Jan;62(1):53-8. doi: 10.1007/s12576-011-0176-5. Epub 2011 Sep 20.
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Structure-activity relationships of anthraquinone derivatives derived from bromaminic acid as inhibitors of ectonucleoside triphosphate diphosphohydrolases (E-NTPDases).溴氨乙酸衍生蒽醌衍生物作为核苷酸三磷酸二磷酸水解酶(E-NTPDases)抑制剂的构效关系。
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6
Ecto-nucleotide pyrophosphatase modulates the purinoceptor-mediated signal transduction and is inhibited by purinoceptor antagonists.胞外核苷酸焦磷酸酶调节嘌呤受体介导的信号转导,并受到嘌呤受体拮抗剂的抑制。
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7
New insights on P2X purinoceptors.P2X嘌呤受体的新见解。
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P2x-purinoceptors of myenteric neurones from the guinea-pig ileum and their unusual pharmacological properties.豚鼠回肠肌间神经元的P2x嘌呤受体及其独特的药理学特性。
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Evaluation of P2-purinoceptor antagonists at two relaxation-mediating P2-purinoceptors in guinea-pig taenia coli.豚鼠结肠带中两种介导舒张的P2嘌呤受体上P2嘌呤受体拮抗剂的评估
Naunyn Schmiedebergs Arch Pharmacol. 1996 Mar;353(4):445-51. doi: 10.1007/BF00261442.

本文引用的文献

1
Quantitative analysis of the agonist and antagonist actions of some ATP analogues at P2X-purinoceptors in the rabbit ear artery.一些ATP类似物对兔耳动脉P2X嘌呤受体的激动剂和拮抗剂作用的定量分析。
Br J Pharmacol. 1993 Feb;108(2):490-6. doi: 10.1111/j.1476-5381.1993.tb12830.x.
2
Characterization of ecto-ATPase on human blood cells. A physiological role in platelet aggregation?人血细胞上ecto-ATP酶的特性。在血小板聚集中的生理作用?
Biochem Pharmacol. 1993 Dec 3;46(11):1959-66. doi: 10.1016/0006-2952(93)90637-c.
3
Distribution and characterisation of [3H]alpha,beta-methylene ATP binding sites in the rat.大鼠体内[3H]α,β-亚甲基ATP结合位点的分布与特性研究
Naunyn Schmiedebergs Arch Pharmacol. 1993 Dec;348(6):608-17. doi: 10.1007/BF00167237.
4
Errors in the measurement of agonist potency-ratios produced by uptake processes: a general model applied to beta-adrenoceptor agonists.摄取过程产生的激动剂效价比测量中的误差:应用于β-肾上腺素能受体激动剂的通用模型
Br J Pharmacol. 1980;71(2):407-17. doi: 10.1111/j.1476-5381.1980.tb10953.x.
5
ATP analogues and the guinea-pig taenia coli: a comparison of the structure-activity relationships of ectonucleotidases with those of the P2-purinoceptor.ATP类似物与豚鼠结肠带:外核苷酸酶与P2嘌呤受体结构-活性关系的比较
Eur J Pharmacol. 1986 Oct 7;129(3):217-24. doi: 10.1016/0014-2999(86)90431-0.
6
Is there a basis for distinguishing two types of P2-purinoceptor?是否有依据区分两种类型的P2嘌呤受体?
Gen Pharmacol. 1985;16(5):433-40. doi: 10.1016/0306-3623(85)90001-1.
7
Self-cancellation of drug properties as a mode of organ selectivity: the antimuscarinic effects of ambenonium.药物特性的自我抵消作为一种器官选择性模式:安贝氯铵的抗毒蕈碱作用
J Pharmacol Exp Ther. 1985 Mar;232(3):732-40.
8
The structure-activity relationships of ectonucleotidases and of excitatory P2-purinoceptors: evidence that dephosphorylation of ATP analogues reduces pharmacological potency.外核苷酸酶与兴奋性P2嘌呤受体的构效关系:ATP类似物去磷酸化降低药理活性的证据。
Eur J Pharmacol. 1987 Sep 2;141(1):123-30. doi: 10.1016/0014-2999(87)90418-3.
9
The effects of some possible inhibitors of ectonucleotidases on the breakdown and pharmacological effects of ATP in the guinea-pig urinary bladder.某些可能的外核苷酸酶抑制剂对豚鼠膀胱中ATP分解及药理作用的影响
Gen Pharmacol. 1989;20(4):413-6. doi: 10.1016/0306-3623(89)90188-2.
10
Analysis of competitive antagonism when this property occurs as part of a pharmacological resultant.当这种特性作为药理学结果的一部分出现时,对竞争性拮抗作用的分析。
Br J Pharmacol. 1986 Nov;89(3):547-55. doi: 10.1111/j.1476-5381.1986.tb11155.x.

胞外ATP酶抑制的药理学分析:P2X嘌呤受体配体中酶抑制与受体拮抗联合作用的证据

Pharmacological analysis of ecto-ATPase inhibition: evidence for combined enzyme inhibition and receptor antagonism in P2X-purinoceptor ligands.

作者信息

Crack B E, Beukers M W, McKechnie K C, Ijzerman A P, Leff P

机构信息

Department of Pharmacology, Fisons R&D Labs, Loughborough, Leicestershire.

出版信息

Br J Pharmacol. 1994 Dec;113(4):1432-8. doi: 10.1111/j.1476-5381.1994.tb17157.x.

DOI:10.1111/j.1476-5381.1994.tb17157.x
PMID:7889301
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1510486/
Abstract
  1. Previous studies have shown that suramin and FPL 66301 are competitive antagonists at the P2X-purinoceptor in the rabbit ear artery. Those studies employed alpha,beta-methylene ATP, a poorly hydrolysable ATP analogue, as the agonist. In this study these compounds have been tested using ATP as the agonist. 2. Suramin, in the concentration range 30-1000 microM, potentiated the contractile effects of ATP, producing a 3-fold leftward shift of the ATP E/[A] curves. FPL 66301, in the concentration range 100-1000 microM, produced a significant but small (approximately 3-fold) rightward shift of the ATP curves. These results are in marked contrast with previous studies using alpha,beta-methylene ATP in which 30-fold rightward shifts were achieved using the same concentration ranges of suramin and FPL 66301. 3. Suramin and FPL 66301 were tested as ecto-ATPase inhibitors in a human blood cell assay. Suramin inhibited the enzyme with a pIC50 of 4.3, FPL 66301 with a pIC50 of 3.3. 4. The pharmacological data were analysed using a theoretical model describing the action of a compound with dual enzyme inhibitory and receptor antagonistic properties on the effects of an agonist susceptible to enzymatic degradation. The model was found to fit the data well using the known pKB estimates for suramin and FPL 66301 and similar relative (but not absolute) pK1 estimates to those obtained for the compounds in the enzyme assay. 5. From this analysis it was concluded that the limited shifts of ATP E/[A] curves produced by suramin and FPL 66301 were the result of 'self-cancellation' of the potentiating (enzyme inhibitory) and rightward-shifting (receptor antagonistic) properties.6. The analysis also indicated that the presence of ecto-ATPase activity in the rabbit ear artery preparation has a marked effect on the apparent potency of ATP. The experimental p[A50] was 3.4,whereas the 'true' value, that is the value which would be obtained in the absence of ecto-ATPase activity, was 6.0, some 400-fold higher.7 Two conclusions are drawn from this study. Firstly, caution must be exercised in the use of suramin and FPL 66301 as tools for receptor classification. Absence of overt antagonism by these compounds when metabolically unstable agonists are used could lead to erroneous claims for receptor subtypes.Secondly, the agonist potency order currently used to designate P2X- purinoceptors may require modification.
摘要
  1. 先前的研究表明,苏拉明和FPL 66301是兔耳动脉中P2X嘌呤受体的竞争性拮抗剂。那些研究使用α,β-亚甲基ATP(一种水解性很差的ATP类似物)作为激动剂。在本研究中,使用ATP作为激动剂对这些化合物进行了测试。2. 苏拉明在30 - 1000微摩尔浓度范围内增强了ATP的收缩作用,使ATP的E/[A]曲线向左移动了3倍。FPL 66301在100 - 1000微摩尔浓度范围内使ATP曲线产生了显著但较小(约3倍)的向右移动。这些结果与先前使用α,β-亚甲基ATP的研究形成了鲜明对比,在先前的研究中,使用相同浓度范围的苏拉明和FPL 66301可使曲线向右移动30倍。3. 在人血细胞试验中测试了苏拉明和FPL 66301作为胞外ATP酶抑制剂的作用。苏拉明抑制该酶的pIC50为4.3,FPL 66301的pIC50为3.3。4. 使用一个理论模型分析药理学数据,该模型描述了一种具有双重酶抑制和受体拮抗特性的化合物对易受酶降解的激动剂作用的影响。发现使用苏拉明和FPL 66301已知的pKB估计值以及与酶试验中获得的化合物类似的相对(但非绝对)pK1估计值时,该模型能很好地拟合数据。5. 从该分析得出的结论是,苏拉明和FPL 66301引起的ATP E/[A]曲线的有限移动是增强作用(酶抑制)和向右移动作用(受体拮抗)“自我抵消”的结果。6. 分析还表明,兔耳动脉制剂中胞外ATP酶活性的存在对ATP的表观效力有显著影响。实验测得的p[A50]为3.4,而“真实”值,即在不存在胞外ATP酶活性时会得到的值为6.0,约高400倍。7. 从本研究得出两个结论。首先,在将苏拉明和FPL 66301用作受体分类工具时必须谨慎。当使用代谢不稳定的激动剂时,这些化合物缺乏明显的拮抗作用可能导致对受体亚型的错误认定。其次,目前用于指定P2X嘌呤受体的激动剂效力顺序可能需要修改。