AH6809,一种作用于人体血小板的前列腺素DP受体阻断药物。
AH6809, a prostaglandin DP-receptor blocking drug on human platelets.
作者信息
Keery R J, Lumley P
机构信息
Department of Cardiovascular Pharmacology, Glaxo Group Research Ltd, Ware, Herts.
出版信息
Br J Pharmacol. 1988 Jul;94(3):745-54. doi: 10.1111/j.1476-5381.1988.tb11584.x.
Abstract
- The effect of AH6809 (6-isopropoxy-9-oxoxanthene-2-carboxylic acid) has been studied upon the anti-aggregatory and aggregatory actions of various agents on human platelets in whole blood. 2. Prostaglandin D2 (PGD2), BW245C, 9 alpha, 11 beta-PGF2, PGI2 and 5'-N-ethylcarboxamide adenosine (NECA) all inhibited ADP-induced platelet aggregation in whole blood. The anti-aggregatory activity of PGD2, BW245C and 9 alpha, 11 beta-PGF2 but not PGI2 or NECA was antagonized by AH6809. NECA was antagonized by AH6809. 3. The antagonism of the anti-aggregatory activity of PGD2 by AH6809 was concentration-related and could be overcome by increasing the concentration of PGD2. Analysis of the data yielded an apparent pA2 for AH6809 of 5.35. 4. At approximately 10 fold higher concentrations than those required to antagonize the action of PGD2, AH6809 also antagonized the aggregatory effect of U-46619 in whole blood (pA2 = 4.45). However, concentrations of AH6809 up to 300 microM were without effect upon either ADP- or platelet activating factor (Paf)-induced aggregation (pA2 less than 3.5). 5. The potency of AH6809 against PGD2 and U-46619 was increased in a resuspended platelet preparation suggesting that the drug is extensively bound to plasma proteins. However, in resuspended platelets the specificity of AH6809 relative to that seen in whole blood was reduced since aggregation by ADP and Paf was also slightly antagonized. 6. In conclusion, AH6809 appears to be a weak but specific DP-receptor blocking drug on human platelets and should prove to be a useful drug tool for defining the involvement of endogenous PGD2 in platelet aggregation and classifying the mode of action of anti-aggregatory prostanoids.
摘要
- 研究了AH6809(6 - 异丙氧基 - 9 - 氧代呫吨 - 2 - 羧酸)对全血中多种药物作用于人体血小板的抗聚集和聚集作用的影响。2. 前列腺素D2(PGD2)、BW245C、9α,11β - PGF2、前列环素(PGI2)和5'-N - 乙基甲酰胺腺苷(NECA)均抑制全血中ADP诱导的血小板聚集。AH6809拮抗PGD2、BW245C和9α,11β - PGF2的抗聚集活性,但不拮抗PGI2或NECA。AH6809拮抗NECA。3. AH6809对PGD2抗聚集活性的拮抗作用与浓度相关,且可通过增加PGD2的浓度来克服。数据分析得出AH6809的表观pA2为5.35。4. 在比拮抗PGD2作用所需浓度高约10倍的浓度下,AH6809也拮抗全血中U - 46619的聚集作用(pA2 = 4.45)。然而,高达300微摩尔的AH6809浓度对ADP或血小板活化因子(Paf)诱导的聚集均无影响(pA2小于3.5)。5. 在重悬血小板制剂中,AH6809对PGD2和U - 46619的效力增加,表明该药物与血浆蛋白广泛结合。然而,在重悬血小板中,AH6809相对于全血中的特异性降低,因为ADP和Paf诱导的聚集也略有拮抗。6. 总之,AH6809似乎是一种作用较弱但对人血小板具有特异性的DP受体阻断药物,应证明是一种有用的药物工具,用于确定内源性PGD2在血小板聚集中的作用以及对抗聚集前列腺素类药物作用模式进行分类。
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