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吲哚布芬的右旋对映体形式完全体现了其体外抗环氧化酶和抗血小板活性,以及在人体中导致出血时间延长的作用。

The d-enantiomer form of indobufen totally accounts for the anti-cyclooxygenase and antiplatelet activity ex vivo and for the increase in bleeding time by indobufen in man.

作者信息

De Caterina R, Sicari R, Yan A, Bernini W, Giannessi D, Lazzerini G, Efthymiopoulos C, Strolin-Benedetti M

机构信息

Laboratory for Thrombosis and Vascular Research, CNR Institute of Clinical Physiology, Pisa, Italy.

出版信息

Thromb Haemost. 1992 Feb 3;67(2):258-63.

PMID:1621247
Abstract

Indobufen is an antiplatelet drug able to inhibit thromboxane production and cyclooxygenase-dependent platelet aggregation by a reversible inhibition of cyclooxygenase. Indobufen exists in two enantiomeric forms, of which only d-indobufen is active in vitro in inhibiting cyclooxygenase. In order to verify that also inhibition of platelet function is totally accounted for by d-indobufen, ten patients with proven coronary artery disease (8 male, 2 female, age, mean +/- S.D., 58.7 +/- 7.5 years) were given, in random sequence, both 100 mg d-indobufen and 200 mg dl-indobufen as single administrations in a double-blind crossover design study with a washout period between treatments of 72 h. In all patients thromboxane (TX) B2 generation after spontaneous clotting (at 0, 1, 2, 4, 6, 8, 12, 24 h), drug plasma levels (at the same times), platelet aggregation in response to ADP, adrenaline, arachidonic acid, collagen, PAF, and bleeding time (at 0, 2, 12 h) were evaluated after each treatment. Both treatments determined peak inhibition of TXB2 production at 2 h from administration, with no statistical difference between the two treatments (97 +/- 3% for both treatments). At 12 h inhibition was 87 +/- 6% for d-indobufen and 88 +/- 6% for dl-indobufen (p = NS). Inhibition of TXB2 production correlated significantly with plasma levels of the drugs.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

吲哚布芬是一种抗血小板药物,能够通过可逆性抑制环氧化酶来抑制血栓素生成及环氧化酶依赖性血小板聚集。吲哚布芬存在两种对映体形式,其中仅d-吲哚布芬在体外具有抑制环氧化酶的活性。为了验证血小板功能的抑制也完全是由d-吲哚布芬引起的,在一项双盲交叉设计研究中,对10例经证实患有冠状动脉疾病的患者(8例男性,2例女性,年龄平均±标准差为58.7±7.5岁),以随机顺序分别单次给予100 mg d-吲哚布芬和200 mg消旋吲哚布芬,两次治疗之间的洗脱期为72小时。在每次治疗后,评估所有患者自发凝血后(在0、1、2、4、6、8、12、24小时)血栓素(TX)B2的生成、药物血浆水平(在相同时间)、对ADP、肾上腺素、花生四烯酸、胶原、PAF的血小板聚集反应以及出血时间(在0、2、12小时)。两种治疗均在给药后2小时使TXB2生成受到最大抑制,两种治疗之间无统计学差异(两种治疗均为97±3%)。在12小时时,d-吲哚布芬的抑制率为87±6%,消旋吲哚布芬为88±6%(p=无显著性差异)。TXB2生成的抑制与药物血浆水平显著相关。(摘要截取自250词)

相似文献

1
The d-enantiomer form of indobufen totally accounts for the anti-cyclooxygenase and antiplatelet activity ex vivo and for the increase in bleeding time by indobufen in man.吲哚布芬的右旋对映体形式完全体现了其体外抗环氧化酶和抗血小板活性,以及在人体中导致出血时间延长的作用。
Thromb Haemost. 1992 Feb 3;67(2):258-63.
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A prostacyclin-sparing effect of indobufen vs. aspirin.吲哚布芬与阿司匹林相比的前列环素保留效应。
Thromb Haemost. 1996 Mar;75(3):510-4.
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Effects of racemic, S- and R-indobufen on cyclooxygenase and lipoxygenase activities in human whole blood.消旋吲哚布芬、S-吲哚布芬和R-吲哚布芬对人全血中环氧化酶和脂氧合酶活性的影响。
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Inhibition of thromboxane biosynthesis and platelet function by indobufen in type II diabetes mellitus.
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In vitro and ex vivo effects of indobufen on human platelet aggregation, the release reaction and thromboxane B2 production.吲哚布芬对人血小板聚集、释放反应及血栓素B2生成的体外和离体效应。
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Pharmacodynamic effects of indobufen compared with aspirin in patients with coronary atherosclerosis.吲哚布芬与阿司匹林在冠心病患者中的药效学比较。
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Differential suppression of thromboxane biosynthesis by indobufen and aspirin in patients with unstable angina.吲哚布芬与阿司匹林对不稳定型心绞痛患者血栓素生物合成的差异抑制作用。
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The (+)-enantiomer is responsible for the antiplatelet and anti-inflammatory activity of (+/-)-indobufen.
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Comparison of aspirin and indobufen in healthy volunteers.阿司匹林与吲哚布芬在健康志愿者中的比较。
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The dispositional enantioselectivity of indobufen in man.
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Indobufen: an updated review of its use in the management of atherothrombosis.吲哚布芬:关于其在动脉粥样硬化血栓形成管理中应用的最新综述。
Drugs Aging. 2001;18(5):369-88. doi: 10.2165/00002512-200118050-00007.