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速释和缓释制剂中乙酰水杨酸和水杨酸的生物利用度,以及与双嘧达莫联合使用时的生物利用度。

Bioavailability of acetylsalicylic acid and salicylic acid from rapid-and slow-release formulations, and in combination with dipyridamol.

作者信息

Brantmark B, Wåhlin-Boll E, Melander A

出版信息

Eur J Clin Pharmacol. 1982;22(4):309-14. doi: 10.1007/BF00548398.

Abstract

Acetylsalicylic acid (ASA) is a strong, irreversible inhibitor of platelet aggregation, but loses this activity following first-pass deacetylation to salicylic acid (SA). In order to compare the bioavailability of unchanged ASA from rapid- and slow-release formulations, the single-dose concentration profiles of ASA and SA were studied in healthy volunteers following intake of two different rapid-release (conventional and effervescent tablets) and three different slow-release (microencapsulated ASA in tablets and in capsules, and enteric-coated tablets) formulations of ASA, and of one slow-release formulation of sodium salicylate. Since anti-platelet therapy with ASA is often combined with dipyridamol, the influence of this drug was also examined. The concentrations of ASA and SA were measured by high-pressure liquid chromatography. While the bioavailability of SA from the 5 ASA formulations was essentially equal and similar to that of the salicylate formulation, the bioavailability and peak concentrations of ASA appeared to be the much greater after rapid-release than after slow-release formulations. Indeed, ASA was only rarely detected in systemic blood following intake of slow-release ASA. Co-administered dipyridamol did not significantly influence the kinetics of ASA or SA. It appears that rapid-release formulations of ASA should be prefered in anti-platelet therapy, either alone or in combination with dipyridamol.

摘要

乙酰水杨酸(ASA)是血小板聚集的一种强效、不可逆抑制剂,但在首过脱乙酰化为水杨酸(SA)后会失去这种活性。为了比较速释和缓释制剂中未改变的ASA的生物利用度,在健康志愿者摄入两种不同的速释(普通片剂和泡腾片)和三种不同的缓释(片剂和胶囊中的微囊化ASA以及肠溶衣片)ASA制剂以及一种水杨酸钠缓释制剂后,研究了ASA和SA的单剂量浓度曲线。由于ASA抗血小板治疗常与双嘧达莫联合使用,因此也研究了该药物的影响。通过高压液相色谱法测量ASA和SA的浓度。虽然5种ASA制剂中SA的生物利用度基本相同且与水杨酸盐制剂相似,但速释制剂后ASA的生物利用度和峰值浓度似乎比缓释制剂后高得多。实际上,摄入缓释ASA后,全身血液中很少检测到ASA。联合使用双嘧达莫对ASA或SA的动力学没有显著影响。在抗血小板治疗中,无论是单独使用还是与双嘧达莫联合使用,ASA的速释制剂似乎更受青睐。

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