Effects of cutaneous aspirin on the human stomach and duodenum.

B Cryer, D Kliewer, H Sie, L McAllister, M Feldman
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引用次数: 12

Abstract

Oral aspirin blocks cyclooxygenase in platelets, lowering serum thromboxane concentrations. Oral aspirin also blocks cyclooxygenase in the gastrointestinal mucosa, lowering prostaglandin production and increasing the risk of gastrointestinal ulceration and bleeding. Aspirin placed on the skin also inhibits cyclooxygenase in platelets, but aspirin absorption through skin is slow, which may minimize the gastrointestinal effects. Our objectives in this study were 1) to compare the pharmacokinetic and pharmacodynamic effects of cutaneous and oral aspirin in healthy volunteers and 2) to compare the effects of cutaneous aspirin on gastroduodenal mucosal prostaglandin E2 and F2 alpha content and on mucosal damage, using endoscopy. The bioavailability of cutaneous aspirin was 4%-8% that of oral aspirin. Cutaneous aspirin (750 mg/day for 10 days) significantly lowered serum thromboxane (by 85%) and gastric and duodenal prostaglandins (by 49%-71%); placebo had no effect. Moreover, cutaneous aspirin, but not placebo, resulted in significant gastric mucosal injury. These findings demonstrate that even tiny amounts of aspirin in the blood (2 microM) have inhibitory effects on prostaglandin production in the human stomach and duodenum that result in gastric mucosal damage, even without direct exposure of the stomach to aspirin.

皮服阿司匹林对人胃和十二指肠的影响。
口服阿司匹林阻断血小板环加氧酶,降低血清血栓素浓度。口服阿司匹林还能阻断胃肠道粘膜的环氧化酶,降低前列腺素的产生,增加胃肠道溃疡和出血的风险。将阿司匹林放在皮肤上也会抑制血小板中的环氧化酶,但阿司匹林通过皮肤的吸收速度较慢,这可能会将胃肠道影响降到最低。我们在这项研究中的目的是:1)比较健康志愿者皮肤和口服阿司匹林的药代动力学和药效学效应;2)比较皮肤阿司匹林对胃十二指肠黏膜前列腺素E2和F2 α含量以及粘膜损伤的影响。皮用阿司匹林的生物利用度为口服阿司匹林的4% ~ 8%。口服阿司匹林(750 mg/天,连用10天)可显著降低血清血栓素(85%)和胃、十二指肠前列腺素(49%-71%);安慰剂没有效果。此外,皮肤阿司匹林,而不是安慰剂,导致显著的胃粘膜损伤。这些发现表明,即使血液中微量的阿司匹林(2微克)也会抑制人胃和十二指肠中前列腺素的产生,从而导致胃粘膜损伤,即使胃没有直接接触阿司匹林。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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