低剂量阿司匹林对健康受试者血小板血栓素生成的选择性累积抑制作用。
Selective cumulative inhibition of platelet thromboxane production by low-dose aspirin in healthy subjects.
作者信息
Patrignani P, Filabozzi P, Patrono C
出版信息
J Clin Invest. 1982 Jun;69(6):1366-72. doi: 10.1172/jci110576.
Acetylation of platelet cyclooxygenase by oral aspirin is dose dependent and cumulative with repeated administration. However, no single dose of aspirin has been found to be completely selective of platelet thromboxane (TX) synthesis inhibition in man. We determined the dose dependence, cumulative nature and selectivity of aspirin effects on platelet TXB(2) and renal prostaglandin (PG) and prostacyclin (PGI(2)) production. We measured, by radioimmunoassay, serum TXB(2) levels after whole blood clotting and urinary excretion of PGE(2), PGF(2alpha), and 6-keto-PGF(1alpha), before and after single or repeated oral aspirin doses given to 46 healthy subjects. Single doses of 6-100 mg aspirin resulted in a linear (r = 0.92, P < 0.01) inhibition of platelet TXB(2) production, ranging from 12 to 95% after 24 h. A daily dose of 0.45 mg/kg given for 7 d produced a cumulative and virtually complete inhibition of platelet TXB(2) production, without significantly reducing the urinary excretion of PGE(2), PGF(2alpha), and 6-keto-PGF(1alpha) in both healthy men and women. The platelet inhibitory effect of this regimen was maintained unaltered throughout 1 mo of therapy, with no evidence of cumulative inhibition of renal PG-synthesis. Moreover, furosemide-induced renal PGI(2) synthesis and renin release were unaffected by chronic low-dose aspirin. Following cessation of aspirin therapy, platelet TXB(2) production returned toward control values at a similar rate as after a single higher dose. WE CONCLUDE THAT IN HEALTHY SUBJECTS: (a) aspirin causes a dose-dependent inhibition of platelet TXA(2) production, with no obvious sex-related difference; (b) the inhibitory effect of daily low-dose aspirin is cumulative on platelet TXA(2) but not on renal PG-synthesis; (c) during chronic low-dose aspirin therapy, renal PGI(2)-producing cells are readily activable by furosemide at a time of virtually complete suppression of platelet cyclooxygenase activity.
口服阿司匹林对血小板环氧化酶的乙酰化作用呈剂量依赖性,且反复给药具有累积性。然而,尚未发现单剂量阿司匹林能完全选择性地抑制人体血小板血栓素(TX)的合成。我们测定了阿司匹林对血小板TXB₂以及肾脏前列腺素(PG)和前列环素(PGI₂)生成的剂量依赖性、累积性质和选择性。我们通过放射免疫分析法,测量了46名健康受试者单次或反复口服阿司匹林前后全血凝固后的血清TXB₂水平以及尿中PGE₂、PGF₂α和6 - 酮 - PGF₁α的排泄量。单剂量6 - 100 mg阿司匹林导致血小板TXB₂生成呈线性抑制(r = 0.92,P < 0.01),24小时后抑制率在12%至95%之间。每日剂量0.45 mg/kg连续给药7天,可产生累积且几乎完全抑制血小板TXB₂生成的效果,同时在健康男性和女性中均未显著降低尿中PGE₂、PGF₂α和6 - 酮 - PGF₁α的排泄量。该方案对血小板的抑制作用在整个1个月的治疗过程中保持不变,没有证据表明对肾脏PG合成有累积抑制作用。此外,呋塞米诱导的肾脏PGI₂合成和肾素释放不受慢性低剂量阿司匹林的影响。停止阿司匹林治疗后,血小板TXB₂生成恢复至对照值的速率与单次较高剂量给药后相似。我们得出结论,在健康受试者中:(a)阿司匹林对血小板TXA₂生成具有剂量依赖性抑制作用,无明显性别差异;(b)每日低剂量阿司匹林对血小板TXA₂的抑制作用具有累积性,但对肾脏PG合成无累积抑制作用;(c)在慢性低剂量阿司匹林治疗期间,在血小板环氧化酶活性几乎完全被抑制时,肾脏产生PGI₂的细胞很容易被呋塞米激活。
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