血小板环氧化酶-2依赖性血栓素A2生成缺乏生物学相关性。
Lack of biological relevance of platelet cyclooxygenase-2 dependent thromboxane A2 production.
作者信息
Riondino Silvia, Trifirò Elisabetta, Principessa Lorenzo, Mascioletti Silvia, Di Renzo Livia, Gaudio Carlo, Biasucci Luigi M, Crea Filippo, Pulcinelli Fabio M
机构信息
Department of Experimental Medicine, "Sapienza" University, Italy.
出版信息
Thromb Res. 2008;122(3):359-65. doi: 10.1016/j.thromres.2007.12.011. Epub 2008 Mar 4.
INTRODUCTION
There is emerging evidence of a considerable variability of the impact of aspirin on clinical outcome and laboratory findings. Persistent TxA2 production seems to be the most likely reason. Aim of this study was to determine whether the mechanism responsible for TxA2 persistent production is, at least partially, dependent upon aspirin-insensitive platelet COX-2 enzymatic pathway.
METHODS AND RESULTS
In 100 consecutive patients, under chronic aspirin anti-platelet treatment (100-160 mg/day) selected on the basis of detectable plasma salicylate levels, serum and Arachidonic Acid (AA)-induced platelet TxA2 production, immunoblot analysis of platelet COX-1/COX-2 expression and COX-2 activity were studied. Immunoblot revealed COX-2 expression in 46% patients, in an amount that was markedly lower than COX-1. In 10 COX-2 positive patients with TxA2 levels over the median, AA-induced TxA2 production performed in vitro in the presence of the COX-2 inhibitor CAY10404 and aspirin demonstrated that COX-2 dependent TxA2 production is less than 2%.
CONCLUSION
Our data demonstrate that the inter-individual variability of platelet sensitivity to aspirin is due to a reduced efficacy of aspirin on platelet COX-1 despite ascertained patient compliance. We suggest that serum TxA2 assay might be performed in future clinical studies to improve our knowledge on the residual TxA2 production in aspirin-treated patients.
引言
越来越多的证据表明,阿司匹林对临床结局和实验室检查结果的影响存在相当大的变异性。持续产生血栓素A2(TxA2)似乎是最可能的原因。本研究的目的是确定负责TxA2持续产生的机制是否至少部分依赖于对阿司匹林不敏感的血小板环氧化酶-2(COX-2)酶促途径。
方法与结果
在100例连续患者中,根据可检测的血浆水杨酸水平选择接受慢性阿司匹林抗血小板治疗(100 - 160毫克/天),研究血清和花生四烯酸(AA)诱导的血小板TxA2产生、血小板COX-1/COX-2表达的免疫印迹分析以及COX-2活性。免疫印迹显示46%的患者有COX-2表达,其数量明显低于COX-1。在10例TxA2水平高于中位数的COX-2阳性患者中,在存在COX-2抑制剂CAY10404和阿司匹林的情况下体外进行AA诱导的TxA2产生实验,结果表明COX-2依赖性TxA2产生小于2%。
结论
我们的数据表明,尽管患者依从性已确定,但血小板对阿司匹林敏感性的个体间变异性是由于阿司匹林对血小板COX-1的疗效降低所致。我们建议在未来的临床研究中进行血清TxA2检测,以增进我们对阿司匹林治疗患者中残余TxA2产生情况的了解。
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