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双嘧达莫样化合物(R-E 244)对人血小板聚集和环磷酸腺苷积累的影响。

Effect of dipyridamole-like compound (R-E 244) on aggregation and cyclic AMP accumulation in human platelets.

作者信息

Söderbäck U, Sollevi A

机构信息

Department of Pharmacology, Karolinska Institutet, Stockholm, Sweden.

出版信息

Thromb Res. 1991 Nov 1;64(3):355-62. doi: 10.1016/0049-3848(91)90006-i.

Abstract

The aim of this in vitro study was to evaluate the effect of a clinical concentration (2 microM) of dipyridamole alone or in combination with adenosine, 5'-N-ethyl-carboxamido-adenosine (NECA), or prostaglandin E2 on ADP-induced whole blood aggregability. Cyclic AMP accumulation in platelet-rich plasma was also evaluated. For comparison, R-E 244 (a dipyridamole analogue with low phosphodiesterase inhibition) was examined. In whole blood, dipyridamole (2 microM), but not R-E 244 (2 microM), had a small inhibitory effect (16% +/- 5%, p less than 0.01) on aggregation. Adenosine (1 or 5 microM) had an inhibitory effect that was enhanced by the combination with dipyridamole or R-E 244. Adenosine + dipyridamole produced an inhibition almost equal to that of adenosine + R-E 244. Dipyridamole and R-E 244 had no influence on the antiaggregatory effect of NECA and prostaglandin E2. In platelet-rich plasma, dipyridamole and R-E 244 did not enhance cyclic AMP, nor did they reinforce the cyclic AMP production during treatment with adenosine, NECA, and prostaglandin E2. Our results suggest that inhibition of the uptake of adenosine into red blood cells may play a more important role than the inhibition of phosphodiesterase as the pharmacological mechanism for the antiaggregatory effect of dipyridamole in clinical treatment.

摘要

本体外研究的目的是评估临床浓度(2微摩尔)的双嘧达莫单独使用或与腺苷、5'-N-乙基-羧酰胺腺苷(NECA)或前列腺素E2联合使用对ADP诱导的全血聚集性的影响。同时也评估了富含血小板血浆中环状AMP的积累情况。为作比较,对R-E 244(一种具有低磷酸二酯酶抑制作用的双嘧达莫类似物)进行了检测。在全血中,双嘧达莫(2微摩尔)对聚集有轻微抑制作用(16%±5%,p<0.01),而R-E 244(2微摩尔)则无此作用。腺苷(1或5微摩尔)有抑制作用,与双嘧达莫或R-E 244联合使用时其抑制作用增强。腺苷+双嘧达莫产生的抑制作用几乎与腺苷+R-E 244相同。双嘧达莫和R-E 244对NECA和前列腺素E2的抗聚集作用没有影响。在富含血小板血浆中,双嘧达莫和R-E 244既不增强环状AMP,在用腺苷、NECA和前列腺素E2治疗期间也不加强环状AMP的产生。我们的结果表明,在临床治疗中,抑制腺苷进入红细胞的摄取可能比抑制磷酸二酯酶作为双嘧达莫抗聚集作用的药理机制发挥更重要的作用。

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