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血小板聚集、ATP释放及细胞质Ca2+移动:氯克罗孟的作用

Platelet aggregation, ATP release and cytoplasmic Ca2+ movement: the effects of cloricromene.

作者信息

Davì G, Giammaresi C, Catalano I, Calà A, Prosdocimi M, Alvino S, Piva S, Notarbartolo A

机构信息

Div. of Hematology, University of Chieti, Italy.

出版信息

Thromb Res. 1994 Oct 15;76(2):121-31. doi: 10.1016/0049-3848(94)90183-x.

Abstract

A placebo-controlled, double-blind, randomized, cross-over study was performed in 24 healthy volunteers. 12 volunteers received Cloricromene (100mg gastroresistant capsules twice a day) for 7 days, the other volunteers received identical placebo capsules. Subsequently, after a 7-day wash-out period, at day 15, each subject received the other treatment. Blood samples were taken on days 1 and 15 (1st day of each treatment) as well as on days 7 and 21 (7th day of each treatment) before the morning drug administration and 2 and 4 hours later. Platelet aggregation and ATP secretion were studied in whole blood (WB) using ADP and collagen as stimulating agents. Ca2+ fluxes were studied in aequorin-loaded, washed platelets stimulated with ADP and collagen, while aggregation in platelet-rich plasma (PRP) was studied using PAF, ADP and adrenaline as agonists. Consistent inhibition of aggregation and release induced by both ADP and collagen was observed in WB after Cloricromene administration. Similarly, Ca2+ flux was also inhibited after drug administration. Platelet aggregation in PRP was inhibited only after 7 days of Cloricromene treatment with ADP and adrenaline as stimuli. We conclude that oral administration of Cloricromene leads to significant antiplatelet activity in healthy volunteers, in particular when platelets are studied in the presence of other blood elements.

摘要

对24名健康志愿者进行了一项安慰剂对照、双盲、随机交叉研究。12名志愿者接受氯克罗孟(100mg胃溶胶囊,每日两次)治疗7天,其他志愿者接受相同的安慰剂胶囊。随后,在7天的洗脱期后,在第15天,每个受试者接受另一种治疗。在第1天和第15天(每种治疗的第1天)以及第7天和第21天(每种治疗的第7天)早晨给药前以及给药后2小时和4小时采集血样。使用ADP和胶原蛋白作为刺激剂,在全血(WB)中研究血小板聚集和ATP分泌。在用ADP和胶原蛋白刺激的水母发光蛋白负载的洗涤血小板中研究Ca2+通量,而在富含血小板血浆(PRP)中使用PAF、ADP和肾上腺素作为激动剂研究聚集。氯克罗孟给药后,在WB中观察到ADP和胶原蛋白诱导的聚集和释放受到持续抑制。同样,给药后Ca2+通量也受到抑制。仅在氯克罗孟治疗7天后,以ADP和肾上腺素为刺激剂时,PRP中的血小板聚集才受到抑制。我们得出结论,口服氯克罗孟在健康志愿者中具有显著的抗血小板活性,特别是在存在其他血液成分的情况下研究血小板时。

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