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维拉帕米对 ADP、胶原或凝血酶诱导的血小板激活的体外作用。

In vitro Effect of Verapamil on Platelet Activation Induced by ADP, Collagen or Thrombin.

机构信息

Department of Internal Medicine, Section of Medical Pathology, University of Pavia, IRCCS Policlinico S. Matteo, Pavia, Italy.

出版信息

Platelets. 1995;6(4):195-9. doi: 10.3109/09537109509078454.

Abstract

We studied the effects in Vitro of the calcium channel blocker verapamil (0.1, 0.2 or 0.3 mM) on platelet aggregation, on cytoplasmic Ca(+ +) levels and on TxB(2) production after activation of platelets with adenosine diphosphate (ADP) (100 µM), collagen (20 µg/ml) or thrombin (1 U/ml). A Platelet Ionized Calcium Aggregometer was used and washed, aequorin loaded platelets were employed. The drug was able to inhibit similarly and always significantly aggregation, Ca(+ +) fluxes and TxB(2) production when collagen was the agonist. Furthermore, inhibition of aggregation and TxB(2) production was significant at all the concentrations tested when platelets were activated by ADP or thrombin, but in this case inhibition of Ca (+ +) fluxes was observed only with the higher concentrations of the drug (0.2 or 0.3 mM). Hence, with these two last agonists inhibition of Ca(+ +) movements was less pronounced than inhibition of aggregation or TxB(2) production. These data suggest that platelet activation by collagen depends directly and almost exclusively on Ca(+ +) fluxes through biological membranes, while activation by ADP or thrombin is less strictly related to Ca(+ +) movements. Indeed, with these last two agonists verapamil may inhibit platelet activation also by calcium-independent mechanism(s).

摘要

我们研究了钙通道阻滞剂维拉帕米(0.1、0.2 或 0.3 mM)在体外对血小板聚集、细胞内 Ca(+ +)水平和血小板激活后 TxB(2)产生的影响,血小板激活剂为二磷酸腺苷(ADP)(100 μM)、胶原蛋白(20 μg/ml)或凝血酶(1 U/ml)。使用血小板离子钙聚集仪并进行清洗,使用载有荧光素的血小板。当胶原蛋白为激动剂时,该药物能够类似地始终显著抑制聚集、Ca(+ +)通量和 TxB(2)的产生。此外,当血小板被 ADP 或凝血酶激活时,在所有测试浓度下,聚集和 TxB(2)的产生抑制均显著,但在这种情况下仅观察到较高浓度的药物(0.2 或 0.3 mM)抑制 Ca (+ +)通量。因此,对于后两种激动剂,Ca(+ +)运动的抑制不如聚集或 TxB(2)的产生明显。这些数据表明,胶原蛋白激活血小板直接且几乎完全依赖于生物膜中 Ca(+ +)的流动,而 ADP 或凝血酶的激活与 Ca(+ +)的运动关系不那么密切。事实上,对于后两种激动剂,维拉帕米可能还通过钙非依赖性机制抑制血小板激活。

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