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普萘洛尔对血小板功能的影响。

Effect of propranolol on platelet function.

作者信息

Weksler B B, Gillick M, Pink J

出版信息

Blood. 1977 Feb;49(2):185-96.

PMID:318874
Abstract

Excessive reactivity of blood platelets may contribute to atherosclerotic vascular disease. Hence drugs which alter platelet function may be protective. Prompted by findings that propranolol therapy normalized hyperactive platelet aggregation in patients with coronary artery disease, we studied propranolol in vitro to assess its action on platelets. At concentrations similar to those achieved in vivo (0.1-1 muM), propranolol raised the thresholds for aggregation of some normal paltelets by adenosine diphosphate (ADP). At higher concentrations (10-50 muM), propranolol abolished the second wave of platelet aggregation induced by ADP and epinephrine, and inhibited aggregation induced by collagen, thrombin, and the ionophore A23187. Propanolol blocked the release of 14C-serotonin from platelets, inhibited platelet adhesion to collagen, and interfered with clot retraction. Propranolol blocked ionophore-induced uptake of 45Ca by platelets. Inhibition appeared unrelated to beta-adrenergic blockage, as d(+) propranolol (which lacks beta-blocking activity) was equipotent with 1(-) propranolol. Moreover, practolol, a beta-blockading drug which is nonlipophilic, did not inhibit platelet function. These studies suggested that propranolol, like local anesthetics, decreased platelet responsiveness by a direct action on the platelet membrane, possibly by interfering with calcium availability. Modulation of platelet function by propranolol may occur at concentrations achieved at usual clinical doses of the drug.

摘要

血小板反应过度可能会导致动脉粥样硬化性血管疾病。因此,改变血小板功能的药物可能具有保护作用。鉴于心得安治疗可使冠心病患者过度活跃的血小板聚集恢复正常,我们对心得安进行了体外研究,以评估其对血小板的作用。在与体内达到的浓度相似(0.1 - 1μM)时,心得安提高了一些正常血小板对二磷酸腺苷(ADP)聚集的阈值。在更高浓度(10 - 50μM)时,心得安消除了由ADP和肾上腺素诱导的血小板聚集的第二波,并抑制了由胶原、凝血酶和离子载体A23187诱导的聚集。心得安阻止了血小板中14C - 5羟色胺的释放,抑制了血小板与胶原的黏附,并干扰了血块收缩。心得安阻止了离子载体诱导的血小板对45Ca的摄取。抑制作用似乎与β - 肾上腺素能阻滞无关,因为d(+)心得安(缺乏β - 阻滞活性)与l(-)心得安具有同等效力。此外,非亲脂性的β - 阻滞药物醋丁洛尔并不抑制血小板功能。这些研究表明,心得安与局部麻醉药一样,通过直接作用于血小板膜,可能是通过干扰钙的可用性来降低血小板反应性。心得安对血小板功能的调节可能发生在该药物常用临床剂量所达到的浓度下。

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