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暴露于GR32191后人血小板上血栓素受体数量的减少。

Reduction in the number of thromboxane receptors on human platelets after exposure to GR32191.

作者信息

Armstrong R A, Humphrey P P, Lumley P

机构信息

Department of Pharmacology, University of Edinburgh Medical School.

出版信息

Br J Pharmacol. 1993 Oct;110(2):548-52. doi: 10.1111/j.1476-5381.1993.tb13845.x.

Abstract
  1. Exposure of human resuspended platelets in vitro for 30 min to the potent thromboxane A2 (TP)-receptor blocking drug GR32191, followed by its removal by dilution-dissociation, reduced the degree of subsequent binding to 2 nM [3H]-GR32191 by almost 50%. Exposure for longer periods (60 min) led to a further reduction. However, no change in the Kd of the radioligand was observed. 2. This effect of GR32191 could not be explained by persistent binding of drug to platelets since a dilution-dissociation stage, designed to remove all drug, was included prior to measurement of binding. 3. Using an alternative TP-receptor radioligand, [3H]-SQ29,548, to monitor receptor number, a reduction in Bmax was observed after GR32191 pre-treatment; the Kd value of the radioligand remained unchanged. 4. The effect was not a common property of TP-receptor blocking drugs since pre-exposure of platelets in vitro for 30 min to BM13.177 or SQ29,548 did not produce a fall in subsequent Bmax to [3H]-SQ29,548. 5. While the mechanism behind this apparent down-regulation of platelet TP-receptor is unknown, it may explain the long duration of action of GR32191 upon platelets in man which persists in the absence of detectable drug in the plasma.
摘要
  1. 将人重新悬浮的血小板在体外暴露于强效血栓素A2(TP)受体阻断药物GR32191 30分钟,随后通过稀释解离将其去除,结果显示,后续与2 nM [3H]-GR32191的结合程度降低了近50%。暴露更长时间(60分钟)会导致进一步降低。然而,未观察到放射性配体的解离常数(Kd)发生变化。2. GR32191的这种作用无法用药物与血小板的持续结合来解释,因为在测量结合之前包含了一个旨在去除所有药物的稀释解离阶段。3. 使用另一种TP受体放射性配体[3H]-SQ29,548来监测受体数量,发现GR32191预处理后最大结合量(Bmax)降低;放射性配体的Kd值保持不变。4. 这种作用并非TP受体阻断药物的共同特性,因为将血小板在体外预先暴露于BM13.177或SQ29,548 30分钟并不会导致后续与[3H]-SQ29,548的Bmax下降。5. 虽然血小板TP受体这种明显下调背后的机制尚不清楚,但这可能解释了GR32191在人体内对血小板的长效作用,即在血浆中检测不到药物的情况下这种作用仍持续存在。

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