首页> 美国卫生研究院文献>Journal of Chemical Biology >In thrombin stimulated human platelets Citalopram Promethazine Risperidone and Ziprasidone but not Diazepam may exert their pharmacological effects also through intercalation in membrane phospholipids in a receptor-independent manner
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In thrombin stimulated human platelets Citalopram Promethazine Risperidone and Ziprasidone but not Diazepam may exert their pharmacological effects also through intercalation in membrane phospholipids in a receptor-independent manner

机译:在凝血酶刺激的人血小板中西酞普兰异丙嗪利培酮和齐普拉西酮(但不是地西p)可能通过以非受体依赖的方式插入膜磷脂中而发挥药理作用

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摘要

Intercalation of drugs in the platelet membrane affects phospholipid-requiring enzymatic processes according to the drugs’ intercalation capability. We investigated effects of Promethazine, Citalopram, Ziprasidone, Risperidone, and Diazepam on phospholipase A2 (PLA2) and polyphosphoinositide (PPI) metabolism in thrombin-stimulated human platelets. We also examined effects of the drugs on monolayers of glycerophospholipids using the Langmuir technique. Diazepam did not influence PLA>2 activity, had no effects on PPI cycle, and caused no change in mean molecular area of phospholipid monolayers. The remaining psychotropic drugs affected these parameters in different ways and levels of potency suggesting that they act by being intercalated between the molecules of adjacent membrane phospholipids, thus causing changes in substrate availability for phospholipid-hydrolyzing enzymes (PLA2 and Phospholipase C). We show that several psychotropic drugs can also have other cellular effects than receptor antagonism. These effects may be implicated in the psychotropic effects of the drugs and/or their side effects.
机译:根据药物的嵌入能力,药物在血小板膜中的嵌入会影响需要磷脂的酶促过程。我们研究了异丙嗪,西酞普兰,齐普拉西酮,利培酮和地西p对凝血酶刺激的人血小板中磷脂酶A2(PLA2)和聚磷酸肌醇(PPI)代谢的影响。我们还使用Langmuir技术检查了药物对甘油磷脂单层的影响。地西p不影响PLA > 2 的活性,对PPI循环没有影响,并且不会引起磷脂单分子层平均分子面积的变化。其余的精神药物以不同的方式和效力水平影响这些参数,表明它们通过插入相邻膜磷脂分子之间而起作用,从而导致磷脂水解酶(PLA2和磷脂酶C)的底物利用率发生变化。我们表明,几种精神药物也可以具有除受体拮抗作用以外的其他细胞作用。这些作用可能与药物的精神作用和/或其副作用有关。

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