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凝血酶在调节内皮细胞前列腺素生成中的作用。

The role of thrombin in the regulation of the endothelial prostaglandin production.

作者信息

de Groot P G, Brinkman H J, Gonsalves M D, Van Mourik J A

出版信息

Biochim Biophys Acta. 1985 Sep 30;846(3):342-9. doi: 10.1016/0167-4889(85)90004-7.

Abstract

Prostaglandin synthesis in endothelial cells may be initiated by the addition of exogenous substrate (arachidonic acid) or by addition of thrombin or the CA2+-ionophore A23187, which leads to prostacyclin formation from endogenous substrates. We noticed that endothelial cells produce more than twice the amount of prostacyclin when incubated with thrombin and arachidonic acid together than with arachidonic acid alone. In addition, it was found that the thrombin-induced conversion of endogenous substrates was inhibited by exogenous arachidonic acid. This means that the conversion of exogenous added arachidonic acid to prostacyclin was stimulated by thrombin. This activation of the enzymes involved in prostacyclin synthesis lasted about 5 min and could be inhibited by phospholipase inhibitors such as mepacrine and p-bromophenyl-acylbromide but not by the cAMP analogue dibutyryl cAMP, an inhibitor of arachidonic acid release from cellular phospholipids. These data demonstrate that, in addition to causing release of endogenous substrate, thrombin and the Ca2+-ionophore also activate the enzyme system involved in the further transformation of arachidonic acid.

摘要

内皮细胞中的前列腺素合成可通过添加外源性底物(花生四烯酸)或添加凝血酶或钙离子载体A23187启动,这会导致内源性底物形成前列环素。我们注意到,与单独使用花生四烯酸相比,内皮细胞在与凝血酶和花生四烯酸一起孵育时产生的前列环素量是单独使用花生四烯酸时的两倍多。此外,还发现外源性花生四烯酸可抑制凝血酶诱导的内源性底物转化。这意味着凝血酶刺激了外源性添加的花生四烯酸向前列环素的转化。这种参与前列环素合成的酶的激活持续约5分钟,可被磷脂酶抑制剂如米帕林和对溴苯基酰溴抑制,但不能被环磷酸腺苷类似物二丁酰环磷酸腺苷抑制,二丁酰环磷酸腺苷是一种抑制花生四烯酸从细胞磷脂中释放的抑制剂。这些数据表明,除了引起内源性底物释放外,凝血酶和钙离子载体还激活参与花生四烯酸进一步转化的酶系统。

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