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Relaxations to oestrogen receptor subtype selective agonists in rat and mouse arteries.

机译:松弛大鼠和小鼠动脉中的雌激素受体亚型选择性激动剂。

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It has been recently reported that the oestrogen receptor alpha agonist PPT (4,4',4"-(4-propyl-[1H]-pyrazole-1,3,5-triyl) tris-phenol) is more potent than the oestrogen receptor beta agonist DPN (2,3-bis(4-hydroxyphenyl)-propionitrile) at producing relaxations in rat mesenteric artery. We have investigated the relaxant actions of PPT and DPN in rat and mouse aorta and mesenteric artery. In rat aortic rings contracted with KCl (40 mM), the oestrogen receptor beta agonist DPN produced significantly greater relaxations than the oestrogen receptor alpha agonist PPT. In wild-type (WT) mouse aorta, the same result was found, but in WT mouse mesenteric artery, as in rat mesenteric artery, DPN was significantly less potent than PPT in females but had similar potency to PPT in males. Relaxations to DPN also occurred in aorta from nitric oxide synthase-3-knockout (NOS-3-KO) mice, and in denuded aorta from both mouse and rat. Hence, in the mouse mesenteric artery, as in the rat mesenteric artery, PPT is at least as potent as DPN at producing relaxations; however, DPN was much more potent than PPT in the rat and mouse aorta. Effects of oestrogen receptor subtype selective agonists are tissue dependent. In addition, actions are largely endothelium-independent.
机译:最近有报道,雌激素受体α激动剂PPT(4,4',4“-(4-丙基-[1H]-吡唑-1,3,5-三基)三酚)比雌激素更有效。受体β激动剂DPN(2,3-双(4-羟苯基)-丙腈)在大鼠肠系膜动脉中产生松弛作用。我们研究了PPT和DPN在大鼠和小鼠主动脉及肠系膜动脉中的松弛作用。在大鼠主动脉环收缩中用KCl(40 mM),雌激素受体β激动剂DPN产生的松弛作用明显大于雌激素受体α激动剂PPT。在野生型(WT)小鼠主动脉中,也发现了相同的结果,但在WT小鼠肠系膜动脉中在大鼠肠系膜动脉中,DPN在雌性中的效力明显低于PPT,但在雄性中的效力与PPT相似;一氧化氮合酶3敲除(NOS-3-KO)小鼠的主动脉和裸露的主动脉中DPN的松弛也发生因此,在小鼠肠系膜动脉中,就像在大鼠肠系膜动脉中一样PPT在产生松弛方面至少与DPN一样有效;然而,在大鼠和小鼠主动脉中,DPN的效力比PPT强得多。雌激素受体亚型选择性激动剂的作用是组织依赖性的。另外,作用在很大程度上与内皮无关。

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