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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Prostaglandin E 2 induced contraction of human intercostal arteries is mediated by the EP 3 receptor
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Prostaglandin E 2 induced contraction of human intercostal arteries is mediated by the EP 3 receptor

机译:前列腺素E 2诱导人肋间动脉收缩是由EP 3受体介导的

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Arterial vascularization of the spinal cord may be mechanically or functionally altered during thoraco-abdominal surgery/intravascular procedures. Increased arterial pressure has been shown to restore spinal perfusion and function probably by increasing the blood flow through the intercostal arteries. The regulation of human intercostal artery (HICA) vascular tone is not well documented. Prostaglandin (PG)E 2 concentration is increased during inflammatory conditions and has been shown to regulate vascular tone in many preparations. In this context, the pharmacological response of HICA to PGE 2 and the characterization of the PGE 2 receptor subtypes (EP 1, EP 2, EP 3 or EP 4) involved are of importance and that is the aim of this study. Rings of HICA were prepared from 29 patients and suspended in organ baths for isometric recording of tension. Cumulative concentration-response curves were performed in these preparations with various EP receptor agonists in the absence or presence of different receptor antagonists or inhibitors. PGE 2 induced the contraction of HICA (E max = 7.28 ± 0.16 g; pEC 50 value = 0.79 ± 0.18; n = 17); contractions were also observed with the EP 3 receptor agonists, sulprostone, 17-phenyl-PGE 2, misoprostol or ONO-AE-248. In conclusion, PGE 2 induced vasoconstriction of HICA via EP 3 receptor subtypes and this result was confirmed by the use of selective EP receptor antagonists (L-826266, ONO-8713, SC-51322) and by a strong detection of EP 3 mRNA. These observations suggest that in the context of perioperative inflammation, increased PGE 2 concentrations could trigger vasoconstriction of HICA and possibly alter spinal vascularization.
机译:在胸腹外科手术/血管内手术期间,脊髓的动脉血管化可能会发生机械或功能改变。已经显示,动脉压的升高可能通过增加流过肋间动脉的血流来恢复脊柱灌注和功能。人体肋间动脉(HICA)血管张力的调节尚未充分记录。在炎症条件下,前列腺素(PG)E 2的浓度会增加,并且在许多制剂中已显示出其可调节血管紧张度。在这种情况下,HICA对PGE 2的药理反应和所涉及的PGE 2受体亚型(EP 1,EP 2,EP 3或EP 4)的表征非常重要,这是本研究的目的。从29位患者中制备了HICA环,并悬挂在器官浴中以等距记录张力。在这些制剂中,在不存在或存在不同受体拮抗剂或抑制剂的情况下,使用各种EP受体激动剂进行累积浓度反应曲线。 PGE 2诱导HICA收缩(E max = 7.28±0.16 g; pEC 50值= 0.79±0.18; n = 17); EP 3受体激动剂舒普司通,17-苯基-PGE 2,米索前列醇或ONO-AE-248也观察到收缩。总之,PGE 2通过EP 3受体亚型诱导了HICA的血管收缩,这一结果通过使用选择性EP受体拮抗剂(L-826266,ONO-8713,SC-51322)和对EP 3 mRNA的强检测得到了证实。这些观察结果表明,在围手术期发炎的情况下,增加的PGE 2浓度可能会触发HICA的血管收缩,并可能改变脊髓的血管形成。

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