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在人体离体模型中,镇痛药安乃近(双氯芬酸钠)的选择性静脉血管舒张特性——对术后疼痛管理的启示

Selective venous vasodilator properties of the analgesic metamizole (dipyrone) in a human ex vivo model-implications for postoperative pain management.

作者信息

Hoenicka Markus, Gorki Hagen, Traeger Karl, Liebold Andreas

机构信息

Department of Cardiothoracic and Vascular Surgery, University of Ulm Medical Center, Albert-Einstein-Allee 23, 89081, Ulm, Germany.

Department of Cardioanaesthesia, University of Ulm Medical Center, Ulm, Germany.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 2017 May;390(5):519-526. doi: 10.1007/s00210-017-1347-6. Epub 2017 Jan 31.

Abstract

Metamizole (dipyrone) is a first-line, non-opioid analgesic used for postoperative pain management. Clinical data and animal experiments indicate a possible vasodilator action of this drug. We investigated the effects of metamizole on human artery and vein tone in an ex vivo model to assess potential contributions to venous pooling. Excess segments of bypass grafts were harvested during coronary artery bypass grafting procedures. Tensions were measured in an organ bath for 120 min after adding metamizole to the preconstricted vessels. Contribution of endothelium was assessed in endothelium-denuded vessels, and indometacin was used to identify cyclooxygenase-mediated effects. Internal mammary arteries (n = 6) constricted after addition of 1, 3, and 10 μM metamizole and remained constricted at the lower doses. Transient constrictions also occurred in saphenous veins (n = 20), but veins relaxed below solvent controls after 20 min at all concentrations. Endothelium removal (n = 12) and cyclooxygenase inhibition (n = 12) suppressed the vasoconstrictor effect but not the vasodilator effect. Metamizole and its metabolites display counteracting effects on blood vessel tone ex vivo. The vasoconstrictor effect is mediated by cyclooxygenase-derived products. The net effect is site-specific, resulting in a selective venous vasodilator action. This may exacerbate unwanted venous pooling during postoperative pain therapy.

摘要

安乃近是一种用于术后疼痛管理的一线非阿片类镇痛药。临床数据和动物实验表明该药物可能具有血管舒张作用。我们在体外模型中研究了安乃近对人体动脉和静脉张力的影响,以评估其对静脉淤积的潜在作用。在冠状动脉搭桥手术过程中采集多余的搭桥血管段。在向预收缩的血管中加入安乃近后,在器官浴中测量张力120分钟。在内皮剥脱的血管中评估内皮的作用,并使用吲哚美辛来确定环氧化酶介导的效应。加入1、3和10 μM安乃近后,乳内动脉(n = 6)收缩,并在较低剂量下持续收缩。隐静脉(n = 20)也出现短暂收缩,但在所有浓度下20分钟后静脉舒张程度低于溶剂对照组。去除内皮(n = 12)和抑制环氧化酶(n = 12)可抑制血管收缩作用,但不能抑制血管舒张作用。安乃近及其代谢产物在体外对血管张力表现出拮抗作用。血管收缩作用由环氧化酶衍生产物介导。净效应具有部位特异性,导致选择性静脉血管舒张作用。这可能会加剧术后疼痛治疗期间不必要的静脉淤积。

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