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新型胃肠外给药的环氧化酶-2特异性抑制剂帕瑞昔布对大鼠离体子宫肌层自发性收缩和前列腺素诱导收缩的抑制作用

Tocolytic effect of parecoxib, a new parenteral cyclo-oxygenase-2-specific inhibitor, on the spontaneous and prostaglandin-induced contractions of rat isolated myometrium.

作者信息

Ayar A

机构信息

Department of Physiology, Faculty of Medicine, Firat University, Elazig, Turkey.

出版信息

Clin Exp Pharmacol Physiol. 2007 Aug;34(8):737-41. doi: 10.1111/j.1440-1681.2007.04632.x.

DOI:10.1111/j.1440-1681.2007.04632.x
PMID:17600550
Abstract
  1. The present study was undertaken to elucidate the effects of parecoxib, a novel cyclo-oxygenase (COX)-2 inhibitor, on spontaneous and prostaglandin-induced contractions of uterine smooth muscle. 2. Non-pregnant adult Wistar rats were decapitated and dissected to isolate myometrial strips. The tissue was mounted in 5 mL organ baths filled with Krebs' solution that was maintained at 37 degrees C and bubbled continuously with a mixture of 95% O(2)-5% CO(2) to give pH 7.4. Contractions were recorded through transducers for isometric tension recording. The dose-dependent effects of parecoxib on contractility were quantified by changes in the mean amplitude, frequency and area under the contractile curve (AUC; percentage of control conditions) of the isometric tension recordings, averaged over 5 min intervals. Statistical analyses were performed using ANOVA. 3. Application of parecoxib (50-900 micromol/L) caused dose-dependent decreases in mean amplitude, mean frequency and mean AUC of both spontaneous and prostaglandin-induced contractions. Mean percentage inhibition of the AUC of spontaneous contractions was found to be 29, 56, 74 and 84% in the presence of 50, 150, 300 and 600 micromol/L parecoxib, resepctively (n = 8). In the case of prostaglandin (PG) F(2alpha)-induced contractions, 100, 300, 600 and 900 micromol/L parecoxib resulted in a 27, 43, 61 and 73% inhibition, respectively (n = 9). Moreover, pretreatment with parecoxib (600 micromol/L) reduced the responsiveness and maximum contractility to PGF(2alpha) compared with non-treated strips. 4. The data from the present study indicate, for the first time, that parecoxib inhibits spontaneous and prostaglandin-induced contractions of rat myometrium in vitro. These results raise the possibility that parecoxib may be of therapeutic use in the management of preterm labour and dysmenorrhoea.
摘要
  1. 本研究旨在阐明新型环氧化酶(COX)-2抑制剂帕瑞昔布对子宫平滑肌自发收缩和前列腺素诱导收缩的影响。2. 将未孕成年Wistar大鼠断头并解剖,分离出子宫肌条。将组织置于装有Krebs溶液的5 mL器官浴中,溶液保持在37℃,并持续用95% O₂-5% CO₂的混合气体鼓泡以使pH值为7.4。通过换能器记录等长张力收缩。帕瑞昔布对收缩性的剂量依赖性效应通过等长张力记录的平均振幅、频率和收缩曲线下面积(AUC;对照条件的百分比)的变化进行量化,在5分钟间隔内进行平均。使用方差分析进行统计分析。3. 应用帕瑞昔布(50 - 900 μmol/L)导致自发收缩和前列腺素诱导收缩的平均振幅、平均频率和平均AUC呈剂量依赖性降低。在存在50、150、300和600 μmol/L帕瑞昔布的情况下,自发收缩的AUC的平均抑制百分比分别为29%、56%、74%和84%(n = 8)。对于前列腺素(PG)F₂α诱导的收缩,100、300、600和900 μmol/L帕瑞昔布分别导致27%、43%、61%和73%的抑制(n = 9)。此外,与未处理的肌条相比,用帕瑞昔布(600 μmol/L)预处理降低了对PGF₂α的反应性和最大收缩性。4. 本研究的数据首次表明,帕瑞昔布在体外抑制大鼠子宫肌层的自发收缩和前列腺素诱导的收缩。这些结果增加了帕瑞昔布可能在早产和痛经管理中具有治疗用途的可能性。

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