A Pharmacokinetic and Analgesic Efficacy Study of Carprofen in Female CD1 Mice.

Brandon A McKenna, Hannah L Weaver, Jeffrey Kim, Madelyn W Bowman, Heather K Knych, Lon V Kendall
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Abstract

The minimization of pain in research animals is a scientific and ethical necessity. Carprofen is commonly used for pain management in mice; however, some data suggest that the standard dosage of 5 mg/kg may not provide adequate analgesia after surgery. We hypothesized that a higher dose of carprofen in mice would reduce pain-associated behaviors and improve analgesia without toxic effects. A pharmacokinetic study was performed in mice given carprofen subcutaneously at 10 or 20 mg/kg. Plasma concentrations were measured at 0.25, 0.5, 1, 2, 4, 8, 12, 24, and 48 h after dosing (n = 3 per time point and treatment). At these doses, plasma levels were above the purported therapeutic level for at least 12 and 24 h, respectively, with respective half-lives of 14.9 and 10.2 h. For the efficacy study, 10 mice per group received anesthesia with or without an ovariectomy. Mice were then given 5 or 10 mg/kg of carprofen, or saline subcutaneously every 12 h. Orbital tightening, arched posture, wound licking, rearing, grooming, nesting behavior, and activity were assessed before surgery and at 4, 8, 12, 24, and 48 h after surgery. The von Frey responses were assessed before and at 4, 12, 24, and 48 h after surgery. The efficacy study showed that all surgery groups had significantly higher scores for orbital tightening, arched posture, and wound licking than did the anesthesia-only groups at 4, 8, 12, and 24-h time points. At the 8 h time point, the surgery groups treated with carprofen had significantly lower arched posture scores than did the surgery group treated with saline only. No significant differences were found between carprofen treatment groups for rearing, grooming, von Frey, activity, or nesting behavior at any time point. These results indicate that subcutaneous carprofen administered at these doses does not provide sufficient analgesia to alleviate postoperative pain in female CD1 mice.

克罗芬在雌性CD1小鼠体内的药代动力学和镇痛作用研究。
尽量减少研究动物的疼痛是科学和伦理的必要条件。卡普罗芬通常用于小鼠的疼痛管理;然而,一些数据表明,5mg/kg的标准剂量可能不能在手术后提供足够的镇痛作用。我们假设,在小鼠中服用更高剂量的卡洛芬可以减少疼痛相关行为,改善痛觉,而不会产生毒性作用。对皮下注射10或20 mg/kg卡洛芬的小鼠进行了药代动力学研究。在给药后0.25、0.5、1、2、4、8、12、24和48小时测量血浆浓度(每个时间点和治疗n=3)。在这些剂量下,血浆水平分别在至少12和24小时内高于预期的治疗水平,半衰期分别为14.9和10.2小时。在疗效研究中,每组10只小鼠接受麻醉,无论是否进行无卵巢切除术。然后每12小时给小鼠皮下注射5或10 mg/kg的卡洛芬或生理盐水。在手术前和手术后4、8、12、24和48小时评估眼眶收紧、足弓支撑、舔舐伤口、饲养、梳理、筑巢行为和活动。在手术前和手术后4、12、24和48小时评估von Frey反应。疗效研究表明,在4、8、12和24小时的时间点,所有手术组在眼眶收紧、弓形姿势和舔舐伤口方面的得分都明显高于仅麻醉组。在8h时间点,用卡洛芬治疗的手术组的弓形姿势得分显著低于仅用生理盐水治疗的手术小组。在任何时间点,carprofen治疗组在饲养、梳理、von Frey、活动或筑巢行为方面均未发现显著差异。这些结果表明,在雌性CD1小鼠中,以这些剂量皮下施用的卡洛芬不能提供足够的镇痛来减轻术后疼痛。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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