3种丁丙诺啡制剂对免疫缺陷NSG小鼠足底切开后超敏反应的抑制作用。

IF 1.2 3区 农林科学 Q3 VETERINARY SCIENCES Journal of the American Association for Laboratory Animal Science Pub Date : 2022-09-01 DOI:10.30802/AALAS-JAALAS-22-000058
Justin D Arthur, Eden D Alamaw, Katechan Jampachairsri, Patrick Sharp, Claude Nagamine, Monika K Huss, Cholawat Pacharinsak
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引用次数: 0

摘要

丁丙诺啡可能是治疗小鼠术后疼痛最常用的镇痛药。尽管各种丁丙诺啡制剂在常用的免疫能力小鼠株中有效,但其在免疫缺陷小鼠中的有效性存在知识差距。本研究采用足底切口,评价3种丁丙诺啡制剂对免疫缺陷NSG小鼠品系术后机械和热超敏反应的缓解效果。我们还描述了这些制剂在72小时内的药代动力学。我们假设评估的所有3种丁丙诺啡制剂——标准制剂和2种缓释制剂(分别为Bup-HCl、Bup-ER和Bup-XR)——都能减轻NSG小鼠足底切口术后引起的机械和热过敏。雄性和雌性NSG小鼠48只,随机分为4个处理组:生理盐水(0.9% NaCl, 5 mL/kg SC 1次);Bup-HCl (0.1 mg/kg SC, BID 2 d);Bup-ER (1.0 mg/kg SC一次);Bup-XR (3.25 mg/kg SC一次)。术前24小时和术后4、8、24、48、72小时分别进行力学和热超敏反应评估。各组小鼠在术后24小时内均出现机械和热超敏反应。观察术后各时间点各组部分小鼠的行为性疼痛指标(守卫、触趾[间歇性部分负重]、舔切口、发声)。在另一组小鼠中测量血浆丁丙诺啡,Bup-HCl浓度超过建议治疗水平(1.0 ng/mL)不到4小时,Bup-ER超过至少24小时,Bup-XR超过72小时。我们的研究结果表明,在研究剂量下,这些丁丙诺啡制剂不能充分减轻NSG小鼠足底切口模型的术后机械和热过敏。这些发现支持了在研究中使用小鼠的特定品系镇痛方案的必要性。
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Efficacy of 3 Buprenorphine Formulations for the Attenuation of Hypersensitivity after Plantar Incision in Immunodeficient NSG Mice.

Buprenorphine is perhaps the most prescribed analgesic for management of postoperative pain in mice. Although various buprenorphine formulations are effective in commonly used immunocompetent mouse strains, a knowledge gap exists regarding its efficacy in immunodeficient mice. Here we used a plantar incision to evaluate the efficacy of 3 buprenorphine formulations for attenuating postoperative mechanical and thermal hypersensitivity in the immunodeficient NSG mouse strain. We also characterized the pharmacokinetics of these formulations over a 72-h period. We hypothesized that all 3 buprenorphine formulations evaluated-the standard preparation and 2 extended-release products (Bup-HCl, Bup-ER, and Bup-XR, respectively)-would attenuate postoperative mechanical and thermal hypersensitivity resulting from a plantar incision in NSG mice. Male and female NSG mice (n = 48) were allocated to 4 treatment groups: saline (0.9% NaCl, 5 mL/kg SC once); Bup-HCl (0.1 mg/kg SC, BID for 2 d); Bup-ER (1.0 mg/kg SC once); and Bup-XR (3.25 mg/kg SC once). Mechani- cal and thermal hypersensitivity assessments were conducted 24 h before surgery and at 4, 8, 24, 48, and 72 h afterward. All groups of mice showed mechanical and thermal hypersensitivity within the first 24 h after surgery. Behavioral pain indicators (guarding, toe-touching [intermittent partial weight bearing], licking the incision, vocalizations) were observed in some mice from each group at every postoperative time point. Plasma buprenorphine was measured in a separate group of mice and concentrations surpassed the suggested therapeutic level (1.0 ng/mL) for less than 4 h for Bup-HCl, for at least 24 h for Bup-ER, and for 72 h for Bup-XR. Our results indicate that at the dosages studied, these buprenorphine formulations do not adequately attenuate postoperative mechanical and thermal hypersensitivity in the plantar incisional model in NSG mice. These findings support the need for strain-specific analgesic protocols for mice used in research.

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来源期刊
CiteScore
3.10
自引率
35.30%
发文量
122
审稿时长
6-12 weeks
期刊介绍: The Journal of the American Association for Laboratory Animal Science (JAALAS) serves as an official communication vehicle for the American Association for Laboratory Animal Science (AALAS). The journal includes a section of refereed articles and a section of AALAS association news. All signed articles, including refereed articles and book reviews, editorials, committee reports, and news and commentary, reflect the individual views of the authors and are not official views of AALAS. The mission of the refereed section of the journal is to disseminate high-quality, peer-reviewed information on animal biology, technology, facility operations, management, and compliance as relevant to the AALAS membership. JAALAS accepts research reports (data-based) or scholarly reports (literature-based), with the caveat that all articles, including solicited manuscripts, must include appropriate references and must undergo peer review.
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