Evaluation of physical variables, thermal nociceptive threshold testing and pharmacokinetics during placement of transdermal buprenorphine matrix-type patch in healthy adult horses

Frontiers in Pain Research Pub Date : 2024-03-11 DOI:10.3389/fpain.2024.1373555

V. Paranjape, Heather K. Knych, L. Berghaus, Jessica Cathcart, S. Giancola, Hannah Craig, Caroline James, Siddharth Saksena, Rachel A. Reed

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Abstract

Matrix type transdermal buprenorphine patches have not been investigated in horses and may provide an effective means of providing continuous pain control for extended period and eliminating venous catheterization.Assessment of the physiological variables (heart rate, respiratory rate, body temperature) and thermal nociceptive threshold testing, and describing the pharmacokinetic profile of transdermal buprenorphine matrix-type patch (20 μg h−1 and 40 μg h−1 dosing) in healthy adult horses.Randomised experimental study with a Latin-square design.Six adult healthy horses received each of the three treatments with a minimum 10 day washout period. BUP0 horses did not receive a patch (control). BUP20 horses received one patch (20 μg h−1) applied on the ventral aspect of the tail base resulting in a dose of 0.03–0.04 μg kg−1 h−1. BUP40 horses received two patches placed alongside each other (40 μg h−1) on the tail base resulting in a dose of 0.07–0.09 μg kg−1 h−1. Whole blood samples (for determination of buprenorphine concentration), physiological variables and thermal threshold testing were performed before (0 h) and at 2, 4, 8, 12, 16, 24, 32, 40, 48, 56, 64, 72, and 96 h after patch application. The patches were removed 72 h following placement and were analyzed for residual buprenorphine content.Between the three groups, there was no change in physiological variables across timepoints as compared to baseline (p > 0.1). With the higher dose, there was a significant increase in thermal thresholds from baseline values from 2 h until 48 h and these values were significantly higher than the group receiving the lower patch dose for multiple timepoints up to 40 h. 40 μg h−1 patch led to consistent measurable plasma concentrations starting at 2 h up to 96 h, with the mean plasma concentrations of > 0.1 ng/ml from 4 h to 40 h.20 μg h−1 and 40 μg h−1 patch doses were well tolerated by all horses. At higher dose, plasma buprenorphine concentrations were more consistently measurable and blunted thermal thresholds for 48 h vs. 32 h with 20 μg h−1 dosing as compared to control.

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评估健康成年马在贴敷透皮丁丙诺啡基质型贴片期间的物理变量、热痛觉阈值测试和药代动力学

基质型透皮丁丙诺啡贴片尚未在马匹身上进行过研究，但它可能是一种有效的方法，可以长时间持续控制疼痛，并省去静脉导管插入术。评估健康成年马的生理变量（心率、呼吸频率、体温）和热痛觉阈值测试，并描述透皮丁丙诺啡基质型贴片（20 μg h-1 和 40 μg h-1剂量）的药代动力学特征。BUP0 马匹不接受药贴（对照组）。BUP20 马匹在尾基部腹侧接受一贴（20 μg h-1），剂量为 0.03-0.04 μg kg-1 h-1。BUP40 马的尾基部接受两贴（40 μg h-1），剂量为 0.07-0.09 μg kg-1 h-1。在贴敷前（0 h）和贴敷后 2、4、8、12、16、24、32、40、48、56、64、72 和 96 h 进行全血采样（用于测定丁丙诺啡浓度）、生理变量和热阈值测试。贴敷 72 小时后取下贴片，分析残留的丁丙诺啡含量。三组之间，各时间点的生理变量与基线相比没有变化（P > 0.1）。使用高剂量贴片后，从 2 小时到 48 小时，热阈值与基线值相比有显著增加，在 40 小时内的多个时间点，热阈值显著高于使用低剂量贴片的组别。从 2 小时到 96 小时，40 μg h-1 贴片可持续产生可测量的血浆浓度，从 4 小时到 40 小时，平均血浆浓度> 0.1 ng/ml。与对照组相比，在较高剂量下，血浆丁丙诺啡浓度的可测量性更稳定，并且在 20 μg h-1 给药的 48 小时与 32 小时内，热阈值变得迟钝。

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Frontiers in Pain Research

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