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首页> 外文期刊>BMC Veterinary Research >Assessment of the efficacy of firocoxib (Previcox?) and grapiprant (Galliprant?) in an induced model of acute arthritis in dogs
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Assessment of the efficacy of firocoxib (Previcox?) and grapiprant (Galliprant?) in an induced model of acute arthritis in dogs

机译:评估Firocoxib(PREMICOX?)和葡萄普兰(井倾斜剂?)在犬急性关节炎诱导模型中的疗效

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Non-steroidal anti-inflammatory drugs (NSAIDs) are an important tool in the management of canine osteoarthritis, with the most recent introduction into the category being grapiprant, a piprant that selectively targets the EP4 prostaglandin receptor. To date there have been no efficacy studies comparing grapiprant with other NSAIDs. A randomized, two-sequence, assessor-blinded study involving two separate experiments was undertaken to measure the potency and persistence of acute pain control over 24?h resulting from a single oral dose of either firocoxib (Previcox?) or grapiprant (Galliprant?) in an acute arthritis model. Force-plate derived lameness ratios (0, no force recorded on the plate; 1, normal force) for the untreated group remained at 0 for most post-arthritis induction (PAI) assessments in both experiments. Throughout Experiment 1, mean PAI lameness ratios of the firocoxib-treated group remained at or above 0.80. In the grapiprant-treated group, ratios were 0 at 5 and 7?h PAI (7 and 9?h post-treatment), and 0.16 at 10?h PAI (12?h post-treatment). For lameness ratios, relative to the firocoxib group, the control and grapiprant group ratios were significantly lower at each PAI assessment (p?≤?0.026 and p??0.001, respectively), except at 1.5?h PAI at which acute pain was still not installed in untreated control dogs. In Experiment 2 the mean lameness ratios for the control group were 0 at 3, 5 and 7?h PAI, and in the grapiprant group at 5, 7 and 10?h PAI (i.e., 19, 21, and 24?h post-treatment). In the firocoxib group the lowest mean lameness ratio of 0.36 occurred at 3?h PAI (i.e. 17?h post-treatment). Except at 1.5 and 3?h PAI (i.e. 15.5 and 17?h post-treatment), due to the needed time for pain to install in the untreated control dogs, the lameness ratio differences between the firocoxib and both the control and grapiprant groups were significant at all assessments (p?≤?0.033 for both groups). No significant differences were detected between the grapiprant and control groups in either experiment. Firocoxib treatment prior to induction of arthritis in dogs resulted in a high level of analgesia from the first post-treatment assessment at 1.5?h through 24?h post-treatment. The reduction in lameness provided by firocoxib was consistently superior to that provided by grapiprant, which was not significantly different from untreated controls.
机译:非甾体抗炎药(NSAIDs)是犬骨关节炎的管理中的重要工具,最近的介绍是葡萄翻进剂,一种选择性地靶向EP4前列腺素受体的液体。迄今为止,没有对其他NSAID的葡萄球菌进行了疗效研究。随机,双序列,评估综合症研究涉及两个单独的实验,以测量急性疼痛控制超过24μm的效力和持续性,由萤火虫(PREMICOX?)或葡萄普(Galliprant?)中的单一口服剂量引起24℃。在急性关节炎模型中。强制板衍生的跛足比(0,在板上记录的力; 1,未处理组的1,正常力)在两个实验中的大多数关节炎诱导(PAI)评估中保持为0。在整个实验1中,萤火虫治疗组的平均PAI浸润率保持在或高于0.80。在Grapiprant治疗组中,比率在5和7?H pai(治疗后7和9→H后),0.16℃,0.16°Pai(治疗后12μl)。对于跛子比率,相对于萤火虫基团,每个PAI评估,对照和葡萄脂剂群体比率显着降低(P?≤α.026和p≤0.026和p?0.001分别),除了1.5μpai,急性疼痛仍然没有安装在未经治疗的对照犬中。在实验2中,对照组的平均跛足比在3,5和7?H pai,以及在5,7和10℃的甘油链组中(即,19,21和24℃。治疗)。在Firocoxib组中,最低平均跛足比为0.36发生在3°Pai(即治疗后17℃)。除了1.5和3?H Pai(即15.5和17次后处理),由于在未处理的对照犬内安装所需的时间,萤火虫和对照和葡萄浮药组之间的跛足比差异在所有评估中重大(P?≤β033)。在两种实验中,贪婪药物和对照组之间没有检测到显着差异。 Firocoxib治疗在诱导关节炎的疾病中,导致高水平的镇痛从第一个治疗后的第一个治疗后的治疗后24?H. Firocoxib提供的跛足的降低始终如一地优于Grapiprant提供,这与未处理的对照没有显着不同。

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