Mullins Kathleen B, Thomason John M, Lunsford Kari V, Pinchuk Lesya M, Langston Vernon C, Wills Robert W, McLaughlin Ronald M, Mackin Andrew J
Department of Clinical Sciences, College of Veterinary Medicine, Mississippi State University, Mississippi State, MS, USA.
Vet Anaesth Analg. 2012 Mar;39(2):206-17. doi: 10.1111/j.1467-2995.2011.00684.x. Epub 2012 Jan 17.
To determine effects of anti-inflammatory doses of COX-2 selective NSAIDs carprofen, meloxicam, and deracoxib on platelet function in dogs and urine 11-dehydro-thromboxane B2.
Randomized, blocked, crossover design with a 14-day washout period.
Healthy intact female Walker Hounds aged 1-6 years and weighing 20.5-24.2 kg.
Dogs were given NSAIDs for 7 days at recommended doses: carprofen (2.2 mg kg(-1), PO, every 12 hours), carprofen (4.4 mg kg(-1), PO, every 24 hours), meloxicam (0.2 mg kg(-1), PO, on the 1st day then 0.1 mg kg(-1), PO, every 24 hours), and deracoxib (2 mg kg(-1), PO, every 24 hours). Collagen/epinephrine and collagen/ADP PFA-100 cartridges were used to evaluate platelet function before and during and every other day after administration of each drug. Urine 11-dehydro-thromboxane B(2) was also measured before and during administration of each drug.
All NSAIDs significantly prolonged PFA-100 closure times when measured with collagen/epinephrine cartridges, but not with collagen/ADP cartridges. The average duration from drug cessation until return of closure times (collagen/epinephrine cartridges) to baseline values was 11.6, 10.6, 11 and 10.6 days for carprofen (2.2 mg kg(-1) every 12 hours), carprofen (4.4 mg kg(-1) every 24 hours), meloxicam and deracoxib, respectively.
Oral administration of some COX-2 selective NSAIDs causes detectable alterations in platelet function in dogs. As in humans, PFA-100 collagen/ADP cartridges do not reliably detect COX-mediated platelet dysfunction in dogs. Individual assessment of platelet function is advised when administering these drugs prior to surgery, particularly in the presence of other risk factors for bleeding.
确定抗炎剂量的环氧化酶-2(COX-2)选择性非甾体抗炎药(NSAIDs)卡洛芬、美洛昔康和德拉考昔对犬血小板功能及尿11-脱氢血栓素B2的影响。
采用随机、区组、交叉设计,洗脱期为14天。
1至6岁、体重20.5至24.2千克的健康未绝育雌性沃克猎犬。
犬按推荐剂量服用NSAIDs 7天:卡洛芬(2.2毫克/千克,口服,每12小时一次)、卡洛芬(4.4毫克/千克,口服,每24小时一次)、美洛昔康(第1天0.2毫克/千克,口服,之后每24小时0.1毫克/千克)、德拉考昔(2毫克/千克,口服,每24小时一次)。在每种药物给药前、给药期间及给药后每隔一天,使用胶原/肾上腺素和胶原/二磷酸腺苷(ADP)全血血小板功能分析仪(PFA-100)检测盒评估血小板功能。在每种药物给药前及给药期间还检测尿11-脱氢血栓素B2。
当用胶原/肾上腺素检测盒测量时,所有NSAIDs均显著延长PFA-100封闭时间,但用胶原/ADP检测盒测量时则不然。卡洛芬(2.2毫克/千克,每12小时一次)、卡洛芬(4.4毫克/千克,每24小时一次)、美洛昔康和德拉考昔从停药至封闭时间(胶原/肾上腺素检测盒)恢复到基线值的平均持续时间分别为11.6天、10.6天、11天和10.6天。
口服某些COX-2选择性NSAIDs会导致犬血小板功能出现可检测到的改变。与人类一样,PFA-100胶原/ADP检测盒不能可靠地检测犬体内COX介导的血小板功能障碍。在手术前使用这些药物时,建议对血小板功能进行个体评估,尤其是存在其他出血风险因素时。
