Prospective, controlled, blinded, randomized crossover trial evaluating the effect of maropitant versus ondansetron on inhibiting tranexamic acid-evoked emesis

被引:8
|
作者
Kantyka, Marta E. [1 ]
Meira, Carolina [1 ]
Bettschart-Wolfensberger, Regula [1 ]
Hartnack, Sonja [2 ]
Kutter, Annette P. N. [1 ]
机构
[1] Univ Zurich, Vetsuisse Fac, Sect Anesthesiol, Dept Clin Diagnost & Serv, Zurich, Switzerland
[2] Univ Zurich, Vetsuisse Fac, Epidemiol Sect, Zurich, Switzerland
关键词
antifibrinolytic agents; canine; nausea; side effects; vomiting; EPSILON-AMINOCAPROIC ACID; RETIRED RACING GREYHOUNDS; BLEEDING TRAUMA PATIENTS; LOW-DOSE CISPLATIN; POSTOPERATIVE NAUSEA; DOGS; PREVENTION; EFFICACY; HYPERFIBRINOLYSIS; PHARMACOKINETICS;
D O I
10.1111/vec.12954
中图分类号
S85 [动物医学(兽医学)];
学科分类号
0906 ;
摘要
Objective To evaluate the incidence of tranexamic acid (TXA)-induced nausea and vomiting after the prophylactic use of 2 antiemetics, ondansetron and maropitant, compared with saline. Design Prospective, blinded, placebo-controlled, randomized, crossover study. Setting University research facility. Animals Eight adult, purpose-bred Beagles. Intervention Dogs received 3 treatments on 3 occasions with a 3-week washout period. Either maropitant (1 mg/kg), ondansetron (0.2 mg/kg), or saline solution was given intravenously in equal volumes, followed 10 minutes later by 50 mg/kg IV TXA. A blinded observer evaluated the dogs for signs of vomiting and nausea for 30 minutes. The severity of nausea was assessed with a visual analog scale (VAS) and recorded at baseline before TXA, and at the end of 3 observational periods: 0-5, 5-15, and 15-30 minutes after TXA. A generalized linear mixed effect model was used to assess for group and period effects. Statistical significance was set at P<0.05. Measurements and main results None of the dogs vomited after maropitant. Emesis occurred in 5 out of 8 dogs (62.5%), a median (range) of 1 time (1-2) after ondansetron and 1 time (1-3) after saline. There was a significant effect on vomiting of maropitant against saline (P < 0.0001) but not for ondansetron against saline (P = 0.53). The highest nausea VASs were recorded during the first 5 minutes after TXA with a significant reduction of VAS variability in the maropitant group (P = 0.003). The effect of maropitant and ondansetron against saline on the severity of nausea was not statistically significant (P = 0.069). Conclusion The neurokinin 1 receptor antagonist maropitant at the dose used, administered IV 10 minutes before 50 mg/kg TXA, was effective in preventing vomiting compared with ondansetron and placebo. Our results support the prophylactic IV administration of maropitant in dogs that are scheduled to receive TXA.
引用
收藏
页码:436 / 441
页数:6
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