Ondansetron achieved complete or major control of emesis in 86% of patients compared to 42% with metoclopramide in the first 24 hours (P<.001).
RCT (n=75)
Double-blind
Randomized
Does ondansetron improve control of chemotherapy-induced emesis compared to metoclopramide in breast cancer patients?
Ondansetron is significantly more effective than metoclopramide in preventing acute emesis and nausea induced by cyclophosphamide-based chemotherapy in breast cancer patients.
Absolute Event Rate: 86% vs 42%
p-value: p=<.001
Seventy-five breast cancer patients scheduled to receive a first course (in a new cycle) of cyclophosphamide, fluorouracil, and doxorubicin (FAC) or epirubicin (FEC) participated in a double-blind crossover study to compare the antiemetic efficacy and safety of ondansetron (GR38032), a 5-hydroxytryptamine3 (5-HT3) receptor antagonist, and metoclopramide. Ondansetron was given as an 8 mg loading dose (4 mg intravenously IV plus 4 mg orally) before chemotherapy followed by 8 mg every 8 hours orally for 3 to 5 days. Metoclopramide was given as an 80 mg loading dose (60 mg IV plus 20 mg orally) before chemotherapy followed by 20 mg every 8 hours orally for 3 to 5 days. A "period" interaction in the analysis of emetic response in the first 24 hours necessitated a parallel group analysis of first treatments only, 68 patients being assessable for this parameter. In the first 24 hours, complete or major control (zero to two emetic episodes) of emesis was achieved in 30 of 35 (86%) patients receiving ondansetron and in 14 of 33 (42%) patients receiving metoclopramide (P less than .001). Ondansetron was also more effective in reducing acute nausea. On days 2 to 3, the complete or major responses were significantly better with ondansetron (81% v 65%; P = .033), but there was no statistical difference in the control of nausea. There was a significant patient preference for ondansetron (63% v 26%; P = .001). Extrapyramidal reactions were observed in two metoclopramide treatments; both treatments were otherwise well tolerated. These results are consistent with serotonin (5-HT), being a significant neurotransmitter of cyclophosphamide/doxorubicin- or epirubicin/fluorouracil-induced emesis.
Bonneterre et al. (Fri,) conducted a rct in Breast cancer receiving FAC or FEC chemotherapy (n=75). Ondansetron vs. Metoclopramide was evaluated on Complete or major control (zero to two emetic episodes) of emesis in the first 24 hours (p=<.001). Ondansetron achieved complete or major control of emesis in 86% of patients compared to 42% with metoclopramide in the first 24 hours (P<.001).