Incidence of and risk factors for postoperative nausea and vomiting at a Japanese Cancer Center: first large-scale study in Japan

The subjects of the study were patients with an American Society of Anesthesiologists physical status (ASA PS) of I to III who underwent elective surgery with general or local anesthesia. The following patients were excluded: pregnant women, patients requiring intensive care unit treatment, patients receiving or scheduled to receive a mild or greater emetogenic anticancer drug from 6 days before study entry to 48 h after anesthesia, patients with a symptomatic brain metastasis, patients unable to communicate for a mental reason, and patients for whom any of the following antiemetics were used 48 or fewer hours before the start of anesthesia or during anesthesia: a 5-HT3 receptor antagonist, dexamethasone, phenothiazine drug product, butyrophenone drug product, benzamide drug product, dopamine receptor antagonist, antihistamine, or a NK1 receptor antagonist. Patients for whom none of the exclusion criteria applied and who provided informed consent in writing were included in the study.

No preanesthetic premedication drug was administered. Propofol was administered to induce anesthesia; rocuronium or vecuronium was administered as a muscle relaxant; remifentanil, fentanyl, or morphine hydrochloride was administered as an opioid; sevoflurane, propofol, or nitrous oxide was administered for maintenance of anesthesia; and sugammadex sodium or neostigmine was administered to reverse the muscle relaxants. The attending anesthesiologist selected the particular drugs as normal. The prophylactic administration of antiemetics was not allowed except for postoperative rescue. Metoclopramide, which is approved in Japan for PONV, was used as the antiemetic.

The attending anesthesiologist recorded patient characteristics on the day before surgery. During anesthesia, the anesthesiologist recorded the disease name, surgery type, anesthesia used, type and dose of any anesthesia-related drugs used, and duration of anesthesia. Following anesthesia, a ward nurse recorded the antiemetic used.

We determined that evaluating PONV until 48 h after anesthesia could provide data that would be useful in the future, because NK1 receptor antagonists, the 5-HT3 receptor antagonist palonosetron, and other long-acting drugs have recently been used for treating PONV. PONV was therefore evaluated from 0 to 2, 2 to 24, and 24 to 48 h after anesthesia. PONV was evaluated by an anesthesiologist in the operating room and a nurse in the wards. The evaluator recorded whether nausea was present, and if so, the severity and the number of vomiting or retching episodes. Nausea was defined as a subjective sensation of the desire to vomit by the patient without actual movement of the expelling muscles.

The frequencies and percentages of the patient characteristics were calculated in each category, as follows. The median age and age range (minimum–maximum) were calculated along with the mean body weight and standard deviation. The mean opioid dose was calculated along with the standard deviation. For the duration of anesthesia, the lower quartile, median, and upper quartile were calculated. Next, the frequencies and percentages of subjects with nausea, vomiting, and PONV were calculated individually for each surgery type and risk factor at 0–2 h, 2–24 h, 24–48 h, 0–24 h overall, and 0–48 h overall after anesthesia. Logistic univariate regression analysis 0–2 h, 2–24 h, 24–48 h, 0–24 h overall, and 0–48 h overall after anesthesia was conducted to investigate the relationship of the risk factors to nausea, vomiting, and PONV frequency. The regression coefficients, standard errors, odds ratios (ORs), and 95 % confidence intervals (CIs) were calculated along with Wald P values. To avoid the problems of multicollinearity between individual risk factors, the significance of correlations was tested using Spearman’s correlation coefficient, and r values of ≥0.6 were defined as the presence of association. The 13 factors that had no multicollinearity issues and that were considered relevant to PONV were selected from the factors that univariate analysis suggested as being related and were submitted to logistic multivariate regression analysis by the forced-entry method. Adjusted ORs, 95 % CIs, and Wald P values were calculated. Seven of these 13 factors (sex, history of PONV, nonsmoking status, volatile anesthesia vs. total intravenous anesthesia [TIVA], nitrous oxide, reversal of muscle relaxation, and postoperative opioids) were dichotomous. Because the 13 factors did not include local anesthesia, multivariate analysis was performed after excluding the cases of local anesthesia. Remifentanil and fentanyl doses were analyzed as continuous variables, with adjusted ORs calculated every 1000 μg for remifentanil and every 100 μg for fentanyl. The category variables for the remaining 4 factors were as follows. For body mass index (BMI), ≥25 kg/m² and <25 kg/m², for duration of anesthesia, >1 h and ≤1 h, for alcohol drinking, on ≤4 days per week and >4 days per week, and for age, ≥50 years and <50 years. In all analyses a P value of less than 0.05 constituted statistical significance. SAS 9.2 (SAS Institute, Cary, NC, USA) was used to perform the statistical analyses.