Aprepitant in combination with palonosetron for the prevention of postoperative nausea and vomiting in female patients using intravenous patient-controlled analgesia
Article information
Abstract
Background
The aim of this study was to evaluate aprepitant in combination with palonosetron as compared to palonosetron alone for the prevention of postoperative nausea and vomiting (PONV) in female patients receiving fentanyl- based intravenous patient-controlled analgesia (IV-PCA).
Methods
In this randomized single-blinded study, 100 female patients scheduled for elective surgery under general anesthesia were randomized to two groups: Group AP (80 mg aprepitant plus 0.075 mg palonosetron, n = 50) and Group P (0.075 mg palonosetron, n = 50). The patients in group AP received 80 mg aprepitant per oral 1–3 h before surgery, while all patients received 0.075 mg palonosetron after induction of standardized anesthesia. All patients had postoperative access to fentanyl-based IV-PCA. The incidence of nausea and vomiting, use of rescue medication, and severity of nausea were evaluated at 6 and 24 h after surgery.
Results
The incidence of nausea (54%) and vomiting (2%) in group AP did not differ significantly from that in group P (48% and 14%, respectively) during the first 24 h after surgery (P > 0.05). Patient requirements for rescue medication in group AP (29%) were similar to those in group P (32%) at 24 h after surgery (P > 0.05). There was no difference between the groups in severity of nausea during the first 24 h after surgery (P > 0.05).
Conclusions
Aprepitant combined with palonosetron did not reduce the incidence of PONV as compared to palonosetron alone within 24 h of surgery in women receiving fentanyl-based IV-PCA.
Introduction
Despite advances in anesthesia and the widespread use of antiemetics, postoperative nausea and vomiting (PONV) are still a common and concerning problem that results in decreased patient satisfaction, delayed recovery, and increased hospital costs. The incidence of PONV has been reported to be 20–50% and can be as high as 80% in patients at high-risk of PONV [1,2].
The pathophysiology of PONV is still unclear. PONV has a multifactorial origin and is thought to occur through a variety of receptors including dopamine, serotonin, histamine, acetylcholine, and neurokinin-1 (NK1) receptors. To prevent PONV, various medications that target one of these receptors are used, including dopamine receptor antagonists, serotonin 5-hydroxytryptamine type 3 (5-HT3) receptor antagonists, histamine receptor antagonists, anticholinergics, corticosteroids, and NK1 receptor antagonists [1,3].
Among these antiemetics, 5-HT3 receptor antagonists are the most commonly used for the prevention of PONV because of their efficacy and low side-effect profile. 5-HT3 receptor antagonists, such as ondansetron, dolasetron, tropisetron, and ramosetron, act on the 5-HT3 receptor by competing with central and peripheral serotonin binding [4].
Palonosetron is a second-generation 5-HT3 antagonist that has a longer half-life (> 40 h) and greater affinity to the 5-HT3 receptor than older 5-HT3 antagonists such as ondansetron, granisetron, and ramosetron. Palonosetron has a distinct chemical structure, mechanism of action, and pharmacodynamic profile compared to older 5-HT3 antagonists. It exhibits allosteric binding and positive cooperativity with the 5-HT3 receptor and triggers 5-HT3 receptor internalization leading to its long duration of action [5]. Palonosetron is effective in preventing chemotherapy-induced nausea and vomiting (CINV) in both acute (0–24 h) and delayed settings (24–120 h). It is the only 5-HT3 receptor antagonist approved for both acute and delayed CINV [6–8]. Palonosetron is effective for the prevention of PONV and was approved in 2008, at a dose of 0.075 mg intravenously, by the US Food and Drug Administration (FDA) for the prevention of PONV for up to 24 h post-surgery [9–11].
Aprepitant is a highly selective antagonist at the NK1 receptor with a half-life of 40 h. Substance P is an endogenous ligand for the NK1 receptor and is a potent inducer of emesis. NK1 receptors are located in the gut, in the area postrema and the nucleus tractus solitarius; these areas are involved in the emesis reflex. Like serotonin, substance P is released by emetogenic chemotherapies and appears to act on receptors that are both peripherally and centrally located. Aprepitant crosses the blood-brain barrier and can act on both central and peripherally located NK1 receptors. An advantage of aprepitant is its strong anti-emetic effect in both the acute and delayed periods. Aprepitant is effective for the prevention of acute CINV, but most importantly is effective in delaying CINV when combined with 5-HT3 antagonists or dexamethasone [12,13]. Therefore, it has been endorsed as part of a three-drug combination (an NK1 receptor antagonist, a 5-HT3 receptor antagonist, and dexamethasone) for the prevention of CINV [14]. For the prevention of PONV, aprepitant is effective for up to 24 h post-surgery and has been demonstrated to be more effective than ondansetron for preventing vomiting at 24 and 48 h post-surgery [15–17]. Aprepitant was the first NK1 receptor antagonist for PONV approved by the US FDA [3].
To date, no single antiemetic agent has shown the ability to eliminate PONV; therefore, combination antiemetic therapy with two or more classes of agents is recommended rather than monotherapy to prevent PONV in high-risk patients [1].
Recently, it was reported that a combination of aprepitant with ramosetron was more effective than ramosetron alone for the prevention of PONV in high-risk patients [18]. However, there are no reports about combination therapy using aprepitant and palonosetron to prevent PONV, although combination therapy using aprepitant, palonosetron, and dexamethasone has been used for the prevention of CINV [14].
We hypothesized that the combination of aprepitant and palonosetron might be superior to palonosetron alone for the prevention of PONV in high-risk patients. We compared the effect of aprepitant in combination with palonosetron to that of palonosetron alone in women at high risk for PONV, who received opioid-based intravenous patient-controlled analgesia (IV-PCA).
Materials and Methods
This prospective, single-blinded randomized controlled trial was approved by our hospital’s Institutional Review Board (No. 2012-159) and was registered in the clinical trials registry (KCT0002433).
The trial included 100 female patients aged 20–70 years with an American Society of Anesthesiologists physical status rating of I–II, who used IV-PCA for postoperative pain control after elective surgery under general anesthesia.
Exclusion criteria included the presence of allergies to palonosetron, aprepitant, nonsteroidal anti-inflammatory drugs or opioids, the use of antiemetic drugs, or steroid medication within 24 h of surgery, nausea or vomiting within 24 h of surgery, dementia or communication difficulties, a history of severe respiratory or cardiovascular disease, a history of gastrointestinal, neurologic, liver, or renal disease, pregnancy, and severe obesity.
All patients were given information about the trial and all provided written informed consent. Patients were divided randomly by a computer-generated number table into Group AP (80 mg oral aprepitant [Emend®, MSD Korea, Korea] plus 0.075 mg intravenous palonosetron, n = 50) or Group P (0.075 mg intravenous palonosetron, n = 50).
The patients allocated to group AP received 80 mg aprepitant peroral with water 2–3 h prior to their surgery. All patients received 0.2 mg glycopyrrolate intramuscularly on the ward 30 min before surgery. On arrival in the operating theatre, standard monitoring was performed, including non-invasive blood pressure, peripheral oxygen saturation, and electrocardiography.
General anesthesia was standardized for each patient. Anesthesia was induced using a bolus of 2 mg/kg 1% propofol and 40 mg 2% lidocaine followed by continuous infusion of remifentanil (0.05–0.5 μg/kg/min). After the loss of consciousness, 0.6 mg/kg rocuronium was administered for muscle relaxation and endotracheal intubation was performed. Anesthesia was maintained with inhaled anesthetics (desflurane or sevoflurane) in 50% oxygen with continuous infusion of remifentanil. After induction of anesthesia, 0.075 mg of palonosetron was administered intravenously to all patients. At the end of the surgical procedure, neuromuscular relaxation was reversed with pyridostigmine and glycopyrrolate, and patients were extubated. All patients received fentanyl-based IV-PCA postoperatively.
When a patient complained of moderate to severe nausea or vomiting, intravenous metoclopramide (10 mg) was administered. If this did not improve their condition, 4 mg intravenous ondansetron was injected as a supplementary treatment.
Our primary end-point was the incidence of PONV during the 24 h postoperative period, with secondary end-points of nausea severity, use of rescue medication, patient satisfaction, and adverse events.
All patients were interviewed regarding the occurrence of nausea and vomiting and were asked to rank their nausea using a four-point verbal rating scale (0 = none, 1 = mild, 2 = moderate, 3 = severe). The use of rescue medication and other adverse effects of IV-PCA or antiemetics were also noted at 1, 6, and 24 h postoperatively. Patient satisfaction at 24 h post-surgery was quantified using a three-point scale (0 = dissatisfied, 1 = neither satisfied nor dissatisfied, 2 = satisfied).
Candiotti et al. [10] reported a PONV incidence of 57% when using 0.075 mg palonosetron, whereas Lee et al. [18] reported an absolute rate of reduction of 30% when using aprepitant combined with ramosetron. Based on these two reports, 42 patients were required per group for a one-sided α = 0.05 at a power of 90%; assuming a drop-out rate of 20%, in total, 50 patients were required for the study. Statistical analyses were performed using SPSS Statistics for Windows, ver. 14.0 (SPSS Inc., USA). The categorical data were analyzed using a chi-squared or Fisher’s exact test and presented as frequencies with percentages. The continuous data were analyzed using Student’s t-test and presented as mean ± SD. A P value of < 0.05 was considered statistically significant.
Results
In total, 115 patients were screened, among whom 100 were enrolled in the study and divided randomly into two groups. Of the study patients, nine in group AP and five in group P were excluded from the study due to protocol violations, while one patient in group P withdrew as the surgery was canceled. Data obtained from the remaining 85 patients were analyzed, with 41 patients in group AP and 44 patients in group P (Fig. 1).
The baseline characteristics of the patients, and their previous operation history, PONV history, motion-sickness history, smoking status, surgery type, duration of surgery, and duration of anesthesia were all similar between the groups (P > 0.05, Table 1).
The incidence of nausea (54%) and vomiting (2%) in group AP did not differ significantly from that in group P (48% and 14%, respectively) during the first 24 h after surgery (P > 0.05, Table 2). In group AP, 29% of patients required rescue medication within 24 h of surgery (P > 0.05) compared to 32% of those in group P (Table 2). The severity of nausea during the first 24 h after surgery was similar in the two groups (P > 0.05, Fig. 2) and there was no difference in satisfaction scores between the groups (P > 0.05, Table 3). There was no significant difference in the rate of adverse effects between the groups (P > 0.05, Table 3).
Discussion
This study demonstrated that aprepitant combined with palonosetron did not reduce the incidence of PONV to a greater extent than palonosetron alone in the first 24 h after surgery in female patients receiving fentanyl IV-PCA for postoperative pain control.
Although the precise etiology of PONV is unknown, many risk factors are recognized, such as female sex, non-smoking status, history of PONV and/or motion sickness, use of volatile agents or nitrous oxide for anesthesia, use of postoperative opioids, and the duration and type of surgery [1]. Apfel et al. [19] reported four important independent risk factors: female sex, use of postoperative opioids, a history of PONV or motion sickness, and non-smoker status. Based on these four factors, a simplified risk score for predicting PONV was developed [19]. They suggested that the incidence of PONV increases to 10%, 20%, 40%, 60%, and 80% as the number of risk factors increases from 0 to 1, 2, 3, and 4, respectively. In this study, the risk factors were equivalent between the groups, with most patients having an Apfel’s risk score of 3 or 4, which is considered a high risk for PONV.
In patients at high risk for PONV, it is recommended that antiemetic therapy combining two or more distinct classes of agents should be used to target the various receptors responsible for PONV [1]. While all antiemetic interventions act via independent mechanisms, their combined action is additive [20]. The most widely used combinations for the prevention of PONV are 5-HT3 receptor antagonists combined with either dexamethasone, droperidol, or another antiemetic, and it has been shown that combination therapy is more effective than monotherapy [1,21].
Recently, combination therapies using aprepitant and 5-HT3 receptor antagonists for PONV prevention have been reported. Vallejo et al. [22] reported that aprepitant combined with ondansetron significantly decreased postoperative vomiting (from 29.7% to 9.3%) and nausea severity compared to ondansetron alone for up to 48 h postoperatively, even though the incidence of nausea was not significantly different. Trimas and Trimas [23] also reported improved immediate PONV when using 40 mg aprepitant with ondansetron compared to ondansetron alone (from 15.5% to 1.8%). Lee et al. [18] reported that compared to 0.3 mg ramosetron alone and combination therapy using 80 mg aprepitant plus 0.3 mg ramosetron significantly reduced the incidence of nausea and vomiting during the first 24 h postoperatively from 80.9% to 50% and 42.8% to 4.7%, respectively, in gynecological patients using fentanyl IV-PCA. This represented relative risk reductions of 38% for nausea and 89% for vomiting. Thus, the anti-vomiting effect of this combination was more robust than the anti-nausea effect.
It has been reported that palonosetron inhibits signaling cross-talk between the 5-HT3 and NK1 receptors: 5-HT3 receptor internalization by palonosetron alters signaling cross-talk between 5-HT3 and NK1 receptors, resulting in NK1 receptor internalization and NK1 receptor inhibition without direct binding to the NK1 receptor. In mechanistic studies using rodent-derived NG 108-15 cells, palonosetron and NK1 antagonists exerted an additive/synergic effect on substance-P-mediated inhibition. The authors suggested that the preventive effects of palonosetron and NK1 receptor antagonism on delayed emesis could be additive. However, these in vitro studies using rodent-derived cell models did not take into account species-specific differences in receptor locations and mechanisms of action. It is still unclear whether palonosetron’s preventive effect against substance P on NK1 receptors is enhanced or negated in humans [13,24,25].
In contrast, studies of CINV have reported greater NK1 receptor antagonism when using netupitant combined with palonosetron and dexamethasone [26,27]. Therefore, we postulated that the combination of aprepitant and palonosetron would offer superior protection against PONV as compared to palonosetron alone, similar to the results observed for aprepitant and ondansetron or ramosetron combinations. However, our results reveal that when combined with palonosetron, aprepitant unexpectedly did not reduce the incidence of PONV as compared to palonosetron alone.
We offer possible explanations for our unexpected results cautiously. First, the results may be related to our evaluation period. In the CINV study, acute emesis was largely associated with activation of 5-HT3 receptors by serotonin, while delayed emesis is thought to occur mainly through activation of NK1 receptors by substance P. In other words, serotonin is the dominant mediator in the acute phase, while substance P becomes the dominant mediator in the delayed phase [28]. Therefore, our negative result may be due to our study evaluating patients only for the first 24 h postoperatively. Furthermore, palonosetron in this period may have sufficient effect on the NK1 receptor to prevent PONV through 5-HT3/NK1 receptor cross-talk inhibition, resulting in masking of the effect of aprepitant on NK1 receptors.
One important result of our study is the finding that combination of aprepitant and palonosetron reduced the incidence of vomiting from 14% to 2% compared with palonosetron alone. This corresponds to an 86% relative reduction in the risk of vomiting during the first 24 h postoperatively. This is consistent with a previous finding by Lee et al. [18] of an 89% relative risk reduction for vomiting using aprepitant. Our results suggest that aprepitant does have an anti-vomiting effect, even though there was no statistical group difference due to the low incidence of vomiting even in the palonosetron alone group (P = 0.111).
One limitation of this study was its relatively short evaluation period. We investigated our study medications for only the first 24 h postoperatively, but aprepitant and palonosetron have demonstrated efficacy in preventing both acute and delayed emesis [13]. Therefore, further studies on the delayed effects of aprepitant combined with palonosetron for prevention of PONV for up to 48 h postoperatively are needed.
In conclusion, a combination of aprepitant and palonosetron did not reduce the incidence of PONV to a greater extent than did palonosetron alone in the first 24 h after surgery in female patients receiving fentanyl IV-PCA.
Acknowledgements
This study was supported by the Soonchunhyang University Research Fund.