Abstract
Background For more than 60 years, the synthetic opioid fentanyl has been widely used in anaesthesia and analgesia. While the intravenous formulation is primarily used for general anaesthesia and intensive care settings, the drug's high lipophilic properties also allow various noninvasive routes of administration. Published data suggest that intranasal administration is also attractive for use as intranasal patient-controlled analgesia (PCA). A newly developed intranasal fentanyl formulation containing 47 μg fentanyl, intravenous fentanyl, and oral transmucosal fentanyl citrate were characterised, and bioavailability was compared to assess the suitability of the intranasal formulation for an intranasal PCA product. Methods 27 healthy volunteers were enrolled in a single-centre, open-label, randomised (order of treatments), single-dose study in a three-period crossover design. The pharmacokinetics of one intranasal puff of fentanyl formulation (47 μg, 140 mL per puff), one short intravenous infusion of 50 μg fentanyl, and one lozenge with an integrated applicator (200 μg fentanyl) were studied, and bioavailability was calculated. Blood samples were collected over 12 hours, and plasma concentrations of fentanyl were determined by HPLC with MS/MS detection. Results 24 volunteers completed the study. The geometric mean of AUC0-tlast was the highest with oral transmucosal administration (1106 h ∗ pg/ml, CV% = 32.86), followed by intravenous (672 h ∗ pg/ml, CV% = 32.18) and intranasal administration (515 h ∗ pg/ml, CV% = 30.10). Cmax was 886 pg/ml (CV% = 59.38) for intravenous, 338 pg/ml (CV% = 45.61) for intranasal, and 310 pg/ml (CV% = 29.58) for oral transmucosal administration. tmax was shortest for intravenous administration (0.06 h, SD = 0.056), followed by intranasal (0.21 h, SD = 0.078) and oral transmucosal administration (1.20 h, SD = 0.763). Dose-adjusted absolute bioavailability was determined to be 74.70% for the intranasal formulation and 41.25% for the oral transmucosal product. In total, 38 adverse events (AEs) occurred. Fourteen AEs were potentially related to the investigational items. No serious AE occurred. Conclusion Pharmacokinetic parameters and bioavailability of the investigated intranasal fentanyl indicated suitability for its intended use as an intranasal PCA option.
Highlights
Fentanyl has been used in anaesthesiology and analgesia for almost 60 years
Either fentanyl base or citrate salt is used for pharmaceutical formulations, whereby the base is virtually water-insoluble. e generally accepted explanation for the metabolisation of fentanyl is through N-dealkylation to norfentanyl by the cytochrome P450 (CYP) 3A4 [3,4,5], whereby none of the metabolites are considered to be pharmacologically active in a relevant manner [6]
First reported more than 30 years ago, there is no commercial patient-controlled analgesia (PCA) product available incorporating the advantages of intranasal fentanyl for postoperative pain management. e recently developed technical concept for intranasal administration incorporates features for safe postoperative pain management and might overcome the challenges previously faced [27]
Summary
Fentanyl has been used in anaesthesiology and analgesia for almost 60 years. First synthesised by Paul Janssen in the 1960s, it was introduced in anaesthesia and intensive care medicine as the first high potent μ-receptor agonist with an analgesic potency approximately 100 times higher than morphine [1]. Pharmacological developments over the last 20 years have led to new formulations and drug delivery technologies allowing the noninvasive administration of fentanyl. Such products offer individually adjusted titration and duration of action for a defined episode with a quick onset intended to treat chronic and acute pain states [9,10,11,12]. Intranasal administration of fentanyl has been systematically studied for use in postoperative pain management, in the context of intravenous patient-controlled analgesia (i.v. PCA). First reported more than 30 years ago, there is no commercial PCA product available incorporating the advantages of intranasal fentanyl for postoperative pain management. E objective of this study was to investigate and compare the bioavailability of the new formulation containing 47 μg fentanyl (74 μg fentanyl citrate) and 0.1% sodium hyaluronate (added for better tolerability) in 140 μl per spray puff with intravenous and oral transmucosal administration through a three-way crossover study in 24 healthy subjects
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