Clinical Pharmacokinetics of Alfentanil, Fentanyl and Sufentanil

Scholz, Jens; Steinfath, Markus; Schulz, Martin

doi:10.2165/00003088-199631040-00004

Cited by 239 publications

(139 citation statements)

References 107 publications

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“…Cardiopulmonary bypass significantly changes the pharmacokinetics of opioids in human patients (Scholz et al 1996). This is due to altered distribution volumes (secondary to priming of the ECC), acid-base, organ blood flow, plasma protein concentration and body temperature alterations (Gedney & Ghosh 1995).…”

Section: Laboratory Animals (2005) 39mentioning

confidence: 99%

Prolonged recovery and respiratory depression after fentanyl infusion in a sheep undergoing mitral valve reconstruction

et al. 2005

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SummaryA sheep was anaesthetized for implantation of a novel device (MitroFast s ) to replace the posterior leaflet of the mitral valve. Anaesthetic management included a balanced anaesthetic protocol and consisted of propofol or isoflurane combined with fentanyl infusion (0.15-0.4 mg/kg/min). Deliberate hypothermia during cardiopulmonary bypass was set at 34.5-35.51C. Surgery proceeded uneventfully. Total time of aortic cross-clamping was 35 min and total time on extracorporeal circulation was 60 min. Visual inspection, intracardiac pressure testing and transesophageal echocardiography indicated proper functioning of the device. The anaesthetic period was uneventful, but recovery was prolonged with central nervous and respiratory depression and marked hypoxaemia. Administration of naloxone (1.5 mg/kg, repeated twice at 15-20 min intervals) reversed the central nervous and attenuated the respiratory depressions. An initially low rate of urine production normalized after rewarming and a single intravenous administration of furosemide.

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Section: Laboratory Animals (2005) 39mentioning

confidence: 99%

Prolonged recovery and respiratory depression after fentanyl infusion in a sheep undergoing mitral valve reconstruction

et al. 2005

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“…However, the use of NSAIDs alone can be insufficient to adequately alleviate serve pain in conditions such as orthopedic diseases. On the other hand, fentanyl is a synthetic -opioid receptor agonist of the 4-anilinopiperidine series that is commonly used as an analgesic for moderate to serve pain in a number of species [17]. In humans and small animals, balanced anesthesia with fentanyl provides perioperative analgesia and improves hemodynamics by minimizing the necessary inhalation concentration of anesthetic agents for general anesthesia [11,12,23].…”

mentioning

confidence: 99%

Effects of Intravenous Fentanyl Administration on End-Tidal Sevoflurane Concentrations in Thoroughbred Racehorses undergoing Orthopedic Surgery

Ohta

Wakuno

Okada

et al. 2010

The Journal of Veterinary Medical Science

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ABSTRACT. To evaluate the effects of IV fentanyl administration on the end-tidal sevoflurane concentration (ET SEVO ) in thoroughbred racehorses, the ET SEVO required for internal fixation of longitudinal fractures was compared between horses anesthetized with sevofluranefentanyl (Group SF; n=9) and those anesthetized with sevoflurane alone (Group S; n=9). The loading dose of fentanyl (5.0 g/kg) was administered over 15 min followed by a maintenance dose of fentanyl (0.1 g/kg/min) throughout the operation in Group SF. The mean ET SEVO during the operation in Group SF (2.6  0.2%) was significantly lower than in Group S (3.0  0.3%). The plasma fentanyl concentrations (6.12  0.88 to 7.78  1.12 ng/ml) in 7 out of 9 horses in Group SF were stable and did not change significantly throughout the operation. The mean dobutamine infusion rate required for maintaining a mean arterial blood pressure between 60 and 80 mmHg during the operation in Group SF (0.56  0.30 g/kg/min) was significantly lower than in Group S (0.90  0.16 g/kg/min). The qualities of the recoveries were clinically acceptable, and serious complications were not observed in either group. In conclusion, continuous IV fentanyl administration reduced the sevoflurane requirement by 13% in thoroughbred racehorses undergoing orthopedic surgery; however, fentanyl was considered to be less effective in horses compared with other species.

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“…Alfentanil is a synthetic opioid used for the induction of surgical anesthesia and the management of postsurgical pain. The alfentanil dose needs to be individualized based on numerous factors, including pathological condition, use of other medicines, and the type and duration of the surgical procedure (Scholz et al, 1996). Because alfentanil is a CYP3A4 substrate, CYP3A4 activity is another important determinant of the required alfentanil dose (Kharasch and Thummel, 1993).…”

mentioning

confidence: 99%

Pharmacokinetics and Pharmacodynamics of Alfentanil in P-Glycoprotein-Competent and P-Glycoprotein-Deficient Mice: P-Glycoprotein Efflux Alters Alfentanil Brain Disposition and Antinociception

Kalvass

Olson²,

Pollack³

2006

Drug Metab Dispos

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ABSTRACT:Previous studies have indicated that P-glycoprotein (P-gp) attenuates the central nervous system penetration and central activity of some opioids. The impact of P-gp-mediated efflux on the disposition and efficacy of the synthetic opioid alfentanil currently is unknown. In this study, P-gp-competent [mdr1a(؉/؉)] and P-gpdeficient [mdr1a(؊/؊)] mice were used to investigate the impact of P-gp-mediated efflux on the systemic pharmacokinetics, brain disposition, and central activity of alfentanil. Equipotent doses of alfentanil were administered to mdr1a(؉/؉) and mdr1a(؊/؊) mice (0.2 and 0.067 mg/kg, respectively), and the time course of brain and serum concentrations as well as antinociception were determined. A pharmacokinetic-pharmacodynamic (PK-PD) model was fit to the data and used to assess the impact of P-gp on parameters associated with alfentanil disposition and action. The mdr1a(؉/؉) mice were less sensitive to alfentanil than mdr1a(؊/؊) mice, requiring a 3-fold higher dose to produce similar antinociception. PK-PD modeling revealed no differences in alfentanil systemic pharmacokinetics between P-gp expressers and nonexpressers. However, the steady-state brain-to-serum concentration ratio (K p,brain,ss ) was ϳ3-fold lower in mdr1a(؉/؉) mice compared with mdr1a(؊/؊) mice (0.19 ؎ 0.01 versus 0.54 ؎ 0.04, respectively). Consistent with the ϳ3-fold lower K p,brain,ss , the antinociception versus serum concentration relationship in mdr1a(؉/؉) mice was shifted ϳ3-fold rightward compared with mdr1a(؊/؊) mice. However, there was no difference in the antinociception versus brain concentration relationship, or in the brain tissue EC 50 (11 ؎ 1.8 versus 9.2 ؎ 1.7 ng/g), between mdr1a(؉/؉) and mdr1a(؊/؊) mice. These results indicate that alfentanil is an in vivo P-gp substrate and are consistent with the hypothesis that P-gp-mediated efflux attenuates antinociception by reducing alfentanil K p,brain,ss .

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Clinical Pharmacokinetics of Alfentanil, Fentanyl and Sufentanil

Cited by 239 publications

References 107 publications

Prolonged recovery and respiratory depression after fentanyl infusion in a sheep undergoing mitral valve reconstruction

Prolonged recovery and respiratory depression after fentanyl infusion in a sheep undergoing mitral valve reconstruction

Effects of Intravenous Fentanyl Administration on End-Tidal Sevoflurane Concentrations in Thoroughbred Racehorses undergoing Orthopedic Surgery

Pharmacokinetics and Pharmacodynamics of Alfentanil in P-Glycoprotein-Competent and P-Glycoprotein-Deficient Mice: P-Glycoprotein Efflux Alters Alfentanil Brain Disposition and Antinociception

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