Literature DB >> 10668859

Clinical pharmacokinetics of transdermal opioids: focus on transdermal fentanyl.

S Grond1, L Radbruch, K A Lehmann.   

Abstract

Transdermal delivery allows continuous systemic application of opioids through the intact skin. This review analyses the pharmacokinetic properties of transdermal opioid administration in the context of clinical experience, with a focus on fentanyl. A transdermal therapeutic system (TTS) for fentanyl has been developed. The amount of fentanyl released is proportional to the surface area of the TTS, which is available in different sizes. After the first application of a TTS, a fentanyl depot concentrates in the upper skin layers and it takes several hours until clinical effects are observed. The time from application to minimal effective and maximum serum concentrations is 1.2 to 40 hours and 12 to 48 hours, respectively. Steady state is reached on the third day, and can be maintained as long as patches are renewed. Within each 72-hour period, serum concentrations decrease gradually over the second and third days. When a TTS is removed, fentanyl continues to be absorbed into the systemic circulation from the cutaneous depot. The terminal half-life for TTS fentanyl is approximately 13 to 25 hours. The interindividual variability of serum concentrations, partly caused by different clearance rates, is markedly larger than the intraindividual variability. The effectiveness of TTS fentanyl was first demonstrated in acute postoperative pain. However, the slow pharmacokinetics and large variability of TTS fentanyl, together with the relatively short duration of postoperative pain, precluded adequate dose finding and led to inadequate pain relief or, especially, a high incidence of respiratory depression; such use is now contraindicated. Conversely, in cancer pain, TTS fentanyl offers an interesting alternative to oral morphine, and its effectiveness and tolerability in this indication has been demonstrated by a number of trials. Its usefulness in chronic pain of nonmalignant origin remains to be confirmed in controlled trials. In general, TTS fentanyl produces the same adverse effects as other opioids, mainly sedation, nausea, vomiting and constipation. In comparison with oral morphine, TTS fentanyl causes fewer gastrointestinal adverse events. The risk of hypoventilation is comparatively low in cancer patients. Sufentanil and buprenorphine may also be suitable for transdermal delivery, but clinical results are not yet available. Transdermal morphine is only useful if applied to de-epithelialised skin. However, iontophoresis may allow transdermal administration of opioids, including morphine, with a rapid achievement of steady state concentrations and the ability to adjust delivery rates. This would be beneficial for acute and/or breakthrough pain, and initial clinical trials are in progress.

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Year:  2000        PMID: 10668859     DOI: 10.2165/00003088-200038010-00004

Source DB:  PubMed          Journal:  Clin Pharmacokinet        ISSN: 0312-5963            Impact factor:   6.447


  127 in total

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Journal:  J Pain Symptom Manage       Date:  1997-05       Impact factor: 3.612

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9.  Electromotive administration of a new morphine formulation: morphine citrate.

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Journal:  Artif Organs       Date:  1994-06       Impact factor: 3.094

10.  The iontophoresis of fentanyl citrate in humans.

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  52 in total

1.  [Strong opioids and constipation].

Authors:  A Schwarzer; F Nauck; E Klaschik
Journal:  Schmerz       Date:  2005-06       Impact factor: 1.107

2.  Effect of transdermal opioids in experimentally induced superficial, deep and hyperalgesic pain.

Authors:  T Andresen; C Staahl; A Oksche; H Mansikka; L Arendt-Nielsen; A M Drewes
Journal:  Br J Pharmacol       Date:  2011-10       Impact factor: 8.739

3.  Skin pretreatment with an Er:YAG laser promotes the transdermal delivery of three narcotic analgesics.

Authors:  Woan-Ruoh Lee; Shing-Chuan Shen; Chia-Lang Fang; Ching-Ru Liu; Jia-You Fang
Journal:  Lasers Med Sci       Date:  2007-03-03       Impact factor: 3.161

Review 4.  Clinical pharmacology of analgesic medicines in older people: impact of frailty and cognitive impairment.

Authors:  Andrew J McLachlan; Sally Bath; Vasi Naganathan; Sarah N Hilmer; David G Le Couteur; Stephen J Gibson; Fiona M Blyth
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5.  Comparative study of the efficacy of transdermal buprenorphine patches and prolonged-release tramadol tablets for postoperative pain control after spinal fusion surgery: a prospective, randomized controlled non-inferiority trial.

Authors:  Ho-Joong Kim; Hyo Sae Ahn; Yunjin Nam; Bong-Soon Chang; Choon-Ki Lee; Jin S Yeom
Journal:  Eur Spine J       Date:  2017-07-20       Impact factor: 3.134

6.  Therapeutic dosage assessment based on population pharmacokinetics of a novel single-dose transdermal donepezil patch in healthy volunteers.

Authors:  Hee Youn Choi; Yo Han Kim; Donghyun Hong; Seong Su Kim; Kyun-Seop Bae; Hyeong-Seok Lim
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7.  The combined analgesic effect of gabapentin and transdermal fentanyl patch on acute and chronic pain after maxillary cancer surgeries.

Authors:  Satish Dhasmana; Vibha Singh; U S Pal
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8.  Effect of voriconazole and fluconazole on the pharmacokinetics of intravenous fentanyl.

Authors:  Teijo I Saari; Kari Laine; Mikko Neuvonen; Pertti J Neuvonen; Klaus T Olkkola
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9.  Assisted suicide by fentanyl intoxication due to excessive transdermal application.

Authors:  Martin Juebner; Mathias Fietzke; Justus Beike; Markus A Rothschild; Katja Bender
Journal:  Int J Legal Med       Date:  2014-02-28       Impact factor: 2.686

10.  Multicenter clinical study for evaluation of efficacy and safety of transdermal fentanyl matrix patch in treatment of moderate to severe cancer pain in 474 chinese cancer patients.

Authors:  Yu-Lin Zhu; Guo-Hong Song; Duan-Qi Liu; Xi Zhang; Kui-Feng Liu; Ai-Hua Zang; Ying Cheng; Guo-Chun Cao; Jun Liang; Xue-Zhen Ma; Xin Ding; Bin Wang; Wei-Lian Li; Zuo-Wei Hu; Gang Feng; Jiang-Jin Huang; Xiao Zheng; Shun-Chang Jiao; Rong Wu; Jun Ren
Journal:  Chin J Cancer Res       Date:  2011-12       Impact factor: 5.087

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