Sublingual absorption of selected opioid analgesics

David S. Weinberg, Charles E. Inturrisi, Bruce Reidenberg, Dwight E. Moulin, Tony J. Tip, Stanley Wallenstein, Raymond W. Houde, Kathleen M. Foley

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228 Scopus citations

Abstract

Ongoing interest in the improvement of pain management with opioid analgesics has led to the investigation of sublingual opioid absorption. The present report determined the percent absorption of selected opioid analgesics from the oral cavity of normal subjects under conditions of controlled pH and swallowing when a l.0 ml aliquot of the test drug was placed under the tongue for a 10-minute period. Compared with morphine sulfate at pH 6.5 (18% absorption), buprenorphine C55%), fentanyl C51%), and methadone C34%) were absorbed to a significantly greater extent (p < 0.05), whereas levorphanol, hydromorphone, oxycodone, heroin, and the opioid antagonist naloxone were not. Overall, lipophilic drugs were better absorbed than were hydrophilic drugs. Plasma morphine concentration-time profiles indicate that the apparent sublingual bioavailability of morphine is only 9.0% ± 11.9% (SD) of that after intramuscular administration. In the same subjects the estimated sublingual absorption was 22.4% ± 9.2% (SD), indicating that the sublingual absorption method may overestimate apparent bioavailability. When the oral cavity was buffered to pH 8.5, methadone absorption was increased to 75%. Thus, an alkaline pH microenvironment that favors the unionized fraction of opioids increased sublingual drug absorption. Although absorption was found to be independent of drug concentration, it was contact time dependent. for methadone and fentanyl but not for buprenorphine. These results indicate that although the sublingual absorption and apparent sublingual bioavailability of morphine are poor, the sublingual absorption of methadone, fentanyl, and buprenorphine under controlled conditions is relatively high.

Original languageEnglish
Pages (from-to)335-342
Number of pages8
JournalClinical Pharmacology and Therapeutics
Volume44
Issue number3
DOIs
StatePublished - Sep 1988
Externally publishedYes

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