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First‐pass elimination of lidocaine in the rabbit after peroral and rectal route of administration
Author(s) -
Ritschel W. A.,
Elconin H.,
Alcorn G. J.,
Denson D. D.
Publication year - 1985
Publication title -
biopharmaceutics and drug disposition
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.419
H-Index - 58
eISSN - 1099-081X
pISSN - 0142-2782
DOI - 10.1002/bdd.2510060303
Subject(s) - bioavailability , rectal administration , lidocaine , first pass effect , pharmacology , systemic circulation , medicine , pharmacokinetics , dosage form , absorption (acoustics) , drug , oral administration , route of administration , anesthesia , physics , acoustics
Lidocaine shows pronounced first‐pass metabolism upon peroral administration in man (about 30 per cent peroral bioavailability). Since the rectal bioavailability is about 65 per cent in man it is assumed that some drug is directly absorbed into systemic circulation by‐passing the liver. In rats peroral bioavailability is about 8 per cent whereas rectal bioavailability is about 100 per cent. This indicates that the rat is not a suitable model to study rectal lidocaine dosage forms. The purpose of this study was to investigate lidocaine disposition and bioavailability in rabbits after peroral and rectal administration. The peroral bioavailability in rabbits was found to be about 6 per cent and the rectal bioavailability is about 33 per cent. The results indicate that the rabbit is a suitable model for the study of systemic absorption of rectal lidocaine dosage forms.