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Vol. 301, Issue 1, 391-400, April 2002
West Pharmaceutical Services, Drug Delivery and Clinical Research
Centre Ltd., Albert Einstein Centre, Nottingham Science and Technology
Park, Nottingham, United Kingdom
Morphine administered nasally to humans as a simple solution is only
absorbed to a limited degree, with a bioavailability of the order of
10% compared with intravenous administration. This article describes
the development of novel nasal morphine formulations based on chitosan,
which, in the sheep model, provide a highly increased absorption with a
5- to 6-fold increase in bioavailability over simple morphine
solutions. The chitosan-morphine nasal formulations have been tested in
healthy volunteers in comparison with a slow i.v. infusion (over 30 min) of morphine. The results show that the nasal formulation was
rapidly absorbed with a Tmax of 15 min or
less and a bioavailability of nearly 60%. The shape of the plasma
profile for nasal delivery of the chitosan-morphine formulation was
similar to the one obtained for the slow i.v. administration of
morphine. Furthermore, the metabolite profile obtained after the nasal
administration of the chitosan-morphine nasal formulation was
essentially identical to the one obtained for morphine administered by
the intravenous route. The levels of both morphine-6-glucuronide and
morphine-3-glucuronide were only about 25% of that found after
oral administration of morphine. It is concluded that a properly
designed nasal morphine formulation (such as one with chitosan) can
result in a noninjectable opioid product capable of offering patients
rapid and efficient pain relief.
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