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Improving the ocular absorption of phenylephrine

✍ Scribed by D. S. Chien; R. D. Schoenwald


Publisher
John Wiley and Sons
Year
1986
Tongue
English
Weight
416 KB
Volume
7
Category
Article
ISSN
0142-2782

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✦ Synopsis


An oxazolidine prodrug of phenylephrine and the base form of phenylephrine were synthesized, suspended in sesame oil, and tested for mydriatic activity against phenylephrine HCI. The HCI salt was formulated as a viscous aqueous solution and as a sesame oil suspension. A dosing volume of 10 pl was instilled into rabbit eyes and the pupillary diameter was measured over time. A 0.045M prodrug suspension was judged equal in mydriatic activity to a 0.45 M viscous solution of phenylephrine HCI with the exception that the time of maximum response occurred 60 min earlier with the prodrug.

When phenylephrine base was suspended in sesame oil at 0.045. 0.12, and 0 4 M . the mydriatic activity was also greater than equimolar suspensions of phenylephrine HCI. The p H of tear fluids was also measured over time and found to rise 1.1, 0.70. and 0.30pH units for 045, 0.12, and 0.045M suspensions of the base form but remain unchanged when phenylephrine HCI was instilled in the rabbit eye. The greater activity associated with the base form of phenylephrine was judged a result of the change in p H to favour the absorption of phenylephrine. This latter approach should be applicable to either weak acids or weak bases with pK, values outside of the normal p H range (7-8) of the tears and in concentrations greater than 0.045 M suspended in a non-aqueous vehicle.


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