Dipivefrin hydrochloride ophthalmic gel was prepared and the release test and the isolated cornea permeation test of the formulation in vitro were investigated. The release test of the formulation was studied by using...Dipivefrin hydrochloride ophthalmic gel was prepared and the release test and the isolated cornea permeation test of the formulation in vitro were investigated. The release test of the formulation was studied by using permeable membrane. The content and the release amount of Dipivefrin hydrochloride from the gel base were measured by high performance liquid chromatography. The cornea permeation test of the formulation was studied by using isolated rabbit corneas. The formulation release behavior in vitro followed the first-order kinetic equation. The release amount of Dipivefrin hydrochloride raised significantly with less polymer in the formulation. The cornea permeation behavior of the drug in vitro followed the first-order kinetic equation. The eye irritancy of Dipivefrin hydrochloride gel is lower than that of eyedrops.展开更多
The clinical pharmacokinetics of osmotic pump controlled release tablets of terazosin hydrochloride in healthy volunteers was studied.A sensitive and rapid HPLC method was used to determine the terazosin plasma concen...The clinical pharmacokinetics of osmotic pump controlled release tablets of terazosin hydrochloride in healthy volunteers was studied.A sensitive and rapid HPLC method was used to determine the terazosin plasma concentrations,and single and multiple doses of terazosin hydrochloride regular tablets(reference tablets)and osmotic pump controlled release tablets were orally administrated in randomized crossover design.The results showed that the C_(max)of the reference tablets after single oral dose((120.56±23.15)ng/mL)in 20 healthy volunteers was significantly higher than that of controlled release tablets ((95.27±16.35)ng/mL).The T_(max)of the controlled release tablets((2.65±0.82)h)was significantly longer than that of reference tablets((1.27±0.61)h)(P0.05).The relative bioavailability of the controlled release tablets was found to be(105.85±6.12)%. The multiple oral dose pharmacokinetic parameters of the regular tablets and controlled release tablets were as follows:AUC_(SS) were(1275.17±175.35)and(1382.65±205.31)ng·h/mL respectively,C_(max)were(128.15±22.37)and(98.57±18.16)ng/mL respectively,T_(max)were(1.35±0.71)and(2.76±0.85)h respectively,C_(av)were(53.13±9.12)and(57.61±9.25)ng/mL respectively, and DF were(2.25±0.26)%and(1.62±0.25)%respectively.The relative bioavailability of the controlled release tablets to the reference tablets was(108.43±6.26)%.The controlled release tablet of terazosin hydrochloride was bioequivalent to the reference tablet.The controlled release tablet exhibited a sustained-release property with a significantly longer T_(max)and lower C_(max).展开更多
文摘Dipivefrin hydrochloride ophthalmic gel was prepared and the release test and the isolated cornea permeation test of the formulation in vitro were investigated. The release test of the formulation was studied by using permeable membrane. The content and the release amount of Dipivefrin hydrochloride from the gel base were measured by high performance liquid chromatography. The cornea permeation test of the formulation was studied by using isolated rabbit corneas. The formulation release behavior in vitro followed the first-order kinetic equation. The release amount of Dipivefrin hydrochloride raised significantly with less polymer in the formulation. The cornea permeation behavior of the drug in vitro followed the first-order kinetic equation. The eye irritancy of Dipivefrin hydrochloride gel is lower than that of eyedrops.
文摘The clinical pharmacokinetics of osmotic pump controlled release tablets of terazosin hydrochloride in healthy volunteers was studied.A sensitive and rapid HPLC method was used to determine the terazosin plasma concentrations,and single and multiple doses of terazosin hydrochloride regular tablets(reference tablets)and osmotic pump controlled release tablets were orally administrated in randomized crossover design.The results showed that the C_(max)of the reference tablets after single oral dose((120.56±23.15)ng/mL)in 20 healthy volunteers was significantly higher than that of controlled release tablets ((95.27±16.35)ng/mL).The T_(max)of the controlled release tablets((2.65±0.82)h)was significantly longer than that of reference tablets((1.27±0.61)h)(P0.05).The relative bioavailability of the controlled release tablets was found to be(105.85±6.12)%. The multiple oral dose pharmacokinetic parameters of the regular tablets and controlled release tablets were as follows:AUC_(SS) were(1275.17±175.35)and(1382.65±205.31)ng·h/mL respectively,C_(max)were(128.15±22.37)and(98.57±18.16)ng/mL respectively,T_(max)were(1.35±0.71)and(2.76±0.85)h respectively,C_(av)were(53.13±9.12)and(57.61±9.25)ng/mL respectively, and DF were(2.25±0.26)%and(1.62±0.25)%respectively.The relative bioavailability of the controlled release tablets to the reference tablets was(108.43±6.26)%.The controlled release tablet of terazosin hydrochloride was bioequivalent to the reference tablet.The controlled release tablet exhibited a sustained-release property with a significantly longer T_(max)and lower C_(max).
