Literature DB >> 24700272

Rapid delivery of diazepam from supersaturated solutions prepared using prodrug/enzyme mixtures: toward intranasal treatment of seizure emergencies.

Mamta Kapoor1, Tate Winter, Lev Lis, Gunda I Georg, Ronald A Siegel.   

Abstract

Current treatments for seizure emergencies, such as status epilepticus, include intravenous or rectal administration of benzodiazepines. While intranasal delivery of these drugs is desirable, the small volume of the nasal cavity and low drug solubility pose significant difficulties. Here, we prepared supersaturated diazepam solutions under physiological conditions and without precipitation, using a prodrug/enzyme system. Avizafone, a peptide prodrug of diazepam, was delivered with--Aspergillus oryzae (A.O.) protease, an enzyme identified from a pool of hydrolytic enzymes in assay buffer, pH 7.4 at 32°C. This enzyme converted avizafone to diazepam at supersaturated concentrations. In vitro permeability studies were performed at various prodrug/enzyme ratios using Madin-Darby canine kidney II-wild type (MDCKII-wt) monolayers, a representative model of the nasal epithelium. Monolayer integrity was examined using TEER measurement and the lucifer yellow permeability assay. Prodrug/drug concentrations were measured using HPLC. Enzyme kinetics with avizafone-protease mixtures revealed K(M) = 1,501 ± 232 μM and V(max) = 1,369 ± 94 μM/s. Prodrug-protease mixtures, when co-delivered apically onto MDCKII-wt monolayers, showed 2-17.6-fold greater diazepam flux (S = 1.3-15.3) compared to near-saturated diazepam (S = 0.7). Data for prodrug conversion upstream (apical side) and drug permeability downstream (basolateral side) fitted reasonably well to a previously developed in vitro two compartment pharmacokinetic model. Avizafone-protease mixtures resulted in supersaturated diazepam in less than 5 min, with the rate and extent of supersaturation determined by the prodrug/enzyme ratio. Together, these results suggest that an intranasal avizafone-protease system may provide a rapid and alternative means of diazepam delivery.

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Year:  2014        PMID: 24700272      PMCID: PMC4012037          DOI: 10.1208/s12248-014-9596-5

Source DB:  PubMed          Journal:  AAPS J        ISSN: 1550-7416            Impact factor:   4.009


  22 in total

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3.  Acid hydrolysis of diazepam. Kinetic study of the reactions of 2-(N-methylamino)-5-chlorobenzophenone, with HCl in MeOH-H2O.

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5.  Preparation of carbamazepine-Soluplus solid dispersions by hot-melt extrusion, and prediction of drug-polymer miscibility by thermodynamic model fitting.

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6.  Pharmacokinetics and tolerability of intranasal diazepam and midazolam in healthy adult volunteers.

Authors:  V D Ivaturi; J R Riss; R L Kriel; J C Cloyd
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7.  Enhanced permeation of diazepam through artificial membranes from supersaturated solutions.

Authors:  Hao Hou; Ronald A Siegel
Journal:  J Pharm Sci       Date:  2006-04       Impact factor: 3.534

8.  Characterization of curcumin-PVP solid dispersion obtained by spray drying.

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Review 9.  Management of status epilepticus.

Authors:  Joseph I Sirven; Elizabeth Waterhouse
Journal:  Am Fam Physician       Date:  2003-08-01       Impact factor: 3.292

10.  Treatment of Convulsive and Nonconvulsive Status Epilepticus.

Authors:  Trudy Pang; Lawrence J Hirsch
Journal:  Curr Treat Options Neurol       Date:  2005-07       Impact factor: 3.972

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  1 in total

1.  Intranasal Coadministration of a Diazepam Prodrug with a Converting Enzyme Results in Rapid Absorption of Diazepam in Rats.

Authors:  Davin Rautiola; Patricia D Maglalang; Narsihmulu Cheryala; Kathryn M Nelson; Gunda I Georg; Jared M Fine; Aleta L Svitak; Katherine A Faltesek; Leah R Hanson; Usha Mishra; Lisa D Coles; James C Cloyd; Ronald A Siegel
Journal:  J Pharmacol Exp Ther       Date:  2019-03-05       Impact factor: 4.030

  1 in total

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