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Solid Formulation of a Supersaturable Self-microemulsifying Drug Delivery System for Valsartan with Improved Dissolution and Bioavailability

Overview
Journal Oncotarget
Specialty Oncology
Date 2017 Dec 8
PMID 29212229
Citations 11
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Abstract

In order to improve the dissolution and oral bioavailability of valsartan (VST), and reduce the required volume for treatment, we previously formulated a supersaturable self-microemulsifying drug delivery system (SuSMEDDS) composed of VST (80 mg), Capmul MCM (13.2 mg), Tween 80 (59.2 mg), Transcutol P (59.2 mg), and Poloxamer 407 (13.2 mg). In the present study, by using Florite PS-10 (119.1 mg) and Vivapur 105 (105.6 mg) as solid carriers, VST-loaded solidified SuSMEDDS (S-SuSMEDDS) granules were successfully developed, which possessed good flow properties and rapid drug dissolution. By introducing croscarmellose sodium (31 mg) as a superdisintegrant, S-SuSMEDDS tablets were also successfully formulated, which showed fast disintegration and high dissolution efficiency. Preparation of granules and tablets was successfully optimized using D-optimal mixture design and 3-level factorial design, respectively, resulting in percentage prediction errors of <10%. In pharmacokinetic studies in rats, the relative bioavailability of the optimized granules was 107% and 222% of values obtained for SuSMEDDS and Diovan powder, respectively. Therefore, we conclude that novel S-SuSMEDDS formulations offer great potential for developing solid dosage forms of a liquefied formulation such as SuSMEDDS, while improving oral absorption of drugs with poor water solubility.

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