Potential Investigation of Peceol for formulation of Ezetimibe self nano emulsifyingDrug Delivery Systems
Prashant Pp,Vaishali K,Santosh P +2 more
Reads0
Chats0
TLDR
In this article, a self-Nano emulsifying drug delivery system (SNEDDS) was proposed for ezetimibe and evaluated in vitro and in vivo potential.Abstract:
The present work was aimed at formulating and physicochemical characterization SNEDDS (self Nano emulsifying drug delivery system) of ezetimibe and evaluating its in vitro and in vivo potential. The solubility of both drugs was determined in excipient screening studies. Pseudoternary phase diagrams were used to evaluate the Nano emulsification existence area, composed of different surfactants, co surfactants, and oils at different surfactant to-cosurfactant (S/CoS) ratios, and the system exhibiting the largest percentage area of the self-Nano emulsifying region was selected and optimum oil ratio in the SNEDDS was selected by evaluating the clarity, precipitation and mean droplet size of the resultant Nanoemulsions. The release rate of ezetimibe was investigated using an in vitro dissolution test. In vitro dissolution studies showed that the SNEDDS composed of Peceol (20% wt/wt), Tween 80 (30% wt/wt), Ethanol (30% wt/wt), and ezetimibe (20% wt/wt) had higher initial dissolution rates for both drugs when compared with plain EZT. More importantly, EZT SNEDDS had a significantly increased dissolution profile in distilled water and pH 4.0 acetate buffer, implying enhanced bioavailability. The underlying mechanism of the loading capacity of EZT was elucidated by measurement of the zeta potential analysis. The results implied that EZT was located both in the Nanoemulsion core and the surfactant–cosurfactant layer. Comparative pharmacokinetic evaluation of EZT SNEDDS was investigated in terms of C max, tmax and AUC using rats. The SNEDDS formulation significantly increases pharmacokinetics parameter as compared with plain ezetimibe. The optimized formulation was then subjected to stability studies and was found to be stable over 6 months. Thus, the study confirmed that the SNEDDS formulation can be used as a possible alternative to traditional oral formulations of ezetimibe to improve its bioavailabilityread more
Citations
More filters
Journal ArticleDOI
Preparation, Optimization, and Evaluation of Hyaluronic Acid-Based Hydrogel Loaded with Miconazole Self-Nanoemulsion for the Treatment of Oral Thrush.
Khaled M. Hosny,Khaled M. Hosny,Hibah M. Aldawsari,Rahaf H. Bahmdan,Amal M. Sindi,Mallesh Kurakula,Majed Alrobaian,Ahmed Y. Aldryhim,Hala M. Alkhalidi,Hiba Bahmdan,Rasha A Khallaf,Amani M. El Sisi +11 more
TL;DR: Optimize MZ-NE hyaluronic acid-based oral gel demonstrated better antifungal activity, indicating its potential in oral thrush pharmacotherapy.
Journal ArticleDOI
Curcumin-loaded nanostructured lipid carriers prepared using Peceol™ and olive oil in photodynamic therapy: development and application in breast cancer cell line
TL;DR: CUR loading in NLCs enhanced its cell penetration and cytotoxic anticancer properties both in dark and in light conditions.
Journal ArticleDOI
A Solid Ultra Fine Self-Nanoemulsifying Drug Delivery System (S-SNEDDS) of Deferasirox for Improved Solubility: Optimization, Characterization, and In Vitro Cytotoxicity Studies.
TL;DR: The overall results indicated that the S-SNEDDS formulation of D FX could have the potential to enhance the solubility of DFX, which would in turn have the ability to improve its oral bioavailability as a safe novel delivery system.
Journal ArticleDOI
Nano-vesicular delivery system loaded by Bifonazole: Preparation, optimization, and assessment of pharmacokinetic and antifungal activity
TL;DR: BF-SNEDDS had enhanced anti-fungal pharmacotherapy and acts as a promising medium for transdermal delivery.
Journal ArticleDOI
Quality by Design Approach for the Development of Self-Emulsifying Systems for Oral Delivery of Febuxostat: Pharmacokinetic and Pharmacodynamic Evaluation
Nagarjun Rangaraj,Saurabh Shah,Maruthi A J,Sravanthi Reddy Pailla,Hanumanth Srikanth Cheruvu,D. Sujatha,Sunitha Sampathi +6 more
TL;DR: The developed formulation was found superior to pure FXT with enhanced oral bioavailability and anti-gout activity (with reduced uric acid levels), signifying a lipidic system being an efficacious substitute for gout treatment.
References
More filters
Journal ArticleDOI
Microemulsion-based media as novel drug delivery systems
M. Jayne Lawrence,Gareth D. Rees +1 more
TL;DR: The use of microemulsions and closely related microemulsion-based systems as drug delivery vehicles is reviewed, with particular emphasis being placed on recent developments and future directions.
Journal ArticleDOI
Formulation of self-emulsifying drug delivery systems
TL;DR: Self-emulsifying drug delivery systems (SEDDS) are mixtures of oils and surfactants, ideally isotropic, sometimes including cosolvents, which emulsify under conditions of gentle agitation, similar to those which would be encountered in the gastro-intestinal tract as discussed by the authors.
Journal ArticleDOI
Biopharmaceutical challenges associated with drugs with low aqueous solubility--the potential impact of lipid-based formulations.
TL;DR: The need for more examples of in vitro-in vivo correlations as a means of maximizing the development potential and commercial future for lipid-based formulations, and, promoting confidence within the industry for these delivery systems is highlighted.
Journal ArticleDOI
Preparation and in vivo evaluation of SMEDDS (self-microemulsifying drug delivery system) containing fenofibrate.
Ashok R. Patel,Pradeep R. Vavia +1 more
TL;DR: The study confirmed that the SMEDDS formulation can be used as a possible alternative to traditional oral formulations of fenofibrate to improve its bioavailability.
Journal ArticleDOI
A new solid self-microemulsifying formulation prepared by spray-drying to improve the oral bioavailability of poorly water soluble drugs
TL;DR: It is demonstrated that the solid SMEDDS may preserve an improved bioavailability with releasing microemulsion lipid droplets from the formulation in vivo, and may provide a useful solid dosage form for oral poorly water-soluble drugs.