Aqueous Solubility Enhancement of Mirtazapine: Effect of Cosolvent and Surfactant

Ezealisiji, Kenneth E.; Mbah, Chika J; Osadebe, PO

doi:10.4236/pp.2015.610049

Cited by 9 publications

(7 citation statements)

References 12 publications

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“…There were no significant differences in the solubility of PR in various pH condition and ethanol concentrations between 48 and 72 h, displayed no noticeable differences, which indicated that the solubility of PR had reached equilibrium. The low water solubility of PR may be due to the inability of water, to break into the lattice structure of PR [19]. On the other hand, when the co-solvent systems were used, the PR solubility increased when the ethanol concentration increased.…”

Section: Discussionmentioning

confidence: 99%

Enhanced stability of phenylethyl resorcinol in elastic vesicular formulations

Limsuwan¹,

Boonme²,

Amnuaikit³

2019

Trop. J. Pharm Res

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Purpose: To enhance the stability and reduce photo-degradation of phenylethyl resorcinol (PR) by elastic vesicle formation. Methods: PR solution was stored at different temperatures, pH conditions, and under protected and unprotected natural light. The color of the solution and total active content were investigated. Three types of elastic vesicles, viz, ethosomes, transfersomes and invasomes, were prepared and their sedimentation in formulations and total active content were investigated before and after storage under various conditions for 4 months. The stability of the solutions and vesicular formulations were assessed. Results: PR solution was unstable at pH 9, higher temperature (70 ± 1 o C) and under natural light. The color of PR solution changed from colorless to orange tone and the PR content decreased. On the other hand, PR entrapped within ethosome, tranfersome and invasome vesicles showed better stability, color change was not observed in the formulations, and PR content remained > 90 %. Conclusion: All the vesicles display reduced degradation of PR under thermal and natural light. Thus, PR vesicular formulation enhances stability and improves the quality of the product for use in topical administration.

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Section: Discussionmentioning

confidence: 99%

Enhanced stability of phenylethyl resorcinol in elastic vesicular formulations

Limsuwan¹,

Boonme²,

Amnuaikit³

2019

Trop. J. Pharm Res

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“…The samples were agitated for 48 hours at 37 ± 1 °C in an incubator shaker. The solution was passed through a 0.45 μm Millipore filter, and the drug concentration was evaluated by UV- Vis spectrophotometer at λ max 293 nm (K. E. Ezealisiji et al., 2015 ).…”

Section: Methodsmentioning

confidence: 99%

“…Additionally, it has a low bioavailability of about 50%. It was estimated that increasing its water solubility might result in increased bioavailability and reduce the dose required to achieve the desired therapeutic effect (K. E. Ezealisiji et al., 2015 ).…”

Section: Introductionmentioning

confidence: 99%

Optimization of mirtazapine loaded into mesoporous silica nanostructures via Box-Behnken design: in-vitro characterization and in-vivo assessment

et al. 2022

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Employment of mesoporous silica nanostructures (MSNs) in the drug delivery field has shown a significant potential for improving the oral delivery of active pharmaceutical products with low solubility in water. Mirtazapine (MRT) is a tetracyclic antidepressant with poor water solubility (BCS Class II), which was recently approved as a potent drug used to treat severe depression. The principle of this research is to optimize the incorporation of Mirtazapine into MSNs to improve its aqueous solubility, loading efficiency, release performance, and subsequent bioavailability. The formulation was optimized by using of Box-Behnken Design, which allows simultaneous estimation of the impact of different types of silica (SBA-15, MCM-41, and Aluminate-MCM-41), a different drug to silica ratios (33.33%, 49.99%, and 66.66%), and different drug loading procedures (Incipient wetness, solvent evaporation, and solvent impregnation) on the MRT loading efficiency, aqueous solubility and dissolution rate. The optimized formula was achieved by loading MRT into SBA-15 at 33.33% drug ratio prepared by the incipient wetness method, which displayed a loading efficiency of 104.05%, water solubility of 0.2 mg/ml, and 100% dissolution rate after 30 min. The pharmacokinetic profile of the optimized formula was obtained by conducting the in -vivo study in rabbits which showed a marked improvement (2.14-fold) in oral bioavailability greater than plain MRT. The physicochemical parameters and morphology of the optimized formula were characterized by; gas adsorption manometry, scanning electron microscopy (SEM), polarized light microscopy (PLM), Fourier-transform infrared spectroscopy (FT-IR), differential scanning calorimetry (DSC), and X-ray powder diffraction (XRPD).

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“…This indicates a high hydrophobicity, but it does dissolve in ethanol and an acidic condition. The MTZ has a low bioavailability (50%), high protein-binding (85%), and a long half-life (20-40 h) [4]. MTZ has a relatively narrow therapeutic index and should be individually optimized to obtain a therapeutic effect [5].…”

Section: Introductionmentioning

confidence: 99%

Fabrication of Hydroxypropyl Methylcellulose Orodispersible Film Loaded Mirtazapine Using a Syringe Extrusion 3D Printer

et al. 2022

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Depression is a mental illness causing a continuous negative feeling and loss of interest and affects physical and mental health. Mirtazapine (MTZ) is an effective medicine for treating depression, but patients lack compliance. However, transforming a pharmaceutical dosage form to an orodispersible film (ODF) could resolve this issue. This study aims to fabricate ODF-loading mirtazapine, using a syringe extrusion 3D printer, and compare its properties with the solvent-casting method. The ODFs were prepared by dissolving the mirtazapine in a hydroxypropyl methylcellulose E15 solution, and then fabricated by a 3D printer or casting. The 3D printing was accurate and precise in fabricating the ODFs. The SEM micrographs showed that the mirtazapine-printed ODF (3D-MTZ) was porous, with crystals of mirtazapine on the film’s surface. The 3D-MTZ exhibited better mechanical properties than the mirtazapine-casted ODF (C-MTZ), due to the 3D-printing process. The disintegration time of the 3D-MTZ in a simulated salivary fluid, pH 6.8 at 37 °C, was 24.38 s, which is faster than the C-MTZ (46.75 s). The in vitro dissolution study, in 0.1 N HCl at 37 °C, found the 3D-MTZ quickly released the drug by more than 80% in 5 min. This study manifested that 3D-printing technology can potentially be applied for the fabrication of ODF-containing mirtazapine.

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Aqueous Solubility Enhancement of Mirtazapine: Effect of Cosolvent and Surfactant

Cited by 9 publications

References 12 publications

Enhanced stability of phenylethyl resorcinol in elastic vesicular formulations

Enhanced stability of phenylethyl resorcinol in elastic vesicular formulations

Optimization of mirtazapine loaded into mesoporous silica nanostructures via Box-Behnken design: in-vitro characterization and in-vivo assessment

Fabrication of Hydroxypropyl Methylcellulose Orodispersible Film Loaded Mirtazapine Using a Syringe Extrusion 3D Printer

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