Formulation of Intranasal Mucoadhesive Thermotriggered In Situ Gel Containing Mirtazapine as an Antidepressant Drug.
Mohammed Y GhazwaniRajalakshimi VasudevanGeetha KandasamyNaredla ManusriPraveen DevanandanRanadheer Chowdary PuvvadaVinoth Prabhu VeeramaniPremalatha PaulsamyKrishnaraju VenkatesanKumarappan ChidmabaramRajeshri DhurkePublished in: Gels (Basel, Switzerland) (2023)
The purpose of the present work was to develop nanoemulsion-based formulations of mirtazapine for intranasal delivery using a spray actuator to target the brain for treating depression. Research on the solubility of medications in different oils, surfactants, co-surfactants, and solvents has been done. Using pseudo-ternary phase diagrams, the various ratios of the surfactant and co-surfactant mix were computed. Thermotriggered nanoemulsion was formulated using different concentrations of poloxamer 407 (i.e., 15%, 15.5%, 16%, 16.5% up to 22%). Similarly, mucoadhesive nanoemulsion using 0.1% Carbopol and water-based plain nanoemulsions were also prepared for comparative assessment. The developed nanoemulsions were analyzed for physicochemical properties, i.e., physical appearance, pH, viscosity, and drug content. Drug-excipient incompatibility was determined by Fourier transform infrared spectral (FTIR) analysis and differential scanning calorimetry (DSC). In vitro drug diffusion studies were conducted for optimized formulations. Among the three formulations, RD1 showed the highest percentage of drug release. Ex vivo drug diffusion studies were conducted on freshly excised sheep nasal mucosa with Franz diffusion cell simulated nasal fluid (SNF) for all three formulations up to 6 h, and the thermotriggered nanoemulsion (RD1) showed 71.42% drug release with 42.64 nm particle size and a poly dispersity index of 0.354. The zeta potential was found to be -6.58. Based on the above data, it was concluded that thermotriggered nanoemulsion (RD1) has great potential to be used as an intranasal gel for treating depression in patients. It can offer great benefits by reducing dosing frequency and improving bioavailability of mirtazapine by direct nose-to-brain delivery.
Keyphrases
- drug release
- drug delivery
- adverse drug
- white matter
- depressive symptoms
- end stage renal disease
- newly diagnosed
- ejection fraction
- multiple sclerosis
- mental health
- optical coherence tomography
- resting state
- photodynamic therapy
- magnetic resonance
- human health
- magnetic resonance imaging
- cell therapy
- cerebral ischemia
- blood brain barrier
- bipolar disorder
- patient reported outcomes
- wound healing
- data analysis