<i>In vivo</i> nose-to-brain delivery of the hydrophilic antiviral ribavirin by microparticle agglomerates

Giuliani, Alessandro; Balducci, AG; Zironi, Elisa; Colombo, Gaia; Bortolotti, Fabrizio; Lorenzini, Luca; Galligioni,; Pagliuca, Giampiero; Scagliarini, Alessandra; Calzà, Laura; Sonvico, Fabio

doi:10.1080/10717544.2018.1428242

Cited by 61 publications

(36 citation statements)

References 67 publications

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“…Chitosan has previously been utilised as a release modulator and PE for an array of biological membranes including buccal tissue (Duttagupta, Jadhav et al 2015, Kontogiannidou, Andreadis et al 2017, intestinal tissue (Chougule, Patel et al 2014, Maher, Mrsny et al 2016, Ates, Kaynak et al 2016, nasal cavity (Benediktsdottir, Baldursson et al 2014, Giuliani, Balducci et al 2018. Chitosan has also been scrutinised in the ocular drug delivery due to its permeation enhancement properties; with drugs such as ofloxacin (Di Colo, Burgalassi et al 2004), triamcinolone acetonide (Raval, Khunt et al 2018) and timolol maleate (Rodriguez, Antonio Vazquez et al 2017).…”

Section: Introductionmentioning

confidence: 99%

Engineering and Development of Chitosan-Based Nanocoatings for Ocular Contact Lenses

Mehta

Al-Kinani

Arshad

et al. 2019

Journal of Pharmaceutical Sciences

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This research manuscript reports on Electrohydrodynamic Atomisation (EHDA) to engineer ondemand coatings for ocular contact lenses. A formulation approach was adopted to modulate the release of timolol maleate (TM) using chitosan and borneol. Polyvinylpyrrolidone (PVP) and poly (Nisopropylacrylamide) (PNIPAM) were electrically atomised to produce optimised, stationary contact lens coatings to encapsulate TM. The particle and fibre diameter, thermal stability, compatibility of the formed coatings along with their in vitro release-modulating effect and ocular tolerability were investigated. The results demonstrated highly stable nano-matrices with advantageous morphology and size. All formulations yielded coatings with high TM encapsulation (>88%); with excellent ocular biocompatibility. The coatings presented biphasic and triphasic release; depending on composition. Kinetic modelling revealed a noticeable effect of chitosan; the higher the concentration, the more the TM release due to chitosan swelling; with the release mechanism changing from Fickian diffusion (1% w/v; n = 0.5) to non-Fickian (5% w/v, 0.45 < n < 0.89). The use of EHDA has not yet been explored in depth within the ocular research remit; engineering on demand lens coatings capable of sustaining TM release. This is likely to offer an alternative dosage form for management of glaucoma with particular emphasis on improving poor patient compliance.

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Section: Introductionmentioning

confidence: 99%

Engineering and Development of Chitosan-Based Nanocoatings for Ocular Contact Lenses

Mehta

Al-Kinani

Arshad

et al. 2019

Journal of Pharmaceutical Sciences

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“…Nerve endings of CNS in nasal cavity can take-up the drug directly from nose by means of olfactory pathway and trigeminal nerves by circumventing BBB [15][16][17]. Different formulation approaches like nanosuspension based gels [18], polymeric nanoparticles [19], solid lipid nanoparticles [20], nanostructured lipid nanoparticles [21], microemulsions [22], cyclodextrin complexes [23] etc., are being experimented to carry drug directly to brain. However, the surface area of nasal cavity is 150 cm 2 with total volume of 15-20 mL nasal fluid and thus the volume of intranasal drug delivery is restricted to 25-200 μL [19,24,25].…”

Section: Introductionmentioning

confidence: 99%

Intranasal Zotepine Nanosuspension: intended for improved brain distribution in rats

et al. 2019

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Background Zotepine (ZTP), an antipsychotic drug is well tolerated and particularly effective for treating negative symptoms of psychosis. But is limited by low oral bioavailability caused by substantial first pass metabolism and thereby less amount of drug reaches the brain due to blood brain barrier (BBB). Objectives Since ZTP displays dose dependent side effects, purpose of the contemporary study is to develop zotepine loaded nanosuspension (ZTP-NS) for increased brain targeting in rats at lower doses. Methods ZTP-NS is prepared by two techniques viz., sonoprecipitation (SP) and combination technique (high pressure homogenization preceded by precipitation) by employing various stabilizers. Optimized ZTP-NS was characterized for particle size, solid state, morphology and solubility. In vitro drug release of ZTP and formulations was conducted using Franz diffusion cell. Stability study was performed at different temperature conditions. Pharmacokinetic study was performed in Wistar rats to determine the bioavailability and brain distribution of ZTP after intra-nasal (IN) and intravenous (IV) administration. Histopathology of brain was done after repeated administration of IN ZTP dispersion and NS up to 14 days. Results The optimized ZTP-NS formulated with Pluronic F-127 (0.3%w/v), Hydroxypropyl methyl cellulose E15 (0.3%w/v) and soya lecithin (0.4%w/v) showed particle size of 519.26 ± 10.44 nm & 330.2 ± 12.90 nm and zeta potential of −21.7 ± 1.39 mV and − 18.26 ± 1.64 mV with sonoprecipitation and combination technique respectively. In vitro drug release was high (81.79 ± 3.23%) for ZTP-NS prepared by combination technique. Intranasal NS resulted in high brain concentrations of 8.6 fold (sonoprecipitation) and 10.79-fold hike in AUC 0-24h in contrast to intravenous ZTP solution. Histopathology results reveal no significant changes in brain microscopic images. Conclusion ZTP-NS was successfully developed, characterized and found that nanosuspension is a favorable approach for intranasal delivery of zotepine.

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“…They were initially intended to deliver powders into lungs of rats (DP-4R) or mice (DP-4 M) after inserting the tip into the trachea of the anaesthetized animal. However, the DP-4 device has also been used to deliver powder into the nasal cavity of rats (Giuliani et al, 2018) and to deposit powder onto Calu-3 monolayers under an air-liquid interface (ALI) (Meindl et al, 2015;Cingolani, 2017).…”

Section: Formulation Deposition Methodsmentioning

confidence: 99%

How to characterize a nasal product. The state of the art of in vitro and ex vivo specific methods

Salade

Wauthoz

Goole

et al. 2019

International Journal of Pharmaceutics

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Nasal delivery offers many benefits over other conventional routes of delivery (e.g. oral or intravenous administration). Benefits include, among others, a fast onset of action, non-invasiveness and direct access to the central nervous system. The nasal cavity is not only limited to local application (e.g. rhinosinusitis) but can also provide direct access to other sites in the body (e.g. the central nervous system or systemic circulation). However, both the anatomy and the physiology of the nose impose their own limitations, such as a small volume for delivery or rapid mucociliary clearance. To meet nasal-specific criteria, the formulator has to complete a plethora of tests, in vitro and ex vivo, to assess the efficacy and tolerance of a new drug-delivery system. Moreover, depending on the desired therapeutic effect, the delivery of the drug should target a specific pathway that could potentially be achieved through a modified release of this drug. Therefore, this review focuses on specific techniques that should be performed when a nasal formulation is developed. The review covers both the tests recommended by regulatory agencies (e.g. the Food and Drug Administration) and other complementary experiments frequently performed in the field.

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In vivo nose-to-brain delivery of the hydrophilic antiviral ribavirin by microparticle agglomerates

Cited by 61 publications

References 67 publications

Engineering and Development of Chitosan-Based Nanocoatings for Ocular Contact Lenses

Engineering and Development of Chitosan-Based Nanocoatings for Ocular Contact Lenses

Intranasal Zotepine Nanosuspension: intended for improved brain distribution in rats

How to characterize a nasal product. The state of the art of in vitro and ex vivo specific methods

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