Your search keyword '"Shasha Rao"' showing total 4 results

1. Synergistic role of solid lipid and porous silica in improving the oral delivery of weakly basic poorly water soluble drugs

Author

Clive A. Prestidge, Kristen E. Bremmell, Rokhsana Yasmin, Shasha Rao, Yasmin, Rokhsana, Rao, Shasha, Bremmell, Kristen Elizabeth, and Prestidge, Clive

Subjects

Drug, Cinnarizine, Scanning electron microscope, media_common.quotation_subject, Administration, Oral, Pharmaceutical Science, Nanoparticle, 02 engineering and technology, 030226 pharmacology & pharmacy, 03 medical and health sciences, Drug Delivery Systems, 0302 clinical medicine, medicine, Porosity, Dissolution, media_common, Drug Carriers, solid lipid, Chromatography, Chemistry, Water, Drug Synergism, poorly water soluble drugs, Hydrogen-Ion Concentration, Silicon Dioxide, 021001 nanoscience & nanotechnology, Lipids, oral delivery, Water soluble, Solubility, Drug delivery, porous silica, 0210 nano-technology, solubilization, medicine.drug

Abstract

Oral absorption of weakly basic drugs (e.g. cinnarizine (CIN)) is limited by their pH dependent precipitation in intestinal conditions. To overcome this challenge, a novel drug delivery system composed of solid lipid and porous silica, namely silica encapsulated solid lipid (SESL) particles, was developed via hot homogenization of melted lipid dispersion, followed by ultra-sonication of the silica stabilized homogenized melted lipid dispersion. Scanning electron microscope (SEM) images of the SESL formulation revealed non-spherical and aggregated hybrid particles, with rough exterior and structured nanoparticles visible on the surface. A 1.5, 2.2 and 7-fold improvement in the dissolution of CIN was observed for the SESL particles, under simulated intestinal non-digesting conditions, in comparison to the drug loaded in solid lipid (CIN-SL) matrix, drug loaded in porous silica (CIN-PS) and pure drug powder. Under simulated intestinal digestive condition, significant improvement in the drug solubilization was reported for the SESL formulation in compared to the individual drug loaded systems i.e. CIN-PS and CIN-SL. Thereby, silica encapsulated solid lipid system provides a promising oral delivery approach for poorly water soluble weakly basic drugs. Refereed/Peer-reviewed

Published

2017

2. Silica encapsulated lipid-based drug delivery systems for reducing the fed/fasted variations of ziprasidone in vitro

Author

Nicky Thomas, Clive A. Prestidge, Tahnee J. Dening, Shasha Rao, Dening, Tahnee J, Rao, Shasha, Thomas, Nicky, and Prestidge, Clive Allan

Subjects

solid-dosage forms, Chemistry, Pharmaceutical, Administration, Oral, Polysorbates, Pharmaceutical Science, 02 engineering and technology, silica nanoparticles, Pharmacology, 030226 pharmacology & pharmacy, Piperazines, Drug Delivery Systems, 0302 clinical medicine, Drug Stability, lipid-based drug delivery systems, Solubility, silica–lipid hybrid microparticles, poorly water-soluble drugs, media_common, Drug Carriers, Chemistry, Fasting, General Medicine, Silicon Dioxide, 021001 nanoscience & nanotechnology, Lipids, 3. Good health, Drug delivery, Emulsions, 0210 nano-technology, Drug carrier, Biotechnology, medicine.drug, Drug, media_common.quotation_subject, ziprasidone, Biological Availability, Absorption (skin), 03 medical and health sciences, food effect, medicine, Humans, Lipolysis, Ziprasidone, Chromatography, self-nanoemulsifying drug delivery systems, Water, antipsychotic, Bioavailability, Thiazoles, solubilisation, Nanoparticles

Abstract

Ziprasidone is a poorly water-soluble antipsychotic drug that demonstrates low fasted state oral bioavailability and a clinically significant two-fold increase in absorption when dosed postprandially. Owing to significant compliance challenges faced by schizophrenic patients, a novel oral formulation of ziprasidone that demonstrates improved fasted state absorption and a reduced food effect is of major interest, and is therefore the aim of this research. Three lipid-based drug delivery systems (LBDDS) were developed and investigated: (a) a self-nanoemulsifying drug delivery system (SNEDDS), (b) a solid SNEDDS formulation, and (c) silica-lipid hybrid (SLH) microparticles. SNEDDS was developed using Capmul MCM® and Tween 80®, and solid SNEDDS was fabricated by spray-drying SNEDDS with Aerosil 380® silica nanoparticles as the solid carrier. SLH microparticles were prepared in a similar manner to solid SNEDDS using a precursor lipid emulsion composed of Capmul MCM® and soybean lecithin. The performance of the developed formulations was evaluated under simulated digesting conditions using an in vitro lipolysis model, and pure (unformulated) ziprasidone was used as a control. While pure ziprasidone exhibited the lowest rate and extent of drug solubilization under fasting conditions and a significant 2.4-fold increase in drug solubilization under fed conditions, all three LBDDS significantly enhanced the extent of drug solubilization under fasting conditions between 18- and 43-folds in comparison to pure drug. No significant difference in drug solubilization for the fed and fasted states was observed for the three LBDDS systems. To highlight the potential of LBDDS, mechanism(s) of action and various performance characteristics are discussed. Importantly, LBDDS are identified as an appropriate formulation strategy to explore further for the improved oral delivery of ziprasidone. Refereed/Peer-reviewed

Published

2016

3. Oral nanomedicine approaches for the treatment of psychiatric illnesses

Author

Shasha Rao, Clive A. Prestidge, Tahnee J. Dening, Nicky Thomas, Dening, Tahnee J, Rao, Shasha, Thomas, Nicky, and Prestidge, Clive A

Subjects

Drug, medicine.medical_specialty, Polymers, media_common.quotation_subject, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, 030226 pharmacology & pharmacy, 03 medical and health sciences, Drug Delivery Systems, 0302 clinical medicine, Aqueous solubility, Solid lipid nanoparticle, medicine, Humans, lipid-based drug delivery systems, Psychiatry, media_common, psychiatric illnesses, business.industry, Mental Disorders, 021001 nanoscience & nanotechnology, Lipids, nanomedicine, Treatment efficacy, 3. Good health, Nanomedicine, controlled drug release, oral bioavailability, drug delivery, Drug delivery, Nanoparticles, 0210 nano-technology, business, Psychotropic Agent, Oral retinoid

Abstract

Psychiatric illnesses are a leading cause of disability and morbidity globally. However, the preferred orally dosed pharmacological treatment options available for depression, anxiety and schizophrenia are often limited by factors such as low drug aqueous solubility, food effects, high hepatic first-pass metabolism effects and short half-lives. Furthermore, the discovery and development of more effective psychotropic agents has stalled in recent times, with the majority of new drugs reaching the market offering similar efficacy, but suffering from the same oral delivery concerns. As such, the application of nanomedicine formulation approaches to currently available drugs is a viable option for optimizing oral drug delivery and maximizing treatment efficacy. This review focuses on the various delivery challenges encountered by psychotropic drugs, and the ability of nanomedicine formulation strategies to overcome these. Specifically, we critically review proof of concept in vitro and in vivo studies of nanoemulsions/microemulsions, solid lipid nanoparticles, dendrimers, polymeric micelles, nanoparticles of biodegradable polymers and nanosuspensions, and provide new insight into the various mechanisms for improved drug performance. The advantages and limitations of current oral nanomedicine approaches for psychotropic drugs are discussed, which will provide guidance for future research directions and assist in fostering the translation of such delivery systems to the clinical setting. Accordingly, emphasis has been placed on correlating the in vitro/in vivo performance of these nanomedicine approaches with their potential clinical outcomes and benefits for patients. Refereed/Peer-reviewed

Published

2016

4. Virtual screening for Raf-1 kinase inhibitors based on pharmacophore model of substituted ureas

Author

Li-Ye Hu, Bo-Tao Xin, Huifang Li, Tian Zhu, Shasha Rao, Tao Lu, Yadong Chen, Yong-Jun Jiang, Li, Hui-Fang, Lu, Tao, Zhu, Tian, Jiang, Yong-Jun, Rao, Sha-Sha, Hu, Li-Ye, and Xin, Bo-Tao

Subjects

Models, Molecular, Pharmacology, Virtual screening, Training set, pharmacophore, Molecular model, Stereochemistry, Chemistry, Organic Chemistry, Rational design, molecular docking, General Medicine, virtual screening, Proto-Oncogene Proteins c-raf, Virtual database, Docking (molecular), Drug Discovery, Raf 1 kinase, Database Management Systems, Urea, Pharmacophore, Protein Kinase Inhibitors, Raf-1 kinase inhibitors

Abstract

A three-dimensional (3D) quantitative pharmacophore model was developed from a training set of structurally diverse substituted ureas against Raf-1 kinase, which was well validated to be highly predictive by two methods, namely, test set prediction and Cat-Scramble method. Then a virtual database searching was performed with the pharmacophore model as a 3D query, and the bioactivities of the retrieved hits were predicted by the pharmacophore. Subsequently, molecular docking was carried out on the selected hits whose estimated IC50 was less than 1 μM. Finally, 29 hits were identified as potential leads against Raf-1 kinase, which exhibited good estimated activities, high docking scores, similar binding mode to experimentally proven compounds and favorable drug-like properties. The study may facilitate the discovery and rational design of novel leads with potent inhibitory activity targeting Raf-1 kinase. Refereed/Peer-reviewed

Published

2009