Your search keyword '"Risperidone chemistry"' showing total 136 results

1. Accelerated removal of solvent residuals from PLGA microparticles by alcohol vapor-assisted fluidized bed drying.

Author

Kias F and Bodmeier R

Subjects

Drug Liberation, Polyglycolic Acid chemistry, Lactic Acid chemistry, Ethanol chemistry, Methylene Chloride chemistry, Particle Size, Water chemistry, Solvents chemistry, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Dexamethasone chemistry, Desiccation methods, Risperidone chemistry

Abstract

The removal of residual solvents from biodegradable poly(D,L-lactide-co-glycolide) (PLGA) microparticles by fluidized bed drying was investigated. Microparticles were prepared by the O/W solvent extraction/evaporation method and the influence of various process and formulation parameters on the secondary drying was studied. PLGA microparticles and films were characterized for residual organic solvent and water content, recrystallisation, surface morphology, drug loading and in-vitro release of the drugs dexamethasone and risperidone. While alcohol-free fluidized bed drying decreased the residual dichloromethane content only from about 7 % (w/w) to 6.4 % (w/w) (18 °C) or 3.2 % (w/w) (35 °C) within 24 h, 140 mg/L methanol vapor in purge gas facilitated almost complete removal of dichloromethane or ethyl acetate from microparticles (0-0.11 % (w/w) after 6 h). By controlling the alcohol concentration and temperature of the purge gas, the alcohol absorption and complete removal was controlled. Risperidone increased the methanol absorption enhancing the plasticization. A high initial residual water content was identified to promote aggregation and was eliminated by starting fluidized bed drying without alcohol. Alcohol vapor-assisted fluidized bed drying accelerated microparticle manufacturing without affecting the redispersibility, the drug loading and the in-vitro release of risperidone and dexamethasone., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

2. Control of encapsulation efficiency and morphology of poly(lactide-co-glycolide) microparticles with a diafiltration-driven solvent extraction process.

Author

Kias F and Bodmeier R

Subjects

Polyglycolic Acid chemistry, Lactic Acid chemistry, Drug Compounding methods, Porosity, Filtration methods, Drug Liberation, Microspheres, Drug Carriers chemistry, Methylene Chloride chemistry, Chemistry, Pharmaceutical methods, Solvents chemistry, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Particle Size, Dexamethasone chemistry, Dexamethasone administration & dosage, Risperidone chemistry, Risperidone administration & dosage

Abstract

The removal of organic solvents during the preparation of biodegradable poly(D,L-lactide-co-glycolide) (PLGA) microparticles by an O/W- solvent extraction/evaporation process was investigated and controlled by diafiltration. Emulsification and steady replacement of the aqueous phase were performed in parallel in a single-vessel setup. During the process, the solidification of the dispersed phase (drug:PLGA:solvent droplets) into microparticles was monitored with video-microscopy and focused beam reflectance measurement (FBRM) and the residual solvent content was analyzed with headspace gas chromatography (organic solvent) and coulometric Karl-Fischer titration (water). Microparticles containing dexamethasone or risperidone were characterized with regard to particle size, morphology, encapsulation efficiency and in-vitro release. Diafiltration-accelerated solvent extraction shortened the process time by accelerating solidification of dispersed phase but reduced the residual dichloromethane content only in combination with increased temperature. Increasing the diafiltration rate increased particle size, porosity, and the encapsulation efficiency of risperidone. The latter effect was particularly evident with increasing lipophilicity of PLGA. A slower and more uniform solidification of end-capped and increased lactide content PLGA grade was identified as the reason for an increased drug leaching. Accelerated solvent extraction by diafiltration did not affect the in-vitro release of risperidone from different PLGA grades. The initial burst release of dexamethasone was increased by diafiltration when encapsulated in concentrations above the percolation threshold. Both porosity and burst release could be reduced by increasing the process temperature during diafiltration. Residual water content was established as an indicator for porosity and correlated with the burst release of dexamethasone., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

3. Microfluidic preparation of monodisperse PLGA-PEG/PLGA microspheres with controllable morphology for drug release.

Author

Chen W, Li H, Zhang X, Sang Y, and Nie Z

Subjects

Microfluidic Analytical Techniques instrumentation, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Drug Carriers chemistry, Risperidone chemistry, Porosity, Particle Size, Polyglactin 910, Microspheres, Polyethylene Glycols chemistry, Drug Liberation

Abstract

Monodisperse biodegradable polymer microspheres show broad applications in drug delivery and other fields. In this study, we developed an effective method that combines microfluidics with interfacial instability to prepare monodispersed poly(lactic- co -glycolic acid)- b -polyethylene glycol (PLGA-PEG)/poly(lactic- co -glycolic acid) (PLGA) microspheres with tailored surface morphology. By adjusting the mass ratio of PLGA-PEG to PLGA, the concentration of stabilizers and the type of PLGA, we generated microspheres with various unique folded morphologies, such as "fishtail-like", "lace-like" and "sponge-like" porous structures. Additionally, we demonstrated that risperidone-loaded PLGA-PEG/PLGA microspheres with these folded morphologies significantly enhanced drug release, particularly in the initial stage, by exhibiting a logarithmic release profile. This feature could potentially address the issue of delayed release commonly observed in sustained-release formulations. This study presents a straightforward yet effective approach to construct precisely engineered microspheres offering enhanced control over drug release dynamics.

Published

2024

4. Acceleration of Final Residual Solvent Extraction From Poly(lactide-co-glycolide) Microparticles.

Author

Kias F and Bodmeier R

Subjects

Particle Size, Risperidone chemistry, Lactic Acid chemistry, Polyglycolic Acid chemistry, Drug Compounding methods, Microspheres, Solvents chemistry, Methylene Chloride chemistry, Dexamethasone chemistry, Polylactic Acid-Polyglycolic Acid Copolymer chemistry

Abstract

Purpose: The removal of the residual solvent dichloromethane from biodegradable poly(D,L-lactic-co-glycolic acid) (PLGA) microparticles was investigated by aqueous or alcoholic wet extraction or vacuum-drying., Methods: Microparticles were prepared by the O/W solvent extraction/evaporation method. The solidified microparticles were separated by filtration and the effect of subsequent drying and wet extraction methods were investigated. The residual solvent content was analysed with gas chromatography (organic solvents) and Karl Fischer titration (water). The effect of extraction conditions on microparticle aggregation, surface morphology and encapsulation of the drugs dexamethasone and risperidone was investigated., Results: Residual dichloromethane was reduced to 2.43% (w/w) (20 °C) or 0.03% (w/w) (35 °C) by aqueous wet extraction. With vacuum-drying, residual dichloromethane only decreased from about 5% (w/w) to 4.34% (w/w) (20 °C) or 3.20% (w/w) (35 °C) due to the lack of the plasticizing effect of water. Redispersion of filtered, wet microparticles in alcoholic media significantly improved the extraction due to an increased PLGA plasticization. The potential of different extractants was explained with the Gordon-Taylor equation and Hansen solubility parameters. Extraction in methanol: or ethanol:water mixtures reduced residual dichloromethane from 4 - 7% (w/w) to 0.5 - 2.3% (w/w) within 1 h and 0.08 - 0.18% (w/w) within 6 h. Higher alcohol contents and higher temperature resulted in aggregation of microparticles and lower drug loadings., Conclusion: The final removal of residual dichloromethane was more efficient with alcoholic wet extraction followed by aqueous wet extraction at elevated temperature and vacuum drying of the microparticles., (© 2024. The Author(s).)

Published

2024

5. Risperidone-cyclodextrin complex reservoir combined with hydrogel-forming microneedle array patches for enhanced transdermal delivery.

Author

Ghanma R, Anjani QK, Naser YA, Sabri AHB, Hutton ARJ, Vora LK, Himawan A, Greer B, McCarthy HO, and Donnelly RF

Subjects

Animals, Rats, Needles, Rats, Sprague-Dawley, Skin Absorption, Cyclodextrins chemistry, Antipsychotic Agents administration & dosage, Antipsychotic Agents pharmacokinetics, Female, Skin metabolism, Risperidone administration & dosage, Risperidone pharmacokinetics, Risperidone chemistry, Hydrogels chemistry, Drug Delivery Systems methods, Drug Delivery Systems instrumentation, Administration, Cutaneous, Solubility, 2-Hydroxypropyl-beta-cyclodextrin chemistry

Abstract

Hydrogel-forming microneedle array patches (HFMAPs) are microneedles that create microconduits upon insertion and swelling in the skin, potentially allowing prolonged drug delivery without generating sharps waste. Delivering hydrophobic drugs using HFMAPs poses challenges, which can be addressed using solubility enhancers such as cyclodextrins (CDs). This study aimed to deliver risperidone (RIS) transdermally using HFMAPs. To enhance the aqueous solubility of RIS hydroxypropyl-beta-cyclodextrin (HP-β-CD) and hydroxypropyl-gamma-cyclodextrin (HP-γ-CD) were utilised and their performance was tested using phase solubility studies. The aqueous solubility of RIS was enhanced by 4.75-fold and 2-fold using HP-β-CD and HP-γ-CD, respectively. RIS-HP-β-CD complex (CX) and physical mixture (PM) directly compressed tablets were prepared and combined with HFMAPs. Among the tested formulations, RIS-HP-β-CD PM reservoirs with 11 x 11 PVA/PVP HFMAPs exhibited the best performance in ex vivo studies and were further evaluated in in vivo experiments using female Sprague Dawley rats. The extended wear time of the MAPs resulted in the sustained release of RIS and its active metabolite 9-hydroxyrisperidone (9-OH-RIS) in plasma samples, lasting from 3 to 5 days with a 1-day application and up to 10 days with a 5-day application. For a 1-day application, HFMAPs showed greater systemic exposure to RIS compared to intramuscular control (AUC 0-t : 13330.05 ± 2759.95 ng/mL/hour versus 2706 ± 1472 ng/mL/hour). Moreover, RIS exposure was extended to 5 days (AUC 0-t : 12292.37 ± 1801.94 ng/mL/hour). In conclusion, HFMAPs could serve as an alternative for delivering RIS in a sustained manner, potentially improving the treatment of schizophrenia., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

6. Towards in vitro - In vivo correlation models for in situ forming drug implants.

Author

Wang X, Roy M, Wang R, Kwok O, Wang Y, Wang Y, Qin B, and Burgess DJ

Subjects

Antipsychotic Agents administration & dosage, Antipsychotic Agents pharmacokinetics, Antipsychotic Agents chemistry, Animals, Solubility, Risperidone administration & dosage, Risperidone pharmacokinetics, Risperidone chemistry, Drug Liberation, Drug Implants

Abstract

In vitro-In vivo correlation (IVIVC) is a main focus of the pharmaceutical industry, academia and the regulatory sectors, as this is an effective modelling tool to predict drug product in vivo performance based on in vitro release data and serve as a surrogate for bioequivalence studies, significantly reducing the need for clinical studies. Till now, IVIVCs have not been successfully developed for in situ forming implants due to the significantly different in vitro and in vivo drug release profiles that are typically achieved for these dosage forms. This is not unexpected considering the unique complexity of the drug release mechanisms of these products. Using risperidone in situ forming implants as a model, the current work focuses on: 1) identification of critical attributes of in vitro release testing methods that may contribute to differences in in vitro and in vivo drug release from in situ forming implants; and 2) optimization of the in vitro release method, with the aim of developing Level A IVIVCs for risperidone implants. Dissolution methods based on a novel Teflon shape controlling adapter along with a water non-dissolvable glass fiber membrane (GF/F) instead of a water dissolvable PVA film (named as GF/F-Teflon adapter and PVA-Teflon adapter, respectively), and an in-house fabricated Glass slide adapter were used to investigate the impact of: the surface-to-volume ratio, water uptake ratio, phase separation rate (measured by NMP release in 24 h post injection in vitro or in vivo), and mechanical pressure on the drug release patterns. The surface-to-volume ratio and water uptake were shown to be more critical in vitro release testing method attributes compared to the phase separation rate and mechanical pressure. The Glass slide adapter-based dissolution method, which allowed for the formation of depots with bio-mimicking surface-to-volume ratios and sufficient water uptake, has the ability to generate bio-relevant degradation profiles as well as in vitro release profiles for risperidone implants. For the first time, a Level A IVIVC (rabbit model) has been successfully developed for in situ forming implants. Release data for implant formulations with slightly different PLGA molecular weights (MWs) were used to develop the IVIVC. The predictability of the model passed external validation using the reference listed drug (RLD), Perseris®. IVIVC could not be developed when formulations with different PLGA molar ratios of lactic acid to glycolic acid (L/G) were included. The present work provides a comprehensive understanding of the impact of the testing method attributes on drug release from in situ forming implants, which is a valuable practice for level A IVIVC development., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

7. Visualization and correlation of drug release of risperidone/clozapine microspheres in vitro and in vivo based on FRET mechanism.

Author

Chen Y, He Q, Lu H, Yang J, Han J, Zhu Y, and Hu P

Subjects

Rats, Animals, Polylactic Acid-Polyglycolic Acid Copolymer, Lactic Acid chemistry, Polyglycolic Acid chemistry, Drug Liberation, Microspheres, Fluorescence Resonance Energy Transfer, Risperidone chemistry, Clozapine, Carbocyanines

Abstract

This study addresses the challenging task of quantitatively investigating drug release from PLGA microspheres after in vivo administration. The objective is to employ Förster resonance energy transfer (FRET) to visualize drug-encapsulated microspheres in both in vitro and in vivo settings. The primary goal is to establish a quantitative correlation between FRET fluorescence changes and microsphere drug release. The study selects drugs with diverse structures and lipid solubility to explore release mechanisms, using PLGA as the matrix material. Clozapine and risperidone serve as model drugs. FRET molecules, Cy5 and Cy5.5, along with Cy7 derivatives, create FRET donor-acceptor pairs. In vitro results show that FRET fluorescence changes align closely with microsphere drug release, particularly for the Cy5.5-Cy7 pair. In vivo experiments involve subcutaneous administration of microspheres to rats, tracking FRET fluorescence changes while collecting blood samples. Pharmacokinetic studies on clozapine and risperidone reveal in vivo absorption fractions using the Loo-Riegelman method. Correlating FRET and in vivo absorption data establishes an in vitro-in vivo relationship (IVIVR). The study demonstrates that FRET-based fluorescence changes quantitatively link to microsphere drug release, offering an innovative method for visualizing and monitoring release in both in vitro and in vivo settings, potentially advancing clinical applications of such formulations., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Ping Hu reports financial support was provided by National Natural Science Foundation of China. Ping Hu reports financial support was provided by Science and Technology Program of Guangzhou, China. Ping Hu reports financial support was provided by Natural Science Foundation of Guangdong Province of China. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

8. Reverse engineering of Perseris and development of compositionally equivalent formulations.

Author

Wang X, Bao Q, Wang R, Wan B, Wang Y, Qin B, and Burgess DJ

Subjects

Humans, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Risperidone chemistry, Pharmaceutical Preparations, Microspheres, Polyglycolic Acid chemistry, Lactic Acid chemistry

Abstract

Six injectable, long-acting in situ forming implant drug products based on poly(lactide-co-glycolide) (PLGA) and N-Methyl-2-Pyrrolidone (NMP) are available on the market. However, generic products, which would likely be more affordable for patients, are not yet available. This is partially due to the unique complexity of these formulations as well as the inherent heterogeneity of PLGA and the challenges in the manufacture and characterization of this polymer. This article focuses on a comprehensive characterization of Perseris (risperidone) in situ forming implant drug product, and the development of compositionally equivalent formulations. The molecular weight (MW), lactide/glycolide (L/G) ratio, end group, blockiness and glass transition temperature (T g ) of PLGA, as well as the crystal form and particle size of risperidone powder used in Perseris were identified through reverse engineering. The dissolved/suspended drug ratio in the final implant suspension for administration, as well as the real-time drug solid state in the solidified Perseris drug depot were investigated. Two compositionally equivalent formulations prepared using customized PLGA polymers with similar properties to the Perseris PLGA showed similar in vitro release and swelling behavior to Perseris as demonstrated using a novel adapter-based dissolution method. The novelty of this dissolution method lies in its ability to control implant shape, generate reproducible data, distinguish different release phases, as well as identify formulation changes. The knowledge gained in this work and the methodology established for characterization of the implant formulations are important for implant formulation development., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

9. Drug Repurposing: Deferasirox Inhibits the Anti-Apoptotic Activity of Mcl-1.

Author

Bourafai-Aziez A, Benabderrahmane M, Paysant H, Weiswald LB, Poulain L, Carlier L, Ravault D, Jouanne M, Coadou G, Oulyadi H, Voisin-Chiret AS, Sopková-de Oliveira Santos J, and Sebban M

Subjects

Deferasirox chemistry, Lenalidomide chemistry, Lenalidomide pharmacology, Magnetic Resonance Spectroscopy, Molecular Docking Simulation, Molecular Dynamics Simulation, Molecular Structure, Oxcarbazepine chemistry, Oxcarbazepine pharmacology, Risperidone chemistry, Risperidone pharmacology, Torsemide chemistry, Torsemide pharmacology, Apoptosis Regulatory Proteins drug effects, Deferasirox pharmacology, Drug Repositioning, Myeloid Cell Leukemia Sequence 1 Protein antagonists & inhibitors

Abstract

Introduction: With the aim of repositioning commercially available drugs for the inhibition of the anti-apoptotic myeloid cell leukemia protein, Mcl-1, implied in various cancers, five molecules, highlighted from a published theoretical screening, were selected to experimentally validate their affinity toward Mcl-1., Results: A detailed NMR study revealed that only two of the five tested drugs, Torsemide and Deferasirox, interacted with Mcl-1. NMR data analysis allowed the complete characterization of the binding mode of both drugs to Mcl-1, including the estimation of their affinity for Mcl-1. Biological assays evidenced that the biological activity of Torsemide was lower as compared to the Deferasirox, which was able to efficiently and selectively inhibit the anti-apoptotic activity of Mcl-1. Finally, docking and molecular dynamics led to a 3D model for the Deferasirox:Mcl-1 complex and revealed the positioning of the drug in the Mcl-1 P2/P3 pockets as well as almost all synthetic Mcl-1 inhibitors. Interestingly, contrary to known synthetic Mcl-1 inhibitors which interact through Arg263, Deferasirox, establishes a salt bridge with Lys234., Conclusion: Deferasirox could be a potential candidate for drug repositioning as Mcl-1 inhibitor., Competing Interests: The authors report no conflicts of interest in this work., (© 2021 Bourafai-Aziez et al.)

Published

2021

10. Main interactions of dopamine and risperidone with the dopamine D2 receptor.

Author

Martínez A, García-Gutiérrez P, Zubillaga RA, Garza J, and Vargas R

Subjects

Amino Acid Sequence, Binding Sites, Dopamine pharmacology, Models, Molecular, Protein Binding, Protein Conformation, Risperidone pharmacology, Thermodynamics, Dopamine chemistry, Receptors, Dopamine D2 chemistry, Risperidone chemistry

Abstract

Psychosis is one of the psychiatric disorders that is controlled by dopaminergic drugs such as antipsychotics that have affinity for the dopamine D2 receptor (DRD2). In this investigation we perform quantum chemical calculations of two molecules [dopamine and risperidone] within a large cavity of DRD2 that represents the binding site of the receptor. Dopamine is an endogenous neurotransmitter and risperidone is a second-generation antipsychotic. Non-covalent interactions of dopamine and risperidone with DRD2 are analyzed using the Quantum Theory of Atoms in Molecules (QTAIM) and the Non-Covalent Interaction index (NCI). The QTAIM results show that these molecules strongly interact with the receptor. There are 22 non-covalent interactions for dopamine and 54 for risperidone. The electron density evaluated at each critical binding point is small in both systems but it is higher for dopamine than for risperidone, indicating that the interactions of DRD2 with the first are stronger than with the second molecule. However, the binding energy is higher for risperidone (-72.6 kcal mol-1) than for dopamine (-22.8 kcal mol-1). Thus, the strength of the binding energy is due to the number of contacts rather than the strength of the interactions themselves. This could be related to the ability of risperidone to block DRD2 and may explain the efficacy of this drug for controlling the symptoms of schizophrenia, but likewise its secondary effects.

Published

2021

11. Interaction of graphene with antipsychotic drugs: Is there any charge transfer process?

Author

Del Castillo RM, Ramos E, and Martínez A

Subjects

Dopamine chemistry, Humans, Models, Chemical, Pramipexole chemistry, Receptors, Dopamine D2 drug effects, Risperidone chemistry, Antipsychotic Agents chemistry, Graphite chemistry

Abstract

Antipsychotics represent an effective therapy for schizophrenia (a chronic mental disorder). Their benefits are related to the interaction of the drugs with dopamine D2 receptor (D2R). Antipsychotics are classified as agonists or antagonists. One of the working hypotheses is that there is a charge transfer process between the drugs and the receptors, which is different for agonists and antagonists. To have more insight into the nature of the interaction of these molecules and the differences between agonists and antagonists, we analyze the interaction of graphene with three molecules: dopamine, pramipexole (an agonist of dopamine), and risperidone (an antagonist of dopamine). The idea is to use graphene as a simple model to analyze the charge transfer process of these three drugs. Optimized structures, atomic charges, and Density of States results indicate that global charges of dopamine and pramipexole are similar, while for risperidone, it is more than double. Pramipexole is an agonist, and the charge transfer process is similar to that of dopamine. Risperidone is an antagonist, and the charge transfer process is different from dopamine. The charge transfer is more significant with risperidone than with dopamine, and this could be related to the mechanism of action. This is in agreement with the working hypotheses that establish that it is possible to distinguish between agonists and antagonists since they have different capacity to transfer charge., (© 2020 Wiley Periodicals LLC.)

Published

2021

12. Encapsulation of Risperidone by Methylated β-Cyclodextrins: Physicochemical and Molecular Modeling Studies.

Author

Sbârcea L, Tănase IM, Ledeți A, Cîrcioban D, Vlase G, Barvinschi P, Miclău M, Văruţ RM, Trandafirescu C, and Ledeți I

Subjects

Calorimetry, Differential Scanning methods, Cyclodextrins chemistry, Drug Compounding methods, Models, Molecular, Solubility, Spectroscopy, Fourier Transform Infrared, Thermogravimetry methods, X-Ray Diffraction methods, Risperidone chemistry, beta-Cyclodextrins chemistry

Abstract

Risperidone (RSP) is an atypical antipsychotic drug which acts as a potent antagonist of serotonin-2 (5TH2) and dopamine-2 (D2) receptors in the brain; it is used to treat schizophrenia, behavioral and psychological symptoms of dementia and irritability associated with autism. It is a poorly water soluble benzoxazole derivative with high lipophilicity. Supramolecular adducts between drug substance and two methylated β-cyclodextrins, namely heptakis(2,6-di-O-methyl)-β-cyclodextrin (DM-β-CD) and heptakis(2,3,6-tri-O-methyl)-β-cyclodextrin (TM-β-CD) were obtained in order to enhance RSP solubility and improve its biopharmaceutical profile. The inclusion complexes were evaluated by means of thermoanalytical methods (TG-thermogravimetry/DTG-derivative thermogravimetry/HF-heat flow), powder X-ray diffractometry (PXRD), universal-attenuated total reflectance Fourier transform infrared (UATR-FTIR), UV spectroscopy and saturation solubility studies. Job's method was employed for the determination of the stoichiometry of the inclusion complexes, which was found to be 2:1 for both guest-host systems. Molecular modeling studies were carried out for an in-depth characterization of the interaction between drug substance and cyclodextrins (CDs). The physicochemical properties of the supramolecular systems differ from those of RSP, demonstrating the inclusion complex formation between drug and CDs. The RSP solubility was enhanced as a result of drug encapsulation in the CDs cavity, the higher increase being obtained with DM-β-CD as host; the guest-host system RSP/DM-β-CD can thus be a starting point for further research in developing new formulations containing RSP, with enhanced bioavailability.

Published

2020

13. Systematic development of a bioanalytical UPLC-MS/MS method for estimation of risperidone and its active metabolite in long-acting microsphere formulation in rat plasma.

Author

Rub RA, Beg S, Kazmi I, Afzal O, Almalki WH, Alghamdi S, Akhter S, Ali A, and Ahmed FJ

Subjects

Animals, Delayed-Action Preparations, Drug Stability, Limit of Detection, Linear Models, Liquid-Liquid Extraction, Male, Rats, Rats, Sprague-Dawley, Reproducibility of Results, Risperidone chemistry, Risperidone pharmacokinetics, Chromatography, High Pressure Liquid methods, Risperidone blood, Tandem Mass Spectrometry methods

Abstract

A systematic approach to develop a UPLC-MS/MS method was applied for quantifying of risperidone (RISP), its active metabolite, 9-hydroxy risperidone (9-OH-RISP) and internal standard (propranolol) in rat plasma. Liquid-liquid extraction was performed using methyl tert-butyl ether for quantification of drug and its active metabolite by MS detection in the positive ion mode. Acquity UPLC system with BEH C18 (2.1 mm × 100 mm, particle size 1.7 μm) column was used along with acetonitrile (0.1% formic acid)-2 mM (milli mole) ammonium acetate in isocratic condition was used as the mobile phase. Detection was performed by multiple reactions monitoring with precursor-to-product ion transitions with m/z 411.2 → 191.0 for RISP, m/z 427.2 → 207.0 for 9-OH-RISP and m/z 260.1 → 116.0 for IS. The method was validated as per the FDA guidance on bioanalytical method validation. Linearity (r 2  = 0.999) was observed in the drug concentration ranging between 0.1 and 50 ng mL -1 , while all other parameters were found to be within the acceptable ranges. Method robustness was optimized by Box-Behnken design to monitor the influential variables to achieve maximal recovery of the analytes in the rat plasma. Pharmacokinetic evaluation of the analytes from long-acting microparticles in rat plasma showed two peaks indicating an initial burst effect within 24 h of administration followed by controlled drug release pattern upto 45 days, while marketed formulation (Risperdal Consta®) showed no plasma concentration during the lag-time of 21 days followed by maximal drug absorption between 28 and 40 days., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

14. Organogels based on amino acid derivatives and their optimization for drug release using response surface methodology.

Author

Hu B, Yan H, Sun Y, Chen X, Sun Y, Li S, Jing Y, and Li H

Subjects

Animals, Gels, Hydrophobic and Hydrophilic Interactions, Male, Rats, Rats, Sprague-Dawley, Rheology, Risperidone chemistry, Risperidone pharmacokinetics, Tissue Distribution, Amino Acids chemistry, Drug Carriers chemistry, Drug Liberation

Abstract

Organogels are excellent drug carrier for controlled release. Organogels based on amino acid derivatives has been widely used in the area of drug delivery. In this study, a series of the organogel system based on amino acid derivatives gelators was designed and prepared to investigate the structure-property correlation in organogels. To investigate the factors that influence the property of drug release, we varied the formulation in the organogels: gelator structure, gelator concentration, volume of antigelation solvent, and drug loading. Through the Box-Behnken tests, the optimum organogel formulation in vitro was obtained. The self-healing properties of the organogel have been utilised for injection of a model lipophilic risperidone in situ , and sustained release of the drug has been studied over about one week in vivo . In conclusion, the gelation ability of gelators could be adjusted by the gelator structure. Gel property is related with the whole composition of the formulation. As drug carrier, the drug release property of organogels is affected by multiple factors. Our investigation of the gel release property will play a theoretical guiding role in the application in the in situ drug delivery system.

Published

2020

15. Designed proteinoid polymers and nanoparticles encapsulating risperidone for enhanced antipsychotic activity.

Author

Lugasi L, Grinberg I, Rudnick-Glick S, Okun E, Einat H, and Margel S

Subjects

Animals, Antipsychotic Agents pharmacology, Biological Transport, Blood-Brain Barrier metabolism, Cell Survival drug effects, Drug Compounding, Drug Liberation, Humans, Male, Mice, Inbred BALB C, Polyethylene Glycols chemistry, Polymerization, Porosity, Solubility, Tissue Distribution, Amino Acids chemistry, Antipsychotic Agents chemistry, Nanocapsules chemistry, Polyesters chemistry, Risperidone chemistry

Abstract

Background: Nanoparticles (NPs) incorporating drug formulations can be used to facilitate passage through biological barriers including the blood-brain barrier (BBB) and increase drug delivery and bioavailability. Hence, NP-based administration may enhance the efficiency of current antipsychotics. Encapsulation within NPs can resolve aqueous solubility problems that not only reduce permeability through the BBB but also affect targeting. The present study describes a new drug delivery system based on proteinoid NPs to explore the possibility of improving drug efficacy. Risperidone (RSP) is a commonly used atypical antipsychotic medication, and was therefore selected for encapsulation by proteinoid NPs., Results: Proteinoid polymers with high molecular weight and low polydispersity were synthesized from L-amino acids and poly-L-lactic acid (PLLA) by thermal step-growth polymerization mechanism. RSP-loaded proteinoid NPs were then prepared using a self-assembly process in the presence of RSP, followed by PEGylation. The optimal PEGylated RSP-loaded NPs were characterized in terms of diameter and size distribution, drug loading, ζ-potential, cytotoxicity, biodistribution, and psychopharmacological effects. The findings indicate significantly higher antipsychotic activity of drug-loaded proteinoid NPs compared to free RSP., Conclusions: Proteinoid NPs enhance RSP delivery and may potentially increase drug efficiency by reducing dosage and side effects.

Published

2020

16. Electromembrane extraction of chlorprothixene, haloperidol and risperidone from whole blood and urine.

Author

Yu X, Li X, You S, Shi Y, Zhu R, Dong Y, and Huang C

Subjects

Acids chemistry, Animals, Antipsychotic Agents blood, Antipsychotic Agents chemistry, Antipsychotic Agents urine, Body Fluids, Chlorprothixene chemistry, Chromatography, Liquid, Haloperidol chemistry, Humans, Male, Rats, Sprague-Dawley, Reproducibility of Results, Risperidone chemistry, Solvents chemistry, Tandem Mass Spectrometry, Time Factors, Water chemistry, Chlorprothixene blood, Chlorprothixene urine, Electricity, Haloperidol blood, Haloperidol urine, Membranes, Artificial, Risperidone blood, Risperidone urine

Abstract

Separation of antipsychotic drugs from whole blood and urine is of great importance for clinic and forensic laboratories. In this work, chlorprothixene, haloperidol and risperidone representing the first and second generations of antipsychotic drugs were studied. Among them, chlorprothixene and risperidone were investigated for the first time by electromembrane extraction (EME). After the screening, 2-nitrophenyl octyl ether (NPOE) was used as the supported liquid membrane (SLM). The EME performance for spiked water (pH 2), whole blood and urine was tested and optimized individually. Using NPOE and 60 V, efficient EME was achieved from urine and whole blood with trifluoroacetic acid as the acceptor solution. The equilibrium time required for EME was dependent on the sample matrices. The steady-state of EME was reached in 30 min and 20 min for whole blood and urine, respectively. At steady-state, the EME recoveries of the targets from different sample matrices were satisfactory, and were in the range of 74%-100%. The proposed EME approach combined with liquid chromatography-tandem mass spectrometry (LC-MS/MS) was evaluated using whole blood and urine. The obtained linearity was 1-200 ng mL -1 , and the coefficient of determination (R 2 ) was ≥ 0.9853 for haloperidol and ≥ 0.9936 for chlorprothixene and risperidone. The limit of detection (LOD) and accuracy for all the targets ranged from 0.2-0.6 ng mL -1 and 102%-110%, respectively, and the repeatability at low (1 ng mL -1 ), medium (10 ng mL -1 ) and high (200 ng mL -1 ) concentration was ≤ 12% (RSD). Finally, the validated approach was successfully used to determine chlorprothixene, risperidone and haloperidol in whole blood and urine from rats, which were treated with chlorprothixene, risperidone and haloperidol at low therapeutic dose, respectively., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020. Published by Elsevier B.V.)

Published

2020

17. Proteinoid Nanocapsules as Drug Delivery System for Improving Antipsychotic Activity of Risperidone.

Author

Lugasi L, Grinberg I, Sabag R, Madar R, Einat H, and Margel S

Subjects

Analysis of Variance, Animals, Carbon-13 Magnetic Resonance Spectroscopy, Cell Line, Cell Survival drug effects, Hydrodynamics, Mice, Particle Size, Proton Magnetic Resonance Spectroscopy, Risperidone chemistry, Tissue Distribution drug effects, Antipsychotic Agents pharmacology, Drug Delivery Systems, Nanocapsules chemistry, Risperidone pharmacology

Abstract

Risperidone (RSP) is an atypical antipsychotic drug widely used to treat schizophrenia and bipolar disorder. Nanoparticles (NPs) are being developed as in vivo targeted drug delivery systems, which cross the blood-brain barrier and improve pharmacokinetics and drug effectiveness. Here, biodegradable proteinoids were synthesized by thermal step-growth polymerization from the amino acids l-glutamic acid, l-phenylalanine and l-histidine and poly (l-lactic acid). Proteinoid NPs containing RSP were then formed by self-assembly, overcoming the insolubility of the drug in water, followed by PEGylation (poly ethylene glycol (PEG) conjugation to increase the stability of the NPs in the aqueous continuous phase. These NPs are biodegradable owing to their peptide and ester moieties. They were characterized in terms of diameter, size distribution, drug loading, and long-term storage. Behavioral studies on mice found enhanced antipsychotic activity compared to free RSP.

Published

2020

18. Evaluation of the Impacts of Formulation Parameters on the Pharmacokinetics and Bioequivalence of Risperidone Orodispersible Film: a Physiologically Based Pharmacokinetic Modeling Approach.

Author

Chen F, Liu H, Wang B, Yang Z, Chen Y, Yang L, Wang B, Jiao Z, Lin HS, Quan Y, Wang H, and Xiang X

Subjects

Administration, Oral, Animals, Dogs, Female, Humans, Male, Particle Size, Risperidone chemistry, Serotonin Antagonists administration & dosage, Serotonin Antagonists chemistry, Serotonin Antagonists pharmacokinetics, Solubility, Therapeutic Equivalency, Intestinal Absorption drug effects, Intestinal Absorption physiology, Models, Biological, Risperidone administration & dosage, Risperidone pharmacokinetics

Abstract

The purpose of this study was to investigate the impacts of the formulation parameters on the pharmacokinetics and bioequivalence of risperidone orodispersible film (ODF) using physiologically based pharmacokinetic model. The pharmacokinetic profiles of two risperidone ODFs, which exhibit different in vitro dissolution, were examined in Beagle dogs after supralingual administration. Subsequently, a physiologically based pharmacokinetic (PBPK) model was constructed to evaluate the in vivo performance of risperidone ODF. The parameter sensitivity analysis (PSA) was used to access the impacts of formulation parameters on the pharmacokinetics of risperidone. Moreover, the validated PBPK model was applied to predict human pharmacokinetic profiles and examine the bioequivalence of these two ODFs. These two ODFs displayed similar risperidone pharmacokinetic profiles in dogs. The parameter sensitivity analysis indicated that the changes in the solubility, particle size, particle density, and diffusion coefficient did not have obvious influence on the in vivo properties of risperidone ODF. Alternation of the in vitro complete dissolution time in water from 15 to 30 min led to a 30% decrease in C max and 20% of increase in T max . AUC 0-∞ would be decreased if risperidone was not fully released within 1 h. As both ODFs completely released risperidone within 15 min, the difference in the extent of in vivo absorption, intestinal regional absorption location, and plasma concentration-time curves between these two ODFs was almost negligible. Consequently, a bioequivalence was foreseen in humans. The in vitro cumulative dissolution percentage in water at 15 min was found to be the major determinant on the in vivo properties of risperidone ODF. PBPK modeling appears to be an innovative strategy to guide the development of risperidone ODF.

Published

2020

19. The effect of PLGA molecular weight differences on risperidone release from microspheres.

Author

Kohno M, Andhariya JV, Wan B, Bao Q, Rothstein S, Hezel M, Wang Y, and Burgess DJ

Subjects

Diffusion, Drug Compounding, Drug Liberation, Drug Stability, Kinetics, Microspheres, Molecular Weight, Transition Temperature, Vitrification, Drug Carriers, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Risperidone chemistry

Abstract

The objective of the present study was to investigate the effect of molecular weight differences of poly (lactic-co-glycolic acid) (PLGA) on the in vitro release profile of risperidone microspheres. Four different PLGA molecular weights were investigated and all the microsphere formulations were prepared using the same manufacturing process. Physicochemical properties (particle size, drug loading, morphology and molecular weight) as well as in vitro degradation profiles of the prepared microspheres were investigated in addition to in vitro release testing. The in vitro release tests were performed using a previously developed flow through cell (USP apparatus 4) method. The particle size of the four prepared microsphere formulations varied, however there were no significant differences in the drug loading. Interestingly, the in vitro release profiles did not follow the molecular weight of the polymers used. Instead, the drug release appeared to be dependent on the glass transition temperature of the polymers as well as the porosity of the prepared formulations. The catalytic effect of risperidone (an amine drug) on PLGA during manufacturing and release testing, minimized the differences in the molecular weights of the four formulations, explaining the independence of the release profiles on PLGA molecular weight., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Published by Elsevier B.V.)

Published

2020

20. Distinct inactive conformations of the dopamine D2 and D3 receptors correspond to different extents of inverse agonism.

Author

Lane JR, Abramyan AM, Adhikari P, Keen AC, Lee KH, Sanchez J, Verma RK, Lim HD, Yano H, Javitch JA, and Shi L

Subjects

Binding Sites, Drug Discovery, Molecular Dynamics Simulation, Protein Binding, Protein Conformation, Risperidone chemistry, Risperidone metabolism, Salicylamides chemistry, Salicylamides metabolism, Dopamine Agonists chemistry, Dopamine Agonists metabolism, Dopamine Antagonists chemistry, Dopamine Antagonists metabolism, Receptors, Dopamine D2 chemistry, Receptors, Dopamine D2 metabolism, Receptors, Dopamine D3 chemistry, Receptors, Dopamine D3 metabolism

Abstract

By analyzing and simulating inactive conformations of the highly homologous dopamine D 2 and D 3 receptors (D 2 R and D 3 R), we find that eticlopride binds D 2 R in a pose very similar to that in the D 3 R/eticlopride structure but incompatible with the D 2 R/risperidone structure. In addition, risperidone occupies a sub-pocket near the Na + binding site, whereas eticlopride does not. Based on these findings and our experimental results, we propose that the divergent receptor conformations stabilized by Na + -sensitive eticlopride and Na + -insensitive risperidone correspond to different degrees of inverse agonism. Moreover, our simulations reveal that the extracellular loops are highly dynamic, with spontaneous transitions of extracellular loop 2 from the helical conformation in the D 2 R/risperidone structure to an extended conformation similar to that in the D 3 R/eticlopride structure. Our results reveal previously unappreciated diversity and dynamics in the inactive conformations of D 2 R. These findings are critical for rational drug discovery, as limiting a virtual screen to a single conformation will miss relevant ligands., Competing Interests: JL, AA, PA, AK, KL, JS, RV, HL, HY, JJ, LS No competing interests declared

Published

2020

21. In vitro-in vivo correlation of parenteral PLGA microspheres: Effect of variable burst release.

Author

Andhariya JV, Jog R, Shen J, Choi S, Wang Y, Zou Y, and Burgess DJ

Subjects

Animals, Delayed-Action Preparations, Drug Carriers chemistry, Drug Liberation, Injections, Intramuscular, Leuprolide chemistry, Particle Size, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Porosity, Rabbits, Risperidone chemistry, Leuprolide administration & dosage, Microspheres, Risperidone administration & dosage

Abstract

Development of IVIVCs is a very complicated process, especially for complex drug products such as parenteral PLGA microspheres with multiphasic drug release characteristics. Specifically, microspheres that exhibit an initial burst release phase are even more challenging since the in vitro and in vivo burst release phases may not be comparable if drug absorption is rate-limiting at this stage. Therefore, the objectives of the present work were: 1) to investigate the predictability of developed IVIVCs for the in vivo burst release phase based on the in vitro burst release phase of the formulations; and 2) to evaluate the impact of variable burst release on the predictability of the developed IVIVCs for two different types of microsphere-based drug products. Accordingly, Risperdal Consta® (Risperidone) and Lupron Depot® (Leuprolide acetate, LA) were selected as model products. Compositionally equivalent risperidone and LA formulations with variable burst release phases were prepared with manufacturing process changes (such as solvent systems and mixing methods). The prepared microspheres exhibited differences in critical physicochemical properties (such as particle size, porosity, average pore diameter, and drug distribution) and hence differences in their in vitro release characteristics (such as variable burst release and release rate). The in vitro and in vivo (rabbit model (intramuscular injection) burst release were similar for the risperidone microspheres but were significantly different for the LA microspheres. This had an impact on the complexity of the developed IVIVC models. Level A IVIVCs with the ability to predict various types of burst release were developed using time scaling and shifting factors. Moreover, it was observed that IVIVCs developed using formulations with less variation in burst release had better predictability and vice-versa. Thus, the present research has provided a comprehensive understanding of the impact of the burst release phase on the development, complexity, and predictability of IVIVCs for complex parenteral microspheres containing a variety of therapeutic molecules., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

22. Probing Binding Landscapes and Molecular Recognition Mechanisms of Atypical Antipsychotic Drugs towards the Selective Targeting of D 2 Dopamine Receptor.

Author

Appiah-Kubi P, Olotu FA, and Soliman MES

Subjects

Antipsychotic Agents chemistry, Drug Discovery, Humans, Models, Molecular, Molecular Structure, Receptors, Dopamine D2 chemistry, Risperidone chemistry, Antipsychotic Agents pharmacology, Receptors, Dopamine D2 metabolism, Risperidone pharmacology

Abstract

Dopamine receptors constitute a unique class of G-protein coupled receptors that mediate the activities of dopamine, a neurotransmitter implicated in diverse neurological diseases when dysregulated. Over the years, antipsychotic drugs have been primarily directed towards D 2 dopamine receptor (DRD2) while associable adverse effects have been centred on non-selective targeting. The recent crystal structure of DRD2 in complex with atypical antipsychotic could further aid the structure-based design of highly DRD2-selective antipsychotics. Therefore, in this study, we comprehensively investigate the molecular recognition and differential binding landscapes of class-I and II DRD2 atypical antipsychotics, using membrane-bilayer molecular dynamics simulation and binding free energy techniques. Findings revealed that selected class-I antipsychotics exhibited binding dynamics and poses dissimilar to the class-II types with different interactive mechanisms at the binding cavity of DRD2. More interestingly, the class-II drugs established a highly coordinated binding at the DRD2 active site with a pertinent and recurrent involvement of Asp114 via strong hydrogen interactions. Furthermore, while these compounds exert distinct effects on DRD2 structure, findings revealed that the class-II types favourably engaged the deep hydrophobic pocket of DRD2 compared to the class-I drugs. We speculate that these findings will be fundamental to the discovery of highly selective DRD2 antipsychotics., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

23. Formulation and biopharmaceutical evaluation of risperidone-loaded chitosan nanoparticles for intranasal delivery.

Author

Rukmangathen R, Yallamalli IM, and Yalavarthi PR

Subjects

Administration, Intranasal methods, Animals, Biological Availability, Brain drug effects, Chemistry, Pharmaceutical methods, Drug Carriers chemistry, Drug Compounding methods, Drug Liberation drug effects, Nanoparticles administration & dosage, Particle Size, Poloxamer chemistry, Polyphosphates chemistry, Polysorbates chemistry, Rats, Rats, Wistar, Schizophrenia drug therapy, Chitosan chemistry, Nanoparticles chemistry, Risperidone chemistry

Abstract

Objective: High lipophilicity and extensive hepatic metabolism limits the oral application of risperidone in the treatment of CNS disorders. In order address this limitation, risperidone (RS) loaded chitosan nanoparticles (CS-NPs) were processed for intranasal administration in the management of schizophrenia. Methods: RS loaded CS-NPs were prepared by ionic gelation of chitosan with tripolyphosphate and stabilized by tween 80/ poloxamer 188. The CS-NPs were characterized by FTIR, DSC, particle size, zeta potential and surface morphology. Entrapment efficiency, mucoadhesive strength, in vitro drug release, and release kinetics of CS-NPs were evaluated. Pharmacokinetics and pharmacodynamics of RS loaded CS-NPs were studied using Wistar rats. Stereotypy behavior and swimming normalization tests were conducted in amphetamine induced psychosis in animals. Results: Risperidone nanoparticles (RP12) were produced with an average size of 86 nm, polydispersity index of 0.287, zeta potential of +36.6 mV, mucoadhesion of 68.9% and entrapment efficiency of 77.96%. CS-NPs released the RS in controlled manner with Fickian diffusion mode. Maximum concentration of RS in plasma was 1240 ng/ml at 4 h for RP12, and 403.8 ng/ml at 2 h for RS sample. RS loaded CS-NPs significantly reduced the stereotypy score in experimental animals that indicated the efficiency of CS-NPs in delivery of RS at brain tissues and moreover amphetamine effect was reversed. Thus, RS loaded CS-NPs proved as potential delivery systems against induced psychotic disorders. Conclusion: Risperidone loaded chitosan nanoparticles were effective against schizophrenia via intranasal route.

Published

2019

24. Effect of minor manufacturing changes on stability of compositionally equivalent PLGA microspheres.

Author

Andhariya JV, Shen J, Wang Y, Choi S, and Burgess DJ

Subjects

Drug Compounding, Drug Liberation, Drug Stability, Drug Storage, Particle Size, Porosity, Microspheres, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Risperidone chemistry

Abstract

The physicochemical properties and drug release characteristics of Q1/Q2 equivalent microspheres are sensitive to minor manufacturing changes, which may alter their stability under different storage-conditions. This may be undesirable due to the presence of a substantial amount of drug in microsphere products. Hence, the objective of the present work was to investigate the impact of minor manufacturing changes on the stability of Q1/Q2 equivalent microspheres under various storage conditions. Two Q1/Q2 equivalent risperidone microsphere formulations prepared with minor manufacturing changes (solvent system etc.) showed differences in their physicochemical properties (size, morphology, porosity etc.), drug release characteristics and hence, storage stability. Overall, both formulations were stable under long-term storage conditions (4 °C/ambient humidity). However, under the intermediate storage conditions (25 °C/ambient humidity), only formulation 1 was stable while formulation 2 showed significant polymer degradation, particle aggregation and alteration in the drug release characteristics. Lastly, under accelerated storage conditions (40 °C/ambient humidity vs 75% RH), the extent of polymer degradation, morphological changes and alteration of drug release characteristics of formulation 2 was significantly higher compared to that of formulation 1. Thus, minor manufacturing changes have the potential to significantly alter the storage stability and, hence, the quality and performance of complex drug products such as microspheres., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

25. Revised Pharmacophore Model for 5-HT 2A Receptor Antagonists Derived from the Atypical Antipsychotic Agent Risperidone.

Author

Shah UH, Gaitonde SA, Moreno JL, Glennon RA, Dukat M, and González-Maeso J

Subjects

Antipsychotic Agents metabolism, HEK293 Cells, Humans, Ketanserin metabolism, Models, Chemical, Receptor, Serotonin, 5-HT2A metabolism, Risperidone metabolism, Tryptamines metabolism, Antipsychotic Agents chemistry, Receptor, Serotonin, 5-HT2A chemistry, Risperidone chemistry

Abstract

Pharmacophore models for 5-HT 2A receptor antagonists consist of two aromatic/hydrophobic regions at a given distance from a basic amine. We have previously shown that both aromatic/hydrophobic moieties are unnecessary for binding or antagonist action. Here, we deconstructed the 5-HT 2A receptor antagonist/serotonin-dopamine antipsychotic agent risperidone into smaller structural segments that were tested for 5-HT 2A receptor affinity and function. We show, again, that the entire risperidone structure is unnecessary for retention of affinity or antagonist action. Replacement of the 6-fluoro-3-(4-piperidinyl)-1,2-benz[ d]isoxazole moiety by isosteric tryptamines resulted in retention of affinity and antagonist action. Additionally, 3-(4-piperidinyl)-1,2-benz[ d]isoxazole (10), which represents less than half the structural features of risperidone, retains both affinity and antagonist actions. 5-HT 2A receptor homology modeling/docking studies suggest that 10 binds in a manner similar to risperidone and that there is a large cavity to accept various N 4 -substituted analogues of 10 such as risperidone and related agents. Alterations of this "extended" moiety improve receptor binding and functional potency. We propose a new risperidone-based pharmacophore for 5-HT 2A receptor antagonist action.

Published

2019

26. Liquid jet breakup: A new method for the preparation of poly lactic-co-glycolic acid microspheres.

Author

Xia Y, Yuan M, Chen M, Li J, Ci T, and Ke X

Subjects

Chemistry, Pharmaceutical methods, Delayed-Action Preparations, Drug Compounding methods, Drug Liberation, Microspheres, Particle Size, Risperidone chemistry, Surface Tension, Viscosity, Drug Carriers chemistry, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Risperidone administration & dosage, Technology, Pharmaceutical methods

Abstract

The purpose of this study was to apply the phenomenon of liquid jet breakup to the preparation of sustained-release microspheres. The mechanisms of liquid jet breakup in different jet states were investigated and the single factor method was used to study the effect of each process parameter on the particle size and size distribution of microspheres. Meantime, the prepared microspheres were characterized by morphology, drug loading, encapsulation efficiency and in vitro release. The results indicated that the process of liquid jet breakup could have 5 different states. The laminar flow state dominated when the Reynolds number (Re) was low, and the prepared microspheres had larger particle sizes. When the Re was high, the turbulent state was dominant and the microspheres had smaller particle sizes. And during the transition state from the laminar flow to the turbulence, the microspheres had a wide particle size distribution. Different process parameters could affect the particle size and distribution of microspheres by changing the Re, surface tension coefficient and viscosity. The microspheres prepared by liquid jet breakup were smooth and round with the drug loading of 35% and the encapsulation efficiency of 88%. In addition, when the polymeric carrier materials were different, the microspheres could have various drug release models such as sustained release with a lag phase, sustained release with no lag phase, pulsed release and so on, which could be applied widespread in the future., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

27. Structures of the 5-HT 2A receptor in complex with the antipsychotics risperidone and zotepine.

Author

Kimura KT, Asada H, Inoue A, Kadji FMN, Im D, Mori C, Arakawa T, Hirata K, Nomura Y, Nomura N, Aoki J, Iwata S, and Shimamura T

Subjects

Humans, Hydrophobic and Hydrophilic Interactions, Molecular Structure, Protein Structure, Secondary, Antipsychotic Agents chemistry, Antipsychotic Agents metabolism, Dibenzothiepins chemistry, Dibenzothiepins metabolism, Receptor, Serotonin, 5-HT2A chemistry, Receptor, Serotonin, 5-HT2A metabolism, Risperidone chemistry, Risperidone metabolism

Abstract

Many drugs target the serotonin 2A receptor (5-HT 2A R), including second-generation antipsychotics that also target the dopamine D 2 receptor (D 2 R). These drugs often produce severe side effects due to non-selective binding to other aminergic receptors. Here, we report the structures of human 5-HT 2A R in complex with the second-generation antipsychotics risperidone and zotepine. These antipsychotics effectively stabilize the inactive conformation by forming direct contacts with the residues at the bottom of the ligand-binding pocket, the movements of which are important for receptor activation. 5-HT 2A R is structurally similar to 5-HT 2C R but possesses a unique side-extended cavity near the orthosteric binding site. A docking study and mutagenic studies suggest that a highly 5-HT 2A R-selective antagonist binds the side-extended cavity. The conformation of the ligand-binding pocket in 5-HT 2A R significantly differs around extracellular loops 1 and 2 from that in D 2 R. These findings are beneficial for the rational design of safer antipsychotics and 5-HT 2A R-selective drugs.

Published

2019

28. Formulation and Evaluation of Neuroactive Drug Loaded Chitosan Nanoparticle for Nose to Brain Delivery: In-vitro Characterization and In-vivo Behavior Study.

Author

Qureshi M, Aqil M, Imam SS, Ahad A, and Sultana Y

Subjects

Administration, Intranasal, Animals, Antipsychotic Agents chemistry, Antipsychotic Agents pharmacokinetics, Behavior, Animal drug effects, Catalepsy chemically induced, Chitosan chemistry, Chitosan pharmacokinetics, Drug Carriers chemistry, Drug Carriers pharmacokinetics, Drug Compounding, Drug Liberation, Locomotion drug effects, Nanoparticles chemistry, Rats, Risperidone chemistry, Risperidone pharmacokinetics, Swine, Antipsychotic Agents administration & dosage, Brain metabolism, Chitosan administration & dosage, Drug Carriers administration & dosage, Nanoparticles administration & dosage, Nasal Mucosa metabolism, Risperidone administration & dosage

Abstract

Background: The present work was designed to explore the efficacy of neuroactive drug (risperidone) loaded chitosan lipid nanoparticle (RIS-CH-LNPs) to enhance the bioactivity in schizophrenia via the nasal route., Methods: The three-factor and three-level formulation by design approach was used for optimization and their effects were observed on (Y1) size in nm, (Y2) % drug loading, and (Y3) % drug release. The optimized formulation RIS-CH-LNPopt was further evaluated for its surface morphology, ex-vivo permeation study, in-vivo behavior study, and stability study. The developed RIS-CH-LNPs showed nanometric size range with high drug loading and prolonged drug release., Results: The optimized formulation (RIS-CH-LNPopt) has shown the particle size (132.7 nm), drug loading (7.6 %), drug release (80.7 %) and further ex-vivo permeation study showed 2.32 fold enhancement over RIS-SUS(suspension). In-vivo behavior studies showed that RIS-CH-LNPopt is able to show significant greater bioefficacy as compared to RIS-SUS [intranasal (i.n), intravenous (i.v)]. The pharmacokinetic and brain/plasma ratio of developed chitosan nanoparticle was higher at all time-points as compared to RIS-SUS either given by intranasal or intravenous route that proves the direct nose to brain transport pathway of the drug via nasal administration. The developed chitosan nanoparticle increases nose to brain drug delivery as compared to the dispersion of equivalent dose., Conclusion: The findings of this study substantiate the existence of a direct nose-to-brain delivery route for RIS-CH-LNPs., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2019

29. Influence of drying processes on the structures, morphology and in vitro release profiles of risperidone-loaded PLGA microspheres.

Author

Wu Z, Zhao M, Zhang W, Yang Z, Xu S, and Shang Q

Subjects

Desiccation, Drug Compounding, Drug Liberation, Freeze Drying, Kinetics, Porosity, Risperidone administration & dosage, Serotonin Antagonists administration & dosage, Drug Carriers chemistry, Polylactic Acid-Polyglycolic Acid Copolymer chemistry, Risperidone chemistry, Serotonin Antagonists chemistry

Abstract

The purpose of this study was to investigate the influences of drying methods on the risperidone (RIS) release profiles of RIS-loaded PLGA microspheres. These microspheres were fabricated with an O/W emulsion solvent evaporation method. The wet microspheres were dried with freeze drying and vacuum drying methods. The microspheres were mono-dispersed spheres with an average diameter of 100 μm. Studies found that drying methods had great influence on the porosity, morphology, and release profiles of RIS-loaded PLGA microspheres. Specifically, the freeze-dried microspheres had higher porosity (78.46 ± 1.64%) than those vacuum-dried ones (52.45 ± 2.68%), and they showed higher RIS release rates ( p  < 0.05). In the accelerated release tests (45 °C), these microspheres dried under the pressures of 700 mmHg and 200 mmHg gave faster release rates than those ones dried under the pressure of 450 mmHg. Importantly, the accelerated release test (45 °C) had a high correlation with the real-time test (37 °C) ( R 2  > 0.99). These studies exhibited a significance in the precise preparation of RIS-loaded PLGA microspheres.

Published

2019

30. Preparation of New Risperidone Depot Microspheres Based on Novel Biocompatible Poly(Alkylene Adipate) Polyesters as Long-Acting Injectable Formulations.

Author

Nanaki S, Barmpalexis P, Papakonstantinou Z, Christodoulou E, Kostoglou M, and Bikiaris DN

Subjects

Adipates chemical synthesis, Biocompatible Materials chemical synthesis, Butylene Glycols chemical synthesis, Delayed-Action Preparations chemical synthesis, Drug Liberation, Injections, Particle Size, Polyesters chemical synthesis, Polymers chemical synthesis, Polypropylenes chemical synthesis, Risperidone chemistry, Serotonin Antagonists chemistry, Solubility, Adipates chemistry, Biocompatible Materials chemistry, Butylene Glycols chemistry, Delayed-Action Preparations chemistry, Polyesters chemistry, Polymers chemistry, Polypropylenes chemistry, Risperidone administration & dosage, Serotonin Antagonists administration & dosage

Abstract

Risperidone (RIS)-loaded microspheres based on poly(alkylene adipate)s derived from dicarboxylic acids and different aliphatic diols were prepared by the oil in water emulsion and solvent evaporation method. Specifically, 3 polyesters, namely poly(ethylene adipate), poly(propylene adipate), and poly(butylene adipate), were prepared with the aid of a 2-stage melt-polycondensation method and characterized by gel permeation chromatography, proton nuclear magnetic resonance ( 1 H NMR), differential scanning calorimetry, and X-ray diffraction analysis. Results showed that the molecular weight of the polyesters increased as the diol molecular weight increased, while all polymers were of semi-crystalline nature and the melting temperature was varying from 49.1°C to 51.8°C and 65.9°C for poly(propylene adipate), poly(ethylene adipate), and poly(butylene adipate), respectively. The particle size of the RIS-loaded microspheres varied from 10 to 100 μm depending on the polyester type and the drug loading, while X-ray diffraction analysis revealed amorphous active pharmaceutical ingredient in the cases of high drug-loaded microspheres. In vitro drug release studies along with scanning electron microscopy images of microspheres after the completion of dissolution process showed that in all cases RIS release was controlled by the glass transition temperature of polyesters and physical state of active pharmaceutical ingredients via diffusion., (Copyright © 2018 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2018

31. Formulation of delivery systems with risperidone based on biodegradable terpolymers.

Author

Turek A, Borecka A, Janeczek H, Sobota M, and Kasperczyk J

Subjects

Delayed-Action Preparations chemistry, Drug Compounding, Drug Liberation, Antipsychotic Agents chemistry, Drug Delivery Systems, Polyesters chemistry, Risperidone chemistry

Abstract

Risperidone is applied in oral dosage formulations in the treatment of mental diseases. Current trends point toward parenteral delivery systems based on poly(lactide-co-glycolide), with wafers or rods being the more attractive option than the routinely used intramuscular suspension with microparticles. The aim of our work was to study the utility of solution casting and hot melt extrusion in the formulation of wafers and rods with risperidone based on terpolymers, namely poly(lactide-co-glycolide-co-trimethylene carbonate) and poly(lactide-co-glycolide-co-ε-caprolactone). Synthesis of the terpolymers was carried out by using a non-toxic zirconium initiator and a racemic (LL/DD) or optically active form of the lactide monomer. The delivery systems were analyzed by NMR, DSC, GPC, and SEM. The release profile was monitored by HPLC. Terpolymer chain microstructure, glass transition temperature, and morphology revealed unchanged values after formulation. Solution casting resulted in a drop in molecular weight to a smaller degree than hot melt extrusion. The presence of risperidone influenced another decrease in molecular weight. Both methods are adequate for the formulation of delivery systems based on terpolymers for prolonged release of risperidone. An adequate selection of monomer composition in terpolymers allows to control the release period. Risperidone was released in three phases, however, the burst effect was observed for poly(L-lactide-co-glycolide-co-ε-caprolactone)., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

32. Nanocrystal-based drug delivery system of risperidone: lyophilization and characterization.

Author

Gol D, Thakkar S, and Misra M

Subjects

Chemistry, Pharmaceutical methods, Drug Delivery Systems methods, Drug Stability, Freeze Drying methods, Particle Size, Poloxamer chemistry, Polyesters chemistry, Solubility, Solvents chemistry, Surface-Active Agents chemistry, Suspensions chemistry, Nanoparticles chemistry, Risperidone chemistry

Abstract

Objective: In the present work nanocrystal-based formulation of risperidone (RIS) was proposed to overcome solubility issue of RIS, while lyophilization technique was used effectively, for conversion of RIS nanosuspension to solid state., Significance: RIS nanosuspension was developed and stabilized with a combination of polycaprolactone and Pluronic ® F-68 as stabilizers. With focus on critical parameters like nature of cryoprotectants and effect of eutectic temperature on properties of nanosuspension, the suitability of lyophilization technique in improving the physical stability of prepared nanosuspension was also evaluated. Additionally, the developed nanocrystals were also assessed for their solid states properties., Methods: Various process parameters affecting average particle size and polydispersity index (PDI), viz. drug to surfactant ratio, solvent to anti-solvent ratio, stirring speed, type of stabilizer were optimized. Assessment of lyophilization as a suitable solidification technique (for conversion to powder form) was done with selective cryoprotectants (trehalose dihydrate and sorbitol)., Results: The formulation was found to be stable at 4 °C for 3 months with size, PDI and zeta potential of 214 ± 3.4 nm, 0.120, and -10.2 ± 0.90 mV, respectively. Release profile of developed nanosuspension showed cumulative % release of ∼90% in initial 10 h whereas the value for the unprocessed drug was ∼11% in same time frame., Conclusions: These findings suggest that developed formulation was able to enhance water solubility of the drug effectively and can be potentially used in the management of psychotic disorders.

Published

2018

33. Classics in Chemical Neuroscience: Risperidone.

Author

Chopko TC and Lindsley CW

Subjects

Animals, Humans, Mental Disorders drug therapy, Risperidone adverse effects, Risperidone chemistry, Risperidone pharmacology, Serotonin Antagonists adverse effects, Serotonin Antagonists chemistry, Serotonin Antagonists pharmacology, Risperidone therapeutic use, Serotonin Antagonists therapeutic use

Abstract

After the identification of the influence of serotonergic receptors in ameliorating the negative symptoms associated with schizophrenia, atypical antipsychotics were developed by incorporating dopamine and serotonin antagonism. Risperidone, sold under the trade name Risperdal, was the second atypical antipsychotic developed following clozapine but quickly became a first-line treatment for acute and chronic schizophrenia because of its preferential side effect profile. Despite initial Food and Drug Administration approval 25 years ago, risperidone continues to be a fundamental treatment for schizophrenia, bipolar I disorder, and autism-related irritability. It is on the World Health Organization's List of Essential Medicines for its balance of efficacy, safety, tolerability, and cost-effectiveness. In this review, we highlight the history and importance of risperidone as an atypical antipsychotic, in addition to its chemical synthesis, manufacturing, drug metabolism and pharmacokinetics, pharmacology, structure-activity relationship, indications, and adverse effects.

Published

2018

34. Quantitative determination of risperidone, paliperidone and olanzapine in human serum by liquid chromatography-tandem mass spectrometry coupled with on-line solid-phase extraction.

Author

Ruan CJ, Guo W, Zhou M, Guo GX, Wang CY, Li WB, and de Leon J

Subjects

Benzodiazepines chemistry, Benzodiazepines isolation & purification, Drug Stability, Humans, Limit of Detection, Linear Models, Olanzapine, Paliperidone Palmitate chemistry, Paliperidone Palmitate isolation & purification, Reproducibility of Results, Risperidone chemistry, Risperidone isolation & purification, Benzodiazepines blood, Chromatography, High Pressure Liquid methods, Paliperidone Palmitate blood, Risperidone blood, Solid Phase Extraction methods, Tandem Mass Spectrometry methods

Abstract

A recent guideline recommends therapeutic drug monitoring for risperidone, paliperidone and olanzapine, which are frequently used second-generation antipsychotics. We developed a simple high-performance liquid chromatography-tandem mass spectrometry coupled with an online solid-phase extraction method that can be used to measure risperidone, paliperidone and olanzapine using small (40 μL) samples. The analytes were extracted from serum samples automatically pre-concentrated and purified by C 8 (5 μm, 2.1 × 30 mm) solid-phase extraction cartridges, then chromatographed on an Xbidge™ C 18 column (3.5 μm, 100 × 2.1 mm) thermostatted at 30°C with a mobile phase consisting of 70% acetonitrile and 30% ammonium hydroxide 1% solution at an isocratic flow rate of 0.3 mL/min, and detected with tandem mass spectrometry. The assay was validated in the concentration range from 2.5 to 160 ng/mL. Intra- and inter-day precision for all analytes was between 1.1 and 8.2%; method accuracy was between 6.6 and 7.6%. The risperidone and paliperidone assay was compared with a high-performance liquid chromatography-ultraviolet assay currently used in our hospital for risperidone and paliperidone therapeutic drug monitoring, and the results of weighted Deming regression analysis showed good agreement. For the olanzapine assay, we compared 20 samples in separate re-assays on different days; all the relative errors were within the 20% recommended limit., (Copyright © 2018 John Wiley & Sons, Ltd.)

Published

2018

35. A water-compatible magnetic molecularly imprinted polymer for the selective extraction of risperidone and 9-hydroxyrisperidone from human urine.

Author

Ji WH, Guo YS, Wang X, and Guo DS

Subjects

Chromatography, High Pressure Liquid, Humans, Magnetics, Microscopy, Electron, Paliperidone Palmitate chemistry, Paliperidone Palmitate urine, Reproducibility of Results, Risperidone chemistry, Risperidone urine, Solid Phase Extraction methods, Water chemistry, Molecular Imprinting, Paliperidone Palmitate isolation & purification, Polymers chemistry, Risperidone isolation & purification

Abstract

An accurate, rapid, and sensitive method for the determination of risperidone and 9-hydroxyrisperidone in urine samples was developed by combining water-compatible magnetic molecularly imprinted solid-phase extraction with high performance liquid chromatography. Several variables relating to the efficiency of magnetic solid phase extraction were optimized, including the amount of adsorbent, adsorption time, type of elution solvent, and desorption time. The analytical performance of this method was validated under the optimized conditions. The linearity for risperidone and 9-hydroxyrisperidone was obtained in the range 1-2000ngmL -1 with correlation coefficient ≥ 0.991. Limits of detection of risperidone and 9-hydroxyrisperidone are 0.21ngmL -1 and 0.24ngmL -1 , respectively. Recoveries at three spike levels (10, 100, and 1000ngmL -1 ) ranged from 94.6% to 102.4% with relative standard deviations (%) ≤ 5.3. These results confirmed that this method can be successfully and facilely used to analyze the multi-residues of risperidone and 9-hydroxyrisperidone in urine samples with high efficiency and good sensitivity., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

36. Structure of the D2 dopamine receptor bound to the atypical antipsychotic drug risperidone.

Author

Wang S, Che T, Levit A, Shoichet BK, Wacker D, and Roth BL

Subjects

Binding Sites, Crystallography, X-Ray, Drug Design, Humans, Hydrophobic and Hydrophilic Interactions, Kinetics, Ligands, Models, Molecular, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Mutation, Receptors, Dopamine D2 genetics, Receptors, Dopamine D3 chemistry, Receptors, Dopamine D3 metabolism, Receptors, Dopamine D4 chemistry, Receptors, Dopamine D4 metabolism, Antipsychotic Agents chemistry, Antipsychotic Agents metabolism, Receptors, Dopamine D2 chemistry, Receptors, Dopamine D2 metabolism, Risperidone chemistry, Risperidone metabolism

Abstract

Dopamine is a neurotransmitter that has been implicated in processes as diverse as reward, addiction, control of coordinated movement, metabolism and hormonal secretion. Correspondingly, dysregulation of the dopaminergic system has been implicated in diseases such as schizophrenia, Parkinson's disease, depression, attention deficit hyperactivity disorder, and nausea and vomiting. The actions of dopamine are mediated by a family of five G-protein-coupled receptors. The D2 dopamine receptor (DRD2) is the primary target for both typical and atypical antipsychotic drugs, and for drugs used to treat Parkinson's disease. Unfortunately, many drugs that target DRD2 cause serious and potentially life-threatening side effects due to promiscuous activities against related receptors. Accordingly, a molecular understanding of the structure and function of DRD2 could provide a template for the design of safer and more effective medications. Here we report the crystal structure of DRD2 in complex with the widely prescribed atypical antipsychotic drug risperidone. The DRD2-risperidone structure reveals an unexpected mode of antipsychotic drug binding to dopamine receptors, and highlights structural determinants that are essential for the actions of risperidone and related drugs at DRD2.

Published

2018

37. An Accelerated Release Method of Risperidone Loaded PLGA Microspheres with Good IVIVC.

Author

Hu X, Zhang J, Tang X, Li M, Ma S, Liu C, Gao Y, Zhang Y, Liu Y, Yu F, Yang Y, Guo J, Li Z, and Mei X

Subjects

Animals, Ethanol chemistry, Hydrogen-Ion Concentration, Least-Squares Analysis, Microspheres, Osmotic Pressure, Polylactic Acid-Polyglycolic Acid Copolymer, Rats, Rats, Sprague-Dawley, Risperidone administration & dosage, Temperature, Drug Liberation, Lactic Acid chemistry, Polyglycolic Acid chemistry, Risperidone chemistry, Risperidone pharmacokinetics

Abstract

Background: A long release period lasting several days or several weeks is always needed and thereby it is tedious and time consuming to screen formulations of such microspheres with so long release period and evaluate their release profiles in vitro with conventional long-term or "real-time" release method. So, an accelerated release testing of such system is necessary for formulation design as well as quality control purpose. The purpose of this study is to obtain an accelerated release method of risperidone loaded poly(lactic-co-glycolic acid) (PLGA) microspheres with good in vitro/in vivo correlation (IVIVC)., Methods: Two formulations of risperidone loaded PLGA microspheres used for evaluating IVIVC were prepared by O/W method. The accelerated release condition was optimized by investigating the effect of pH, osmotic pressure, temperature and ethanol concentration on the release of risperidone from microspheres and the in vitro accelerated release profiles of risperidone from PLGA microspheres were obtained under this optimized accelerated release condition. The plasma concentration of risperidone were also detected after subcutaneous injection of risperidone loaded microspheres to rats. The in vivo cumulative absorption profiles were then calculated using Wagner-Nelson model, Loo- Riegelman model and numerical convolution model, respectively. The correlation between in vitro accelerated release and in vivo cumulative absorption were finally evaluated with Least Square Method., Results: It was shown that temperature and ethanol concentration significantly affected the release of risperidone from the microspheres while pH and osmotic pressure of release media slightly affected the release behavior of risperidone. The in vitro release of risperidone from microspheres were finally undergone in PBS (pH7.0, 300mosm) with 20% (V/V) ethanol at 45°C. The sustained and complete release of risperidone was observed in both formulations under the accelerated release condition although these two release profiles were dissimilar. The correlation coefficients (R2) of IVIVC were all above 0.95 and the slopes were all between 0.9564 and 1.1868 in spite of fitted model and microsphere formulation., Conclusion: An in vitro accelerated release method of risperidone microspheres with good IVIVC was established in this paper and this accelerated release method was supposed to have great potential in both in vivo performance prediction and quality control for risperidone loaded PLGA microspheres., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2018

38. Beyond Q1/Q2: The Impact of Manufacturing Conditions and Test Methods on Drug Release From PLGA-Based Microparticle Depot Formulations.

Author

Garner J, Skidmore S, Park H, Park K, Choi S, and Wang Y

Subjects

Chemistry, Pharmaceutical methods, Drug Carriers chemistry, Drug Compounding methods, Kinetics, Microspheres, Polylactic Acid-Polyglycolic Acid Copolymer, Drug Liberation drug effects, Lactic Acid chemistry, Polyglycolic Acid chemistry, Risperidone chemistry

Abstract

Drug-loaded polymeric microparticles have been used as long-acting injectable (LAI) depot formulations. To obtain U.S. Food and Drug Administration approval, a generic LAI depot product needs to be qualitatively (Q1) and quantitatively (Q2) the same in terms of inactive ingredients as its reference-listed drug. However, Q1/Q2 sameness as the reference-listed drug does not guarantee the same in vitro drug release profile and in vivo performance, especially when the manufacturing methods are different. There is little consensus on how the in vitro testing needs to be done to examine the release profiles of LAI depot formulations. This study examined the manufacturing differences in making risperidone-loaded poly(lactide-co-glycolide) microparticles and their impact on the release kinetics. It also examined the impacts of in vitro testing methods on the drug release profiles. Two in-house manufactured risperidone poly(lactide-co-glycolide) microparticles and Risperdal Consta ® were used in the study. Of the in vitro release methods tested, the orbital agitation method provided the most reproducible release profiles. The results indicate that the in vitro release kinetics depend not only on manufacturing procedures but also on the in vitro testing conditions, such as the agitation speed, vessel-dimensions, solid beads, media exchange volume, and other parameters both under real-time and accelerated testing conditions. In the current case, the in vitro experimental condition seemed to affect the drug release kinetics more than the manufacturing differences. The developed orbital agitation release testing method is simple, robust, and reproducible, which allows the comparison of in vitro release profiles of formulations that are prepared with manufacturing differences., (Copyright © 2018 American Pharmacists Association®. All rights reserved.)

Published

2018

39. The Screening of Anticholinergic Accumulation by Traditional Chinese Medicine.

Author

Zhang M, Vrolijk M, and Haenen GRMM

Subjects

Animals, Atropine chemistry, Atropine pharmacology, Cimetidine chemistry, Cimetidine pharmacology, Drugs, Chinese Herbal chemistry, Ephedra sinica chemistry, Humans, Male, Muscarinic Antagonists chemistry, Pirenzepine chemistry, Rats, Rats, Inbred WKY, Risperidone chemistry, Risperidone pharmacology, Theophylline chemistry, Theophylline pharmacology, Drugs, Chinese Herbal pharmacology, Medicine, Chinese Traditional, Muscarinic Antagonists pharmacology, Receptors, Cholinergic metabolism

Abstract

Many Western drugs can give rise to serious side effects due to their ability to bind to acetylcholine receptors in the brain. This aggravates when they are combined, which is known as anticholinergic accumulation (AA). Some bioactives in Traditional Chinese Medicine (TCM) are known to block acetylcholine receptors and thus potentially cause AA. The AA of TCM was screened by quantifying the displacement of [³H] pirenzepine on acetylcholine receptors in a rat brain homogenate. We used a new unit to express AA, namely the Total Atropine Equivalents (TOAT). The TOAT of various herbs used in TCM was very diverse and even negative for some herbs. This is indicative for the broadness of the pallet of ingredients used in TCM. Three TCM formulas were screened for AA: Ma Huang Decotion (MHD), Antiasthma Simplified Herbal Medicine intervention (ASHMI), and Yu Ping Feng San (YPFS). The TOAT of ASHMI was indicative for an additive effect of herbs used in it. Nevertheless, it can be calculated that one dose of ASHMI is probably too low to cause AA. The TOAT of YPFS was practically zero. This points to a protective interaction of AA. Remarkably, MHD gave a negative TOAT, indicating that the binding to the acetylcholine receptors was increased, which also circumvents AA. In conclusion, our results indicate that TCM is not prone to give AA and support that there is an intricate interaction between the various bioactives in TCM to cure diseases with minimal side effects., Competing Interests: The authors declare no conflict of interest.

Published

2017

40. Discriminative stimulus properties of the atypical antipsychotic amisulpride: comparison to its isomers and to other benzamide derivatives, antipsychotic, antidepressant, and antianxiety drugs in C57BL/6 mice.

Author

Donahue TJ, Hillhouse TM, Webster KA, Young R, De Oliveira EO, and Porter JH

Subjects

Amisulpride, Animals, Anti-Anxiety Agents chemistry, Antidepressive Agents chemistry, Antipsychotic Agents chemistry, Benzamides chemistry, Chlorpromazine chemistry, Chlorpromazine pharmacology, Clozapine chemistry, Clozapine pharmacology, Conditioning, Operant drug effects, Conditioning, Operant physiology, Discrimination Learning physiology, Male, Mice, Mice, Inbred C57BL, Quetiapine Fumarate chemistry, Quetiapine Fumarate pharmacology, Risperidone chemistry, Risperidone pharmacology, Sulpiride chemistry, Sulpiride pharmacology, Anti-Anxiety Agents pharmacology, Antidepressive Agents pharmacology, Antipsychotic Agents pharmacology, Benzamides pharmacology, Discrimination Learning drug effects, Sulpiride analogs & derivatives

Abstract

Rationale: Racemic (RS)-amisulpride (Solian ® ) is an atypical antipsychotic drug used to treat schizophrenia and dysthymia. Blockade of dopamine D 2 /D 3 and/or serotonin 5-HT 7 receptors is implicated in its pharmacological effects. While the (S)-amisulpride isomer possesses a robust discriminative cue, discriminative stimulus properties of (RS)-amisulpride have not been evaluated., Objectives: The present study established (RS)-amisulpride as a discriminative stimulus and assessed amisulpride-like effects of amisulpride stereoisomers, other benzamide derivatives, and antipsychotic, antidepressant, and anxiolytic drugs., Methods: Adult, male C57BL/6 mice were trained to discriminate 10 mg/kg (RS)-amisulpride from vehicle in a two-lever food-reinforced operant conditioning task., Results: (RS)-Amisulpride's discriminative stimulus was dose-related, time-dependent, and stereoselective. (S)-Amisulpride (an effective dose of 50% (ED 50 ) = 0.21 mg/kg) was three times more potent than (RS)-amisulpride (ED 50  = 0.60 mg/kg) or (R)-amisulpride (ED 50  = 0.68 mg/kg). (RS)-Amisulpride generalized fully to the structurally related atypical antipsychotic/antidysthymia drug sulpiride (Sulpor ® ; ED 50  = 7.29 mg/kg) and its (S)-enantiomer (ED 50  = 9.12 mg/kg); moderate to high partial generalization [60-75% drug lever responding (%DLR)] occurred to the benzamide analogs tiapride (Tiapridal ® ) and raclopride, but less than 60% DLR to metoclopramide (Reglan ® ), nemonapride (Emilace ® ), and zacopride. Antipsychotic, antidepressant, and antianxiety drugs from other chemical classes (chlorpromazine, quetiapine, risperidone, and mianserin) produced 35-55% amisulpride lever responding. Lastly, less than 35% DLR occurred for clozapine, olanzapine, aripiprazole imipramine, chlordiazepoxide, and bupropion., Conclusions: (RS)-Amisulpride generalized to some, but not all benzamide derivatives, and it failed to generalize to any other antipsychotic, antidepressant, or antianxiety drugs tested. Interestingly, the (R)-isomer shared very strong stimulus properties with (RS)-amisulpride. This finding was in contrast to findings from Donahue et al. (Eur J Pharmacol 734:15-22, 2014), which found that the (R)-isomer did not share very strong stimulus properties when the (S)-isomer was the training drug.

Published

2017

41. Parenteral nanoemulsions of risperidone for enhanced brain delivery in acute psychosis: Physicochemical and in vivo performances.

Author

Đorđević SM, Santrač A, Cekić ND, Marković BD, Divović B, Ilić TM, Savić MM, and Savić SD

Subjects

Animals, Antipsychotic Agents blood, Antipsychotic Agents chemistry, Antipsychotic Agents pharmacokinetics, Biological Availability, Blood Proteins metabolism, Brain metabolism, Drug Delivery Systems, Emulsions, Lecithins chemistry, Liver metabolism, Locomotion drug effects, Male, Nanostructures chemistry, Oleic Acid chemistry, Polysorbates chemistry, Psychotic Disorders drug therapy, Psychotic Disorders metabolism, Rats, Wistar, Risperidone blood, Risperidone chemistry, Risperidone pharmacokinetics, Tissue Distribution, Antipsychotic Agents administration & dosage, Nanostructures administration & dosage, Risperidone administration & dosage

Abstract

This work aimed to deepen the lately acquired knowledge about parenteral nanoemulsions as carriers for brain delivery of risperidone, a poorly water-soluble antipsychotic drug, through establishing the prospective relationship between their physicochemical, pharmacokinetic, biodistribution, and behavioral performances. For this purpose, two optimized risperidone-loaded nanoemulsions, stabilized by lecithin or lecithin/polysorbate 80 mixture, and costabilized by sodium oleate, were produced by high-pressure homogenization. The characterization revealed the favorable droplet size, narrow size distribution, high surface charge, with proven stability to autoclaving and long-term stability for at least one year at 25±2°C. Pharmacokinetic and tissue distribution results demonstrated improved plasma, liver, and brain pharmacokinetic parameters, resulting in 1.2-1.5-fold increased relative bioavailability, 1.1-1.8-fold decreased liver distribution, and about 1.3-fold improved brain uptake of risperidone active moiety following intraperitoneal administration of nanoemulsions relative to solution in rats. In behavioral study, investigated nanoemulsions showed pronounced reduction in basal and, more pertinently, amphetamine-induced locomotor activity in rats, with an early onset of antipsychotic action, and this effect lasted at least 90min after drug injection. Together, these findings corroborate the applicability of parenteral nanoemulsions as carriers for enhanced brain delivery of risperidone, further suggesting their promise in acute psychosis treatment or other emergency situations., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

42. Risperidone mucoadhesive buccal tablets: formulation design, optimization and evaluation.

Author

Çelik B

Subjects

Administration, Buccal, Drug Delivery Systems, Humans, Risperidone administration & dosage, Risperidone therapeutic use, Schizophrenia drug therapy, Tablets, Drug Compounding, Risperidone chemistry

Abstract

The aim of this study was to design and optimize risperidone (RIS) mucoadhesive buccal tablets for systemic delivery as an alternative route. Direct compression method was used for the preparation of buccal tablets, and screening studies were conducted with different polymers to determine their effects on tablet characteristics. Carbopol ® (CP) and sodium alginate (SA) were selected as two polymer types for further optimization studies by applying response surface methodology. Tablet hardness (TH), ex vivo residence time (RT), and peak detachment force (DF) from buccal mucosa were selected as three important responses. Physicochemical compatibility of formulation excipients and RIS was evaluated by using Fourier transform infrared (FT-IR) spectroscopy and differential scanning calorimetry (DSC) analysis. In vitro drug release profiles and release kinetics were investigated; swelling index and matrix erosion studies were conducted. Optimum formulation consisted of 16.4% CP and 20.3% SA, which provided 7.67±0.29 hour ex vivo RT, 45.52±4.85 N TH, and 2.12±0.17 N DF. FT-IR spectroscopy and DSC analysis revealed that there was no chemical interaction present between tablet ingredients. Cumulative RIS release of >90% was achieved after 8 hours of in vitro dissolution studies, which was supported by swelling and matrix erosion analysis. Mechanism of RIS release was fitted best to zero-order model, while release exponent (n) value of 0.77 demonstrated an anomalous (non-Fickian) release, indicating combined erosion and swelling mechanism. The results suggested that optimized buccal tablets of RIS would be a promising and alternative delivery system for the treatment of schizophrenia., Competing Interests: Disclosure The author reports no conflicts of interest in this work and is responsible for the content and writing of this paper.

Published

2017

43. Formation Mechanism and In Vitro Evaluation of Risperidone-Containing PLGA Microspheres Fabricated by Ultrafine Particle Processing System.

Author

Huang Z, Chen X, Fu H, Wen X, Ma C, Zhang J, Wu C, Huang Y, Pan X, and Wu C

Subjects

Antipsychotic Agents chemistry, Diffusion, Drug Compounding methods, Drug Liberation, Microspheres, Particle Size, Polylactic Acid-Polyglycolic Acid Copolymer, Risperidone chemistry, Surface Properties, Viscosity, Antipsychotic Agents administration & dosage, Delayed-Action Preparations chemistry, Lactic Acid chemistry, Polyglycolic Acid chemistry, Risperidone administration & dosage

Abstract

Ultrafine particle processing system (UPPS) was developed previously by our group to provide a new solution to microsphere fabrication. The UPPS was supposed to possess many featured advantages, but the microsphere formation mechanism during UPPS processing was still unknown. The objective of this study was to perform the formation mechanism investigation and in vitro evaluation on risperidone-containing poly(d, l-lactic-co-glycolic acid) microspheres (RIS-PLGA MS) fabricated by UPPS. Evaporation profile and viscosity of the PLGA-containing solutions were considered as the critical factors for the microsphere formation mechanism and were determined in present study. The formation mechanism of RIS-PLGA MS was put forward by semiquantitative analysis on the basis of the evaporation profile, viscosity, and scanning electron microscopy results. It was established that the evaporation profile and viscosity would have an impact on the evaporation velocity and PLGA molecular diffusion velocity during solidification process, resulting in different appearance of the microspheres. Furthermore, comprehensive in vitro evaluations of RIS-PLGA MS were conducted, including particle size distribution, micromeritics, morphology, drug loading, encapsulation efficiency, residual organic solvent, syringeability, and in vitro release behavior. The results revealed that RIS-PLGA MS was a promising candidate for intramuscular administration, and meanwhile UPPS was a qualified technology for microsphere production., (Copyright © 2017 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2017

44. 3-month parenteral PLGA microsphere formulations of risperidone: Fabrication, characterization and neuropharmacological assessments.

Author

Chaurasia S, Mounika K, Bakshi V, and Prasad V

Subjects

Animals, Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Delayed-Action Preparations pharmacology, Drug Evaluation, Preclinical, Female, Male, Polylactic Acid-Polyglycolic Acid Copolymer, Rats, Lactic Acid chemistry, Lactic Acid pharmacokinetics, Lactic Acid pharmacology, Microspheres, Polyglycolic Acid chemistry, Polyglycolic Acid pharmacokinetics, Polyglycolic Acid pharmacology, Risperidone chemistry, Risperidone pharmacokinetics, Risperidone pharmacology

Abstract

The study aims at formulation and characterization of three months parenteral risperidone loaded polymeric microspheres (p-RLPMs) as a sustained delivery system and established their in vitro and in vivo assessments. The p-RLPMs formulations were prepared by solvent extraction and diffusion method. The optimized p-RLPMs (batch R PLGA -1) formulation demonstrated favorable different physicochemical properties such as mean particle size (104±5.34μm), percent porosity (44.56±3.11%) and percent drug loading (38.42±2.67%). The physical state characterization, Fourier transformed infrared spectroscopy analysis showed no changes in the chemical structure of risperidone (RPD) in the batch R PLGA -1 formulation and differential scanning calorimetry study confirmed, pure RPD retained its crystallinity in the batch R PLGA -1 formulation. The SEM micrographs of the all p-RLPMs formulations revealed the irregular shapes and indentations. The GC/MS results showed that the residual organic solvent content in the batch R PLGA -1 formulation was below the limits. Pharmacokinetic parameters revealed that optimized R PLGA -1 formulation exhibited an initial burst followed by an excellent sustained release as compared to pure RPD as well as other formulations. Furthermore, in vivo studies of the batch, R PLGA -1 formulation showed an antipsychotic effect that was significantly prolonged over that of pure RPD solution for up to 72h with fewer extrapyramidal side effects. Thus, results of this study prove the suitability of using poly(lactic-co-glycolic acid) copolymer to develop sustained release p-RLPMs formulations that can tailor in vivo behavior and enhance the pharmacological effectiveness of the RPD., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

45. Formulation by design based risperidone nano soft lipid vesicle as a new strategy for enhanced transdermal drug delivery: In-vitro characterization, and in-vivo appraisal.

Author

Imam SS, Ahad A, Aqil M, Akhtar M, Sultana Y, and Ali A

Subjects

Administration, Cutaneous, Animals, Drug Evaluation, Preclinical, Rats, Drug Carriers chemistry, Drug Carriers pharmacokinetics, Drug Carriers pharmacology, Lipids chemistry, Lipids pharmacology, Nanoparticles chemistry, Risperidone chemistry, Risperidone pharmacokinetics, Risperidone pharmacology

Abstract

The present study was designed to formulate and optimize transdermal risperidone soft lipid vesicles. The formulation optimized with phospholipid, safranal and ethanol were incorporated as permeation and absorption enhancers. The optimized risperidone soft lipid vesicle was further evaluated for skin irritation study, in-vivo pharmacokinetic study and locomotor activity. Three factor three level Box-Behnken design (BBD) was used to statistically optimize soft lipid vesicle using safranal (A), ethanol (B)and phospholipid (C) as independent variable, while their effect was observed for vesicle size (Y 1 ), entrapment efficiency (Y 2 ) and flux (Y 3 ). The optimized risperidone soft lipid vesicle (Ris-opt) showed nanometric vesicle size, high entrapment efficiency and marked enhancement in transdermal flux. The extent of absorption from Ris-opt was greater when compared to oral suspension with relative bioavailability of 177%. The histopathological evaluation revealed developed formulation did not showed skin irritation compared to standard irritant. The significant findings presented here encourage further studies with risperidone soft lipid vesicles for treatment of schizophrenia., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

46. A method to slow down the ionization-dependent release of risperidone loaded in a thermoresponsive poly(N-acryloyl glycinamide) hydrogel.

Author

Boustta M and Vert M

Subjects

Drug Liberation, Hydrogen-Ion Concentration, Solubility, Temperature, Acrylic Resins chemistry, Antipsychotic Agents chemistry, Drug Delivery Systems, Hydrogels chemistry, Risperidone chemistry

Abstract

Poly(N-acryloyl glycinamide) polymers are soluble in hot aqueous media that gel rapidly on cooling. This gelatin-like behavior was previously compared with drug delivery requirements. Slow releases were demonstrated in vitro using different model molecules and macromolecules and in vivo using methylene blue. Risperidone is a weak basic drug sparingly soluble in water frequently used to treat patients suffering of schizophrenia. A standard risperidone-poly(N-acryloyl glycinamide) hydrogel formulation was selected from which the drug was allowed to release comparatively in buffered and non-buffered isotonic media at 37 °C under pseudo sink conditions. Linear release was observed in pH = 7.4 phosphate buffer whereas in buffer-free 0.15 M NaCl, the release was initially faster than in the buffer but became rapidly slower as the pH increased from 6.8 to 8.2. These features were related to the ionization-dependent solubility of risperidone. In order to minimize the ionization and thus the solubility of the drug inside the hydrogel despite outside buffering at 7.4, Mg(OH 2 ), a sparingly soluble mineral base, was added to the standard formulation. This addition resulted in a c.a. threefold increase of the zero-order release duration. The method should be applicable to other sparingly soluble weakly basic drugs.

Published

2017

47. A chemical genomics approach to drug reprofiling in oncology: Antipsychotic drug risperidone as a potential adenocarcinoma treatment.

Author

Dilly SJ, Clark AJ, Marsh A, Mitchell DA, Cain R, Fishwick CWG, and Taylor PC

Subjects

17-Hydroxysteroid Dehydrogenases chemistry, 17-Hydroxysteroid Dehydrogenases genetics, 17-Hydroxysteroid Dehydrogenases metabolism, 3-Hydroxyacyl CoA Dehydrogenases chemistry, 3-Hydroxyacyl CoA Dehydrogenases genetics, 3-Hydroxyacyl CoA Dehydrogenases metabolism, Adenocarcinoma enzymology, Adenocarcinoma genetics, Animals, Antineoplastic Agents chemistry, Antipsychotic Agents chemistry, Bacteriophage T7 genetics, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drosophila melanogaster enzymology, Drosophila melanogaster genetics, Drug Compounding, Enzyme Inhibitors chemistry, Gene Library, Humans, Linoleic Acids, Conjugated chemistry, Male, Mice, Nude, Molecular Docking Simulation, Molecular Targeted Therapy, Prostatic Neoplasms enzymology, Prostatic Neoplasms genetics, Protein Conformation, Risperidone chemistry, Structure-Activity Relationship, Time Factors, Tumor Burden drug effects, Xenograft Model Antitumor Assays, 17-Hydroxysteroid Dehydrogenases antagonists & inhibitors, 3-Hydroxyacyl CoA Dehydrogenases antagonists & inhibitors, Adenocarcinoma drug therapy, Antineoplastic Agents pharmacology, Antipsychotic Agents pharmacology, Drosophila melanogaster drug effects, Drug Repositioning methods, Enzyme Inhibitors pharmacology, Genomics methods, Prostatic Neoplasms drug therapy, Risperidone pharmacology

Abstract

Drug reprofiling is emerging as an effective paradigm for discovery of cancer treatments. Herein, an antipsychotic drug is immobilised using the Magic Tag ® chemical genomics tool and screened against a T7 bacteriophage displayed library of polypeptides from Drosophila melanogaster, as a whole genome model, to uncover an interaction with a section of 17-β-HSD10, a proposed prostate cancer target. A computational study and enzyme inhibition assay with full length human 17-β-HSD10 identifies risperidone as a drug reprofiling candidate. When formulated with rumenic acid, risperidone slows proliferation of PC3 prostate cancer cells in vitro and retards PC3 prostate cancer tumour growth in vivo in xenografts in mice, presenting an opportunity to reprofile risperidone as a cancer treatment., (Crown Copyright © 2017. Published by Elsevier B.V. All rights reserved.)

Published

2017

48. Development of oral solid self-emulsifying lipid formulations of risperidone with improved in vitro dissolution and digestion.

Author

Kazi M, Al-Qarni H, and Alanazi FK

Subjects

Antipsychotic Agents chemistry, Antipsychotic Agents pharmacokinetics, Delayed-Action Preparations, Drug Compounding, Drug Delivery Systems, Emulsions, Excipients chemistry, Lipids chemistry, Particle Size, Risperidone chemistry, Risperidone pharmacokinetics, Solubility, Antipsychotic Agents administration & dosage, Risperidone administration & dosage

Abstract

Liquid adsorption on solid adsorbent carriers is an emerging technique for oral lipid-based drug delivery systems. The purpose of the current study is to convert liquid into solid self-emulsifying lipid formulations (SELFs) using an inorganic adsorbent Neusilin® grade US2 (NUS2) and investigate in vitro dissolution and digestion performance of the model antipsychotic compound risperidone., Methods: The liquid SELFs were designed using various oils, nonionic surfactants and converted into solid at various SELF: NUS2 (%m/m) mixing ratios. The characterization of solid SELF powder was performed by using SEM, XRD, FT-IR & DSC to investigate the physical nature of the drug. The in vitro dissolution experiments were conducted to compare the representative formulations with marketed product risperdal®. In vitro digestion experiments were performed using a pH-stat at pH 6.8 for 30mins to predict the fate of risperidone in the GI tract after exposure of the solid SELF to pancreatic enzymes and bile., Results: The results from the characterization studies showed that NUS2 with SELF at 1:1 (%m/m) yield superior flowability of the powder. The SEM revealed that pure risperidone was in irregular crystal shape whereas the drug loaded solid SELFs were in smooth regular shape. The XRD and DSC analyses of pure risperidone also confirmed the intense peaks due to the native crystalline form of the drug. However, the absence of sharp peaks in solid SELFs indicated the amorphous form of the drug. From the dissolution studies it was found that solid SELFs provided significant release profiles (>95%) compared to marketed product risperdal®. The digestion experiments suggested that risperidone was in a supersaturated state which could be maintained in the presence of mixed bile salt micelles., Conclusions: Solid SELF of risperidone with improved dissolution and digestion profile was successfully prepared using Neusilin® US2 as an adsorbent carrier., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

49. The use of experimental design in the optimization of risperidone biodegradable nanoparticles: in vitro and in vivo study.

Author

Alzubaidi AF, El-Helw AM, Ahmed TA, and Ahmed OA

Subjects

Animals, Male, Rabbits, Drug Delivery Systems methods, Nanoparticles chemistry, Risperidone chemistry, Risperidone pharmacokinetics, Risperidone pharmacology

Abstract

The aim of this study was optimization of risperidone (model drug) biodegradable nanoparticles utilizing emulsion-solvent evaporation technique. Box-Behnken design was adopted to optimize the preparation process. Optimized nanoparticles were characterized for surface morphology using scanning electron microscope. Pharmacokinetic parameters were compared with the marketed tablets. Results revealed that the optimized formula showed 297.37 nm, 85.12%, and 59.79% for Y1, Y2, and Y3, respectively. Optimized formula showed significant improved bioavailability compared with marketed tablets. Successful achievement of prolonged risperidone release with improved bioavailability is expected to maximize patients' adherence to their antipsychotic drug therapy and to minimize risk of relapse during maintenance therapy.

Published

2017

50. A comparison between conventional liposome and drug-cyclodextrin complex in liposome system.

Author

Wang WX, Feng SS, and Zheng CH

Subjects

Drug Delivery Systems, Drug Liberation, Drug Stability, Microscopy, Electron, Transmission, Particle Size, Cyclodextrins chemistry, Liposomes chemistry, Risperidone chemistry

Abstract

A drug-cyclodextrin complex in liposome system was prepared in order to make a comparison with conventional risperidone-loaded liposome. Thin film hydration, reverse phase evaporation and ethanol injection methods were taken as preparation means to obtain the two types of liposome. Differential thermal analysis (DTA) and transmission electron microscopy (TEM) were used to investigate the thermal characters of inclusion complexes and morphology of liposome, respectively. Particle size, zeta potential and encapsulation efficiency were studied by light scattering analysis and ultrafiltration. In vitro release was carried out in the pH 7.4 phosphate buffer solution and samples were collected at the certain time. As a result, drug-cyclodextrin complex in liposome prepared by various methods displayed lower encapsulation efficiency than conventional liposome. However, size was larger and its stability was better than the latter. The second release phase of novel delivery system was slightly slower after initial burst release at the first phase, while the conventional liposome displayed a more regular trait. Thus, the novel liposome have potential to be developed as co-administration formulation with long-acting injection., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016