Your search keyword '"Mortazavian E"' showing total 8 results

1. Preparation, Design for Optimization and in Vitro Evaluation of Insulin Nanoparticles Integrating Thiolated Chitosan Derivatives

Author

Mortazavian, E., Amini, M., Dorkoosh, F.A., Amini, H., Khoshayand, M.R., Amini, T., and Rafiee-Tehrani, M.

Published

2014

2. Effect of oral administration of GnRHa+nanoparticles of chitosan in oogenesis acceleration of goldfish Carassius auratus.

Author

Kookaram K, Mojazi Amiri B, Dorkoosh FA, Nematollahi MA, Mortazavian E, and Abed Elmdoust A

Subjects

Administration, Oral, Animals, Female, Gonadotropin-Releasing Hormone administration & dosage, Gonadotropin-Releasing Hormone chemistry, Oocytes drug effects, Oocytes growth & development, Chitosan chemistry, Goldfish, Gonadotropin-Releasing Hormone pharmacology, Nanoparticles chemistry, Oogenesis drug effects

Abstract

Several methods have been used to accelerate previtellogenesis and vitellogenesis stages in fish, including hormonal induction, sustained-release delivery systems, and oral delivery of gonadotropin-releasing hormone (GnRH). In this study, we proposed the oral administration of GnRH analog + nanoparticles of chitosan to accelerate oogenesis in goldfish as a model fish in reproductive biology and aquaculture. In this regard, adult female goldfish were fed with six experimental groups: chitosan, 50 μg GnRHa/kg b.w., 100 μg GnRHa/kg b.w., chitosan + 50 μg GnRHa/kg b.w., and chitosan + 100 μg GnRHa/kg b.w., and diet without any additive as the control for 40 days in triplicate. Every 10 days, ovarian samples were collected, and gonadosomatic index (GSI), oocyte diameter (OD), zona radiata thickness (Zr), and diameter of the follicular layer (Fl) were measured to assess ovarian developmental stage for each treatment. Additionally, blood sampling was done to measure serum 17β-estradiol concentration at the end of the experiment. All parameters remained unchanged during the experiment in the chitosan-fed group. In the group fed with 100 μg GnRH or chitosan nanoparticle + 100 μg GnRHa, these parameters in general were increased. However, the effects in 50 μg GnRHa or chitosan nanoparticle + 50 μg GnRHa treatments were uncertain; they affected serum E2 levels as a trend toward a significant increase was observed in goldfish treated with chitosan nanoparticle + 100 μg GnRHa. Finally, the results indicated the oral administration of chitosan + 100 μg GnRHa/kg b.w. significantly accelerated the oocyte development and growth of ovary.

Published

2021

3. Novel chitosan based nanoparticles as gene delivery systems to cancerous and noncancerous cells.

Author

Rahmani S, Hakimi S, Esmaeily A, Samadi FY, Mortazavian E, Nazari M, Mohammadi Z, Tehrani NR, and Tehrani MR

Subjects

Cell Line, Tumor, HEK293 Cells, Humans, MCF-7 Cells, Neoplasms therapy, Particle Size, Plasmids administration & dosage, Polymers chemistry, Transfection, Chitosan chemistry, DNA administration & dosage, Gene Transfer Techniques, Nanoparticles

Abstract

The present study aimed to investigate in vitro DNA transfection efficiency of three novel chitosan derivatives: thiolated trimethyl chitosan (TMC-Cys), methylated 4-N,N dimethyl aminobenzyl N,O carboxymethyl chitosan(MABCC) and thiolated trimethyl aminobenzyl chitosan(MABC-Cys). After polymer synthesis and characterization, nanoparticles were prepared using these polymers and their size, zeta potential and DNA condensing ability were measured. After that, cytotoxicity and transfection efficiency of nanocomplexes were carried out in three different cells. The results showed that all polymers could condense DNA plasmid strongly from N/P 2 and nanocomplexes had eligible sizes and zeta potentials. Moreover, the nanocomplexes had negligible cytotoxicity and MABC-Cys was the most effective vehicle for gene delivery in HEK-293T cells. In the two other cell lines, SKOV-3 and MCF-7, TMC-Cys exhibited the highest transfection efficiency. This study indicated that chemical structure of these novel chitosan derivatives in the interaction with the cell type can lead to successful gene delivery., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

4. Determination of diffusion coefficient for released nanoparticles from developed gelatin/chitosan bilayered buccal films.

Author

Mahdizadeh Barzoki Z, Emam-Djomeh Z, Mortazavian E, Rafiee-Tehrani N, Behmadi H, Rafiee-Tehrani M, and Moosavi-Movahedi AA

Subjects

Analysis of Variance, Cell Death, Cell Survival, Diffusion, Drug Liberation, HEK293 Cells, Humans, Insulin administration & dosage, Insulin pharmacology, Particle Size, Reproducibility of Results, Spectroscopy, Fourier Transform Infrared, Static Electricity, Chitosan chemistry, Gelatin chemistry, Mouth Mucosa metabolism, Nanoparticles chemistry

Abstract

This study aims at the mathematical optimization by Box-Behnken statistical design, fabrication by ionic gelation technique and in vitro characterization of insulin nanoparticles containing thiolated N- dimethyl ethyl chitosan (DMEC-Cys) conjugate. Then Optimized insulin nanoparticles were loaded into the buccal film, and in-vitro drug release from films was investigated, and diffusion coefficient was predicted. The optimized nanoparticles were shown to have mean particle size diameter of 148nm, zeta potential of 15.5mV, PdI of 0.26 and AE of 97.56%. Cell viability after incubation with optimized nanoparticles and films were assessed using an MTT biochemical assay. In vitro release study, FTIR and cytotoxicity also indicated that nanoparticles made of this thiolated polymer are suitable candidates for oral insulin delivery., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

5. New comprehensive mathematical model for HPMC-MCC based matrices to design oral controlled release systems.

Author

Saeidipour F, Mansourpour Z, Mortazavian E, Rafiee-Tehrani N, and Rafiee-Tehrani M

Subjects

Chemistry, Pharmaceutical methods, Diffusion, Drug Liberation drug effects, Excipients chemistry, Lactose chemistry, Methylcellulose chemistry, Models, Theoretical, Polymers chemistry, Tablets chemistry, Chitosan chemistry, Delayed-Action Preparations chemistry, Lactose analogs & derivatives, Methylcellulose analogs & derivatives

Abstract

A comprehensive model with all effective phenomena in drug release such as diffusion, swelling and erosion was considered. In this work, a mathematical model was developed to describe drug release from controlled release HPMC matrices as a favorable system in pharmaceutical industries. As a novel study, the impact of the MCC presence as a filler in tablet preparation process was considered in the mathematical model. In addition, we found that the volume expansion of these polymeric matrices did not follow the ideal mixing rule and we derived an equation for estimating the volume of hydrated matrix. Furthermore, some equations were derived to estimate the parameters of model (K erosion , D eq ) as well as the change in matrix volume based on the amount of polymer and filler in formulation. This investigation gave deeper insight into underlying drug release mechanisms. According to the results, K erosion increases linearly and D eq increases exponentially with the increase in the amount of MCC in formulation. Application of this comprehensive mathematical model enables us to predict the behavior of HPMC-MCC based matrices. Furthermore, this model is able to represent the formulation for the desired drug release profile which is useful to design new controlled release matrix as well as improving the system geometry and dimensions of tablets. The presented model was validated by two independent tests: (a) predicting the behavior of matrix with certain MCC/HPMC ratio upon exposure to the release medium; (b) designing formulation of Bupropion hydrochloride extended release tablet., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

6. Thiolated methylated dimethylaminobenzyl chitosan: A novel chitosan derivative as a potential delivery vehicle.

Author

Hakimi S, Mortazavian E, Mohammadi Z, Samadi FY, Samadikhah H, Taheritarigh S, Tehrani NR, and Rafiee-Tehrani M

Subjects

Cell Survival drug effects, Chitosan toxicity, Drug Carriers toxicity, HEK293 Cells, Humans, Solubility, Sulfhydryl Compounds toxicity, Chitosan analogs & derivatives, Chitosan chemistry, Drug Carriers chemistry, Sulfhydryl Compounds chemistry

Abstract

Chitosan is a natural mucoadhesive, biodegradable, biocompatible and nontoxic polymer which has been used in pharmaceutical industry for a lot of purposes such as dissolution enhancing, absorption enhancing, sustained releasing and protein, gene or drug delivery. Two major disadvantages of chitosan are poor solubility in physiological pH and low efficiency for protein and gene delivery. In this study thiolated methylated N-(4-N,N-dimethylaminobenzyl) chitosan was prepared for the first time in order to improve the solubility and delivery properties of chitosan. This novel chitosan derivative was characterized using 1 H NMR, Ellman test, TGA and Zetasizer. Cell toxicity studies were performed on Human Embryonic Kidney 293 (Hek293) cell line using XTT method, to investigate the potential effect of this new derivative on cell viability. 1 H NMR results showed that all substitution reactions were successfully carried out. Zeta potential of new derivative at acidic and physiological pHs was greater than chitosan and it revealed an increase in solubility of the derivative. Furthermore, it had no significant cytotoxicity against Hek293 cell line in comparison to chitosan. These findings confirm that this new derivative can be introduced as a suitable compound for biomedical purposes., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2017

7. Formulation, in vitro evaluation and kinetic analysis of chitosan-gelatin bilayer muco-adhesive buccal patches of insulin nanoparticles.

Author

Mahdizadeh Barzoki Z, Emam-Djomeh Z, Mortazavian E, Akbar Moosavi-Movahedi A, and Rafiee Tehrani M

Subjects

Administration, Buccal, Humans, Chitosan chemistry, Chitosan pharmacokinetics, Gelatin chemistry, Gelatin pharmacokinetics, Insulin chemistry, Insulin pharmacokinetics, Nanoparticles chemistry

Abstract

The present study was performed to optimise the formulation of a muco-adhesive buccal patch for insulin nanoparticles (NPs) delivery. Insulin NPs were synthesised by an ionic gelation technique using N-di methyl ethyl chitosan cysteine (DMEC-Cys) as permeation enhancer biopolymer, tripolyphosphate (TPP) and insulin. Buccal patches were developed by solvent-casting technique using chitosan and gelatine as muco-adhesive polymers. Optimised patches were embedded with 3 mg of insulin-loaded NPs with a homogeneous distribution of NPs in the muco-adhesive matrix, which displayed adequate physico-mechanical properties. The drug release characteristics, release mechanism and kinetics were investigated. Data fitting to Peppas equation with a correlation coefficient indicated that the mechanism of drug release followed an anomalous transport that means drug release was afforded through drug diffusion along with polymer erosion. In vitro drug release, release kinetics, physical and mechanical studies for all patch formulations reflected the ideal characteristics of this buccal patch for the delivery of insulin NPs.

Published

2016

8. Design, characterization and ex vivo evaluation of chitosan film integrating of insulin nanoparticles composed of thiolated chitosan derivative for buccal delivery of insulin.

Author

Mortazavian E, Dorkoosh FA, and Rafiee-Tehrani M

Subjects

Adhesiveness, Administration, Buccal, Animals, Chemistry, Pharmaceutical, Chitosan administration & dosage, Chitosan chemistry, Drug Delivery Systems, Hydrogen-Ion Concentration, Insulin pharmacokinetics, Mouth Mucosa metabolism, Nanoparticles chemistry, Oral Mucosal Absorption, Rabbits, Surface Properties, Tensile Strength, Chitosan analogs & derivatives, Insulin administration & dosage, Nanoparticles administration & dosage

Abstract

The purpose of this study is to optimize and characterize of chitosan buccal film for delivery of insulin nanoparticles that were prepared from thiolated dimethyl ethyl chitosan (DMEC-Cys). Insulin nanoparticles composed of chitosan and dimethyl ethyl chitosan (DMEC) were also prepared as control groups. The release of insulin from nanoparticles was studied in vitro in phosphate buffer solution (PBS) pH 7.4. Optimization of chitosan buccal films has been carried out by central composite design (CCD) response surface methodology. Independent variables were different amounts of chitosan and glycerol as mucoadhesive polymer and plasticizer, respectively. Tensile strength and bioadhesion force were considered as dependent variables. Ex vivo study was performed on excised rabbit buccal mucosa. Optimized insulin nanoparticles were obtained with acceptable physicochemical properties. In vitro release profile of insulin nanoparticles revealed that the highest solubility of nanoparticles in aqueous media is related to DMEC-Cys nanoparticles. CCD showed that optimized buccal film containing 4% chitosan and 10% glycerol has 5.81 kg/mm(2) tensile strength and 2.47 N bioadhesion forces. Results of ex vivo study demonstrated that permeation of insulin nanoparticles through rabbit buccal mucosa is 17.1, 67.89 and 97.18% for chitosan, DMEC and DMEC-Cys nanoparticles, respectively. Thus, this study suggests that DMEC-Cys can act as a potential enhancer for buccal delivery of insulin.

Published

2014