Synthesis and characterization of poly(N‐vinyl‐2‐pyrrolidone) grafted sodium alginate hydrogel beads for the controlled release of indomethacin

Graft copolymers of sodium alginate (NaAlg) with N‐vinyl‐2‐pyrrolidone were prepared using azobisisobutyronitrile as initiator. The graft copolymers (NaAlg‐g‐PVP) were characterized with Fourier transform infrared spectroscopy, elemental analysis, and differential scanning calorimetry. Polymeric hydrogel beads of NaAlg and NaAlg‐g‐PVP were prepared by crosslinking method using glutaraldehyde (GA) as a crosslinker in the hydrochloric acid catalyst (HCl) and these beads were used to deliver anti‐inflammatory drug, indomethacin (IM). Chemical stability of the IM after encapsulation into beads was confirmed by FTIR. Preparation conditions of the NaAlg‐g‐PVP beads were optimized by considering the percentage entrapment efficiency, particle size, swelling capacity and their release data. In vitro release studies were performed in simulated gastric fluid (pH 1.2) for the initial 2 h, followed by simulated intestinal fluid (pH 7.4) for 4 h. Effects of GA concentration, exposure time to GA, drug/polymer (d/p) ratio, and concentration of HCl on the release of IM were discussed. It was observed that IM release from the beads decreased with increasing GA concentration and exposure time. IM release also decreases with increasing d/p ratio and HCl concentration. The highest IM release was obtained to be 77% for beads crosslinked with 0.027M GA. Swelling experiments were also performed to compute molecular mass between crosslinks of the beads. © 2008 Wiley Periodicals, Inc. J Appl Polym Sci, 2008     

Synthesis of N‐benzyl‐O‐carboxymethylchitosan and application in the solubilization enhancement of a poorly water‐soluble drug (triamcinolone)

N‐Benzyl‐O‐carboxymethyl chitosan (OCChB) was synthesized through a reaction of O‐carboxymethylchitosan (OCCh) and benzaldehyde by the reductive amination method. The chemical structures and physical properties of the derivatives were confirmed by Fourier transform infrared spectroscopy and ¹H‐NMR. The cytotoxicity of the polymers was tested by MTT (3‐[4,5‐dimethylthiazol‐2‐yl]‐2,5‐diphenyltetrazolium bromide) assay at concentrations ranging from 0.01 to 1000 μg/mL. The substitution degrees of the derivatives, calculated by ¹H‐NMR, were 12 and 53% for OCChB1 and OCChB2, respectively. The results show that the derivatives were not toxic at 1000 μg/mL and could decrease the surface tension by concentration on the system surface compared with OCCh. Because of this property, OCChB was applied as a solubility enhancer for triamcinolone (TC), a poorly water‐soluble drug. The polymer solutions at 1.0 mg/mL increased the TC solubility up to 3.5 times for OCChB1 and 5.0 times for OCChB2 compared with its solubility in water. © 2011 Wiley Periodicals, Inc. J Appl Polym Sci, 2012     

Tailoring of water‐soluble cellulose‐g‐ copolymers in homogeneous medium using single‐electron‐transfer living radical polymerization

Cellulose‐graft‐polyacrylamide and cellulose‐graft‐poly(N,N‐dimethylacrylamide) copolymers were prepared by single‐electron‐transfer living radical polymerization (SET‐LRP) in homogeneous medium. Cellulose macroinitiators for SET‐LRP, with different numbers of initiating sites along the cellulose backbone, were successfully synthesized by direct acylation of cellulose with 2‐bromoisobutyryl bromide in LiCl/dimethylacetamide. Dynamic light scattering revealed that cellulose macroinitiator molecules in dimethylsulfoxide (DMSO) exist primarily as individual chains with a certain amount of intermolecular aggregates. SET‐LRP of acrylamide and N,N‐dimethylacrylamide with the cellulose macroinitiators was carried out in DMSO solution. Formation of cellulose‐graft‐copolymers was confirmed using attenuated total reflectance Fourier transform infrared, ¹H NMR and ¹³C NMR spectroscopy, and the products were water‐soluble. High content of poly(N,N‐dimethylacrylamide) in the copolymers enhanced the thermal stability relative to that of cellulose. Scanning electron microscopy studies of cellulose‐based particles formed from the copolymers using the aerosol flow reactor method revealed spherical nanoscale structures. Copyright © 2011 Society of Chemical Industry     

Synthesis of collagen‐modified polylactide and its application in drug delivery

In this article, collagen modified polylactide (CPLA) was synthesized by means of graft modification, and its structure was confirmed by FTIR and FITC‐labeled fluorescence spectra. Subsequently, the performance of CPLA was characterized with hydrophilicity test and degradability test. After that, the aspirin sustained release microspheres of the synthetic copolymers were prepared via the emulsion‐solvent evaporation technique, followed with its measurements of morphology, size, and encapsulation efficiency. Finally, the controlled release properties of the obtained microspheres were investigated. The results showed that the aspirin sustained release microspheres exhibited well‐defined morphology with smooth spherical surface, with average size of 3.990 μm and encapsulation efficiency of 51.83%. Furthermore, compared with aspirin‐loaded PLA microspheres, at the initial 32 h, the drug release was faster for aspirin‐loaded CPLA microspheres favored by its increased hydrophilicity, and then the drug release was slower than that of PLA microspheres because the ? NH₂ group on the introduced collagen inhibited acidic autocatalytic degradation. The results suggested that CPLA showed a great potential as particles for drug delivery. © 2013 Wiley Periodicals, Inc. J. Appl. Polym. Sci., 2013     

Preparation and drug release behaviors of 5‐fluorouracil loaded poly(glycolide‐co‐lactide‐co‐caprolactone) nanoparticles

5‐Fluorouracil (5‐Fu) loaded poly(glycolide‐co‐lactide‐co‐caprolactone) (PGLC) nanoparticles were prepared by modified spontaneous emulsification solvent diffusion method (modified‐SESD method) and characterized by dynamic light scattering, scanning electron microscopy and ¹H NMR determination. It was found that the obtained nanoparticles showed near spherical shape and was controllable with the radius range of 30–100 nm. Compared with the nanoparticles prepared by polylactide and poly (lactide‐co‐glycolide) (PLGA) under the similar preparation condition, yield of PGLC nanoparticles was the highest, which reached to about 100%. On the other hand, drug entrapment efficiency of PGLC nanoparticles was also higher than that of PLGA and PLLA nanoparticles. 5‐Fu release behavior of PGLC nanoparticles in vitro showed that 5‐Fu release of PGLC nanoparticles showed a near zero‐order release profile, and 5‐Fu release rate of PGLC nanoparticles was faster than that of PLLA and PLGA nanoparticles. According to degradation behavior of PGLC nanoparticles, it could be proposed that the kinetic of degradation controlled release played an important role in the release process of PGLC nanoparticles. It revealed that the PGLC nanoparticles could be a promising drug carrier. © 2007 Wiley Periodicals, Inc. J Appl Polym Sci, 2007     

Synthesis and characterization of electrically responsive poly(acrylamide)-grafted-chondroitin sulfate hydrogel for transdermal drug delivery application

Abstract

Electrically-responsive transdermal delivery systems (ETDS) were developed utilizing poly(acrylamide)-grafted-chondroitin sulfate (PAAm-g-CS) copolymer. A nitrogen environment based free radical polymerization was used to synthesize electrically responsive PAAm-g-CS copolymer. This PAAm-g-CS hydrogel was used as drug reservoir and cross-linked blend films of CS and poly(vinyl alcohol) as rate controlling membranes (RCM). The drug permeation decreased with increase in the concentration of glutaraldehyde and RCM thickness; while drug permeation was increased with increasing electric stimulus from 2 to 8?mA. Nearly, three-fold increase in flux was observed with the application of electric stimulus. The permeation study under “on–off” electric stimulus suggested that the higher drug permeation was observed under “on” condition of electric stimulus and permeation was decreased when electric stimulus was “off”. The histopathology evaluation confirmed the changes in skin structure when electrical stimulus was applied. Hence, the PAAm-g-CS hydrogel could be a resourceful material for on-demand discharge of medication.     

Starch–acrylics graft copolymers and blends: Synthesis,characterization, and applications as matrix for drug delivery

A series of acrylic monomers–starch graft copolymers were prepared by ceric ion initiation method by varying the amount of monomers. These graft copolymers were characterized by IR and ¹³C‐NMR spectroscopy. It was seen that as the concentration of monomer [acrylic acid (AA), methacrylic acid (MA), and methyl methacrylate (MMA)] increased the percent add‐on increased in all the graft copolymers, whereas grafting efficiency increased initially but showed a slight decrease with further increase in the monomer concentration (except for MMA). The release rate of paracetamol as a model drug from graft copolymers as well as their blends was studied at two different pH, 1.2 and 7.4, spectrophotometrically. The release of paracetamol in phosphate buffer solution at pH 1.2 was insignificant in the first 3 h for St‐g‐PAA‐ and St‐g‐PMA‐graft copolymers, which was attributed to the matrix compaction and stabilization through hydrogen bonding at lower pH. At pH 7.4, the release rate was seen to decrease with increase in add‐on. The tablet containing poly(methyl methacrylate) (PMMA) did not disintegrate at the end of 30–32 h, which may be attributed to the hydrophobic nature of PMMA. These results indicate that the graft copolymers may be useful to overcome the harsh environment of the stomach and can be used as excipients in colon‐targeting matrices. © 2009 Wiley Periodicals, Inc. J Appl Polym Sci, 2009     

Thermoresponsive/low‐fouling Zwitterionic hydrogel for controlled drug release

A controlled/ living free‐radical polymerization technique was introduced to prepared a homogeneous poly(N‐isopropylacrylamide)‐g‐poly(sulfobetaine methacrylate) hydrogel (RG) possessing a highly porous architecture via two steps. Compared to a poly(N‐isopropylacrylamide)‐co‐poly(sulfobetaine methacrylate) hydrogel (CG) prepared by conventional radical polymerization, RG exhibited a much faster shrinking rate (it lost over 72% of the water in 15 min) in response to the temperature changes. The release behaviors of tetracycline hydrochloride (TCHC) of the hydrogels indicated the TCHC release from the RG could be prolonged to 48 h at 37°C; this was much longer than that for CG (5 h at 37°C). Bovine serum albumin (BSA) was chosen as the model protein to examine the low‐fouling properties of the RG. The BSA adsorption data showed that improved antifouling properties could be achieved by the RG at both 25 and 37°C. © 2013 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2014 , 131, 39816.     

Synthesis and characterization of the environmental‐sensitive hyperbranched polymers as novel carriers for controlled drug release

Novel hyperbranched polymers, which contain a hydrophobic branched poly(p‐(chloromethy)styrene) (PCMS) core and poly(N,N‐dimethylaminoethyl methacrylate) (PDMA) shell that exhibited environmental sensitivity, have been synthesized by atom transfer radical polymerization (ATRP). At first, a hyperbranched polymer (PCMS) core is obtained via ATRP of p‐(chloromethy)styrene (CMS), which may act as an “inimer”‐monomer and initiator. Then the modified hyperbranched polymers having different average arm length consisting of PCMS and PDMA are synthesized by ATRP using anterior PCMS as macroinitiators. Their macromolecular structures are characterized by FTIR and ¹H NMR. Using chlorambucil as a model drug, the behaviors of the controlled drug release from the environmental‐sensitive hyperbranched polymers with different average chain length of PDMA and degree of branching are studied. The data demonstrate that the rate of the drug release can be effectively controlled by pH value, and these environmental‐sensitive hyperbranched polymers have the potential to be used as novel carriers in some controlled drug release systems in the future. © 2006 Wiley Periodicals, Inc. J Appl Polym Sci 101: 311–316, 2006     

Synthesis of chitosan‐graft‐β‐cyclodextrin for improving the loading and release of doxorubicin in the nanopaticles

Chitosan‐graft‐β‐cyclodextrin (CS‐g‐β‐CD) copolymer was synthesized by conjugating β‐cyclodextrins to chitosan molecules through click chemistry. The copolymer structure was characterized by Fourier transform infrared spectroscopy (FTIR) and nuclear magnetic resonance (NMR). CS‐g‐β‐CD/CMC nanoparticles were prepared by a polyelectrolyte complexation process in aqueous solution between CS‐g‐β‐CD copolymer and carboxymethyl chitosan (CMC), which was used to load anticancer drug (Doxorubicin hydrochloride, DOX·HCl) with hydrophobic group. The particle size, surface charge, zeta potential, and morphology of the nanoparticles were characterized with dynamic light scattering. The drug loading efficiency and in vitro release of DOX·HCl of the nanoparticles were measured by ultraviolet spectrophotometer. The results demonstrated that the size, surface charge and drug loading efficiency of the nanoparticles could be modulated by the fabrication conditions. The drug loading efficiency of CS‐g‐β‐CD/CMC nanoparticles was improved from 52.7% to 88.1% because of the presence of β‐CD moieties with hydrophobic cavities, which can form inclusion complexes with the drug molecules. The in vitro release results showed that the CS‐g‐β‐CD/CMC nanoparticles released DOX·HCl in a controlled manner, importantly overcoming the initial burst effect. These nanoparticles possess much potential to be developed as anticancer drug delivery systems, especially those drugs with hydrophobic group. © 2014 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2014 , 131, 41034.     

Non‐catalyst synthesis and in vitro drug release property of poly(5,5‐dimethyl‐1,3‐dioxan‐2‐one)‐block‐methoxy poly(ethylene glycol) copolymers

A series of poly(5,5‐dimethyl‐1,3‐dioxan‐2‐one)‐block‐methoxy poly(ethylene glycol) (PDTC‐b‐mPEG) copolymers were synthesized by the ring‐opening polymerization of 5,5‐dimethyl‐1,3‐dioxan‐2‐one (DTC) in bulk, using methoxy poly(ethylene glycol) (mPEG) as initiator without adding any catalysts. The resulting copolymers were characterized by Fourier transform infrared spectra, ¹H NMR and gel permeation chromatography. The influences of some factors such as the DTC/mPEG molar feed ratio, reaction time and reaction temperature on the copolymerization were investigated. The experimental results showed that mPEG could effectively initiate the ring‐opening polymerization of DTC in the absence of catalyst, and that the copolymerization conditions had a significant effect on the molecular weight of PDTC‐b‐mPEG copolymer. In vitro drug release study demonstrated that the amount of indomethacin released from PDTC‐b‐mPEG copolymer decreased with increase in the DTC content in the copolymer. © 2013 Society of Chemical Industry     

Controlled drug release of silicone‐based adhesive‐containing cross‐linked siloxane powders as a reservoir

We prepared pressure‐sensitive adhesive (PSA)‐containing cross‐linked siloxane powders (CS) as a reservoir for a transdermal drug delivery system (TDDS) and evaluated their sustained drug‐release properties. PSA, as a patch‐type adhesive, was synthesized by a hydrosilylation reaction of vinyl‐terminated polysiloxanes with hydrogen‐terminated polydimethylsiloxanes. CS was also prepared via a hydrosilylation process with vinyl‐terminated polydimethylsiloxane, 1,3,5,7‐tetramethyl‐1,3,5,7‐tetravinyltetracyclosiloxane ( ), hydrogen‐terminated polydimethylsiloxane, and dimethylhydrogenmethyl oligomeric siloxane copolymer. The results of release performances using ascorbic acid as a model drug showed a cumulative linear slope over a week, indicating a constant release performance. Our data suggest that this siloxane TDDS could be useful for constant drug release over a long period. © 2015 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2015 , 132, 42154.     

A convenient scheme for synthesizing reduction‐sensitive chitosan‐based amphiphilic copolymers for drug delivery

A novel type of reduction‐sensitive graft copolymers, chitosan‐S‐S‐poly(ε‐caprolactone) (CS‐S‐S‐PCL, here ‐S‐S‐ means PCL was conjugated onto chitosan backbone through disulfide linkage), was synthesized through a convenient route using dithiodipropionic anhydride (DTDPA) as a disulfide donor. Reaction of hydroxy‐terminated poly(ε‐caprolactone) (PCL) with DTDPA quantitatively yielded DTDPA functionalized PCL (PCL‐S‐S‐COOH). The disulfide‐containing polyester was regioselectively conjugated onto the hydroxy groups of chitosan under mild and homogeneous conditions, utilizing dodecyl sulfate‐chitosan complexes (SCC) as an intermediate. The self‐assembly and Doxorubicin (Dox) release behavior of the copolymers were investigated. Spherical micelles could be formed through self‐assembly of CS‐S‐S‐PCL in aqueous media. The reduction‐sensitive behavior of CS‐S‐S‐PCL micelles was investigated by using Dithiothreitol (DTT) as a reductive reagent. In the presence of 10 mM DTT, the micelles gradually lost their aggregation stability and were precipitated out after four days. In addition, the Dox release was accelerated when the micelles were treated with DTT. © 2011 Wiley Periodicals, Inc. J Appl Polym Sci, 2012     

The polymer free volume as a controlling factor for drug release from poly(lactide‐co‐glycolide) microspheres

Drug release from poly(lactide‐co‐glycolide) (PLGA) microspheres is strongly determined by the pore structure of the particles. This study examines how swelling‐induced pore constriction delays the drug release and by which factors this process is controlled. Combination of different porosimetric and pycnometric methods enabled insight into the submicroscopic range of the pore structure and revealed that remarkably the polymer free volume plays a crucial role in drug release from PLGA microspheres. Surprisingly, the latter was shown to be inversely correlated to the degree of diffusional drug release. This can be explained by a swelling‐induced constriction of the macroporous channel system in the microspheres which is related to the availability of free volume. The hole free volume was shown to be well controllable by the manufacturing conditions. Thus, the study deepens comprehension of the mechanism of drug release from biodegradable microparticles and offers an effective approach for controlling the release behavior. © 2013 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2014 , 131, 39740.     

Synthesis,characterization, and in vitro drug release study of 3‐arm poly‐β‐alanine

Synthesis of three arms star‐shaped poly‐β‐alanine (3‐b‐ala) based on tri(prop‐2‐yn‐1‐yl) benzene‐1,3,5‐tricarboxylate (TBT) and azido terminated poly‐β‐alanine (N₃‐P‐ala) was performed using click reaction. TBT was synthesized by nucleophilic substitution reaction between propargyl alcohol and 1,3,5‐benzenetricarbonyltrichloride. For the first time, N₃‐P‐ala was synthesized through anionic polymerization of acrylamide using sodium azide as an initiator. TBT was characterized by FT‐IR and ¹HNMR. N₃‐p‐ala was characterized by FT‐IR, GPC, and ¹HNMR and 3‐b‐ala was characterized by FT‐IR, GPC, ¹HNMR, TGA, and XRD. The synthesized 3‐b‐ala was used for drug loading and releasing studies. Polymer loaded drug (3‐b‐ala‐D) hybrid was used in in vitro studies of drug (Diclofenac sodium) release in phosphate buffer solution (PBS) at 37 ± 0.5°C and pH 7.4. The drug loading and releasing studies were analyzed by UV‐visible spectrophotometer. 3‐b‐ala‐D was examined by AFM to analyze the surface morphology and roughness. © 2015 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2015 , 132, 42124.     

Preparation and characteristic of lactose‐oleoylchitosan and the application of its self‐aggregates as drug delivery system

Amphiphilic polymers lactose‐oleoylchitosan (Lac‐OCH) with different degree of substitution (DS) of lactose were prepared. The chemical structure of the new chitosan derivative was tested and verified. The rheological features including solubility and viscosity of Lac‐OCH were investigated. The introduction of hydrophilic group lactose could improve the solubility of the polymer and Lac‐OCH was soluble in acetic acid solution under pH 7.0. The viscosity of Lac‐OCH decreased a little along with the increasing of DS of lactose. Lac‐OCH with high DS, middle DS, and low DS of lactose possessed small critical aggregation concentration value, and the critical aggregation concentration value rised along with the increasing of DS of lactose. However, the affect was not obvious. In brief, the CAC values were 0.0325, 0.0340, and 0.0344 mg/mL corresponding to the samples of low DS, middle DS, and high DS. Lac‐OCH, obtained by hydrophilic modified using lactose, could also form self‐assembled nanoparticles by oil/water (O/W) emulsification method comparing with OCH. The Lac‐OCH nanoparticles showed dense, axiolitic texture, and the average diameter was approximate 200 nm. The sustained‐release characteristics of Lac‐OCH nanoparticles were studied using Doxorubicin as model drug. The results revealed the promising potential of amphiphilic Lac‐OCH as drug carrier. © 2011 Wiley Periodicals, Inc. J Appl Polym Sci, 2011     

Synthesis and characterization of star‐shaped PLLA with sorbitol as core and its microspheres application in controlled drug release

The purpose of this study was to investigate the suitability of a six‐arm star‐shaped poly(l ‐lactide)s (s‐PLLA) as controlled drug carriers for hydrophobic drug molecules. First, s‐PLLA was synthesized by ring‐opening polymerization of l ‐lactide using sorbitol as initiator and stannous octoate as catalyst. The structure and molecular weight (M_w) of s‐PLLA was characterized with ¹H NMR, ¹³C NMR, and GPC. Second, rifampicin (RIF) used as a model drug was encapsulated within the microspheres of s‐PLLA via oil‐in‐water emulsion/solvent evaporation technique. The morphology, drug encapsulation efficiency (EE), and in vitro release behavior of the prepared microspheres were studied in details. Results indicated that the average diameters of s‐PLLA microspheres can be controlled between 8 and 20 µm by varying the copolymer's concentration or M_w . The EE of RIF was mainly determined by the concentration of s‐PLLA. The in vitro study showed that the burst release behavior can be depressed by increasing the M_w of the s‐PLLA. Present work suggests that the synthesized s‐PLLA could be used as a new material for drug delivery. © 2015 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2015 , 132, 42213.     

Synthesis and characterization of methoxypolyethyleneglycol and lauric acid grafted novel polyurethanes for controlled release of nifedipine

Novel polyurethanes (PUs) grafted with methoxypolyethyleneglycol (mPEG) and lauric acid (LA) were synthesized by solution polymerization using dibutyl tin dilaurate as a catalyst, taking different molar ratios of LA‐trimethylol propane (LA‐TMP) with respect to mPEG‐trimethylol propane (mPEG‐TMP). The polymers obtained were characterized by Fourier transform infrared spectroscopy and gel permeation chromatography to confirm, respectively, the PU formation and molecular weight. Moderate molecular‐weight PUs were obtained, and nifedipine (NFD)‐loaded microspheres were prepared by solvent evaporation method. The size of the microspheres as measured by laser light scattering technique ranged between 10 and 50 μm. An increase in the size of particles was observed with an increasing molar ratio of mPEG‐TMP with respect to LA‐TMP. The % encapsulation efficiency was found to vary between 65 and 92. The surface morphology of microspheres as studied by scanning electron microscopy revealed the spherical nature of the particles with wrinkles on their surfaces. Crystalline nature of the drug in the microspheres after loading was studied by X‐ray diffraction technique. The release of NFD through the matrix microspheres was investigated in pH‐7.4 phosphate buffer. An increase in release rate was observed with increasing molar ratio of mPEG‐TMP with respect to LA‐TMP. © 2007 Wiley Periodicals, Inc. J Appl Polym Sci 2007     

Synthesis and drug‐release studies of low‐fouling zwitterionic hydrogels with enhanced mechanical strength

Reversible addition–fragmentation chain‐transfer polymerization was introduced to prepare a series of zwitterionic poly(hydroxyethyl methacrylate)‐g‐poly(sulfobetaine methacrylate) (PSBMA) hydrogels (HSGs) with different monomer feed ratios. Compared with PSBMA hydrogels, these hydrogels exhibited enhanced mechanical strengths. Then, the HSGs were characterized by Fourier transform infrared spectroscopy, scanning electron microscopy, and swelling measurements. We found that the equilibrium swelling ratios, mechanical strengths, and drug‐release behaviors were significantly affected by the feed ratios of the gels. The hydrophilic tetracycline hydrochloride release results suggest that the hydrophilic drug release from the HSGs could be prolonged by the variation of the hydroxyethyl methacrylate amount in the gel networks. The bovine serum albumin adsorption data showed that the zwitterionic HSG with 18.2 wt % sulfobetaine methacrylate exhibited good protein‐resistance properties. © 2014 Wiley Periodicals, Inc. J. Appl. Polym. Sci. 2014 , 131, 41041.