Relationship between the volume phase transition and the surface area of poly (N-isopropylacrylamide) and poly (N-isopropylacrylamide-co-sodium methacrylate) hydrogels

The volume phase transition of poly(N-isopropylacrylamide) (PNIPAAm) and poly(N-isopropylacrylamide-co-sodium methacrylate) (P(NIPAAm-co-SMA)) hydrogels was investigated with consideration of the pore characteristics. The volume phase transition temperature of the hydrogel increased by incorporating sodium methacrylate (SMA). Based on the BET equation, the surface area was evaluated by a gas adsorption method. The surface area of PNIPAAm and P(NIPAAm-co-SMA) hydrogels decreased with increasing temperature, resulting from the fact that the depth and the size of pores decreased significantly in the course of the volume phase transition. Hence, it is suggested that the change of surface area has a close relationship with the volume phase transition of PNIPAAm and P(NIPAAm-co-SMA) hydrogels.     

Design of polyvinyl alcohol hydrogel as a controlled-release vehicle for rectal administration of dl-propranolol-HCl and atenolol

Preparations of beta-blockers, propranolol-HCl and atenolol, in poly(vinyl alcohol) (PVA) hydrogel were designed for the therapeutic treatment of hypertension by transrectal delivery. In vitro release characteristics and plasma drug concentration profiles after rectal administration in rats and dogs were examined. The PVA hydrogels containing beta-blockers were prepared by a low-temperature crystallization method. The release of beta-blockers from hydrogel preparations was consistent with Fickian diffusion (Higuchi model); the drug release versus the square root of release time profile gave a straight line over 60% of the total release process. The release of beta-blockers from hydrogel preparations increased at higher concentrations of PVA in the hydrogel preparations and was not affected by the pH of hydrogel preparations. Plasma concentrations of beta-blockers after rectal administration of hydrogels were higher than those after administration of suppositories (Witepsol H-15) in rats and dogs. The drug plasma concentrations increased at higher concentrations of PVA in hydrogel preparations. In the case of propranolol, which is a hepatic high-clearance drug, area under the blood concentration curve, 0-8 h after rectal administration of a hydrogel preparation (20% w/w PVA, pH 7.0) was 2.16 times and 5.26 times higher than those obtained with Witepsol H-15 suppository and oral administration, respectively. Rectal administration with PVA hydrogels is a favorable route for a hepatic high-clearance drug such as propranolol.     

Radiation preparation of PVA-g-NIPAAm in a homogeneous system and its application in controlled release

Thermosensitive PVA-g-NIPAAm copolymers were prepared by graft copolymerization of N-isopropylacrylamide (NIPAAm) onto poly (vinyl alcohol) (PVA) in homogeneous system of dimethyl sulfoxide (DMSO) by ⁶⁰Co-γ irradiation at room temperature. The factors of affecting the grafting yield, such as radiation dose, dose rate, acid concentration, were investigated. It was found that the grafting yield was increased with dose up to 30 kGy, but decreased slightly with dose rate from 61.2 to 50.1 Gy/min. The acid concentration also had influence on the grafting yield. Then the hydrogel of PVA-g-NIPAAm copolymer was made through a freezing–thawing process. The PVA-g-NIPAAm hydrogel exhibited obvious thermal sensitivity, which was observed from the differences of swelling behavior in water at different temperatures (below or above LCST). In addition, the release of Methylene Blue (MB) from this kind of hydrogel was studied. The release rate of MB from PVA-g-NIPAAm copolymer hydrogel at 48°C was faster than that at 15°C due to the shrinkage of the hydrogel at 48°C.     

A bioinspired 4D printed hydrogel capsule for smart controlled drug release

With the ever-increasing demands for personalized drugs, disease-specific and condition-dependent drug delivery systems, four-dimensional (4D) printing can be used as a new approach to develop drug capsules that display unique advantages of self-changing drug release behavior according to the actual physiological circumstances. Herein, a plant stomata-inspired smart hydrogel capsule was developed using an extrusion-based 4D printing method, which featured with UV cross-linked poly(N-isopropylacrylamide) (PNIPAM) hydrogel as the capsule shell. The lower critical solution temperature (LCST) of the PNIPAM hydrogels was approximately 34.9 °C and macroporous PNIPAM hydrogels were prepared with higher molecular weight polyethylene glycols (PEGs) as the pore-forming agents. Owing to the LCST-induced shrinking/swelling properties, the prepared PNIPAM hydrogel capsules exhibited temperature-responsive drug release along with the microstructure changes in the PNIPAM hydrogels. The in vitro drug release test confirmed that the PNIPAM hydrogel capsules can autonomously control their drug release behaviors on the basis of ambient temperature changes. Moreover, the increased PEG molecular weights in the macroporous PNIPAM hydrogel capsules caused an obvious improvement of drug release rate, distinctly indicating that the drug release profiles can be well programmed by adjusting the internal pore size of the hydrogel capsules. In vitro biocompatibility studies confirmed that the PNIPAM hydrogel capsules have great potential for biomedical applications. The bioinspired 4D printed hydrogel capsules pioneer the paradigm of smart controlled drug release.     

Synthesis of gold nanoparticles stabilized with poly(N-isopropylacrylamide)-co-poly(4-vinyl pyridine) colloid and their application in responsive catalysis

The copolymer of poly(N-isopropylacrylamide)-co-poly(4-vinylpyridine) was synthesized by free radical copolymerization of 4-vinylpyridine and N-isopropylacrylamide. The copolymer synthesized with the feed monomer ratio of 4-vinylpyridine/N-isopropylacrylamide equal to 1/3 was associated to form thermoresponsive colloid in neutral water at room temperature, the average size and the cloud-point temperature of which were 40 nm and 32 °C, respectively. The thermoresponsive colloid was used as scaffold to load 2-nm Au nanoparticles to form the responsive catalyst of colloid-stabilizing gold nanoparticles. The catalysis in the model reduction of 4-nitrophenol with NaBH₄ suggested that the catalytic reduction could be modulated due to the thermoresponsive phase-transition of the colloid-stabilizing gold nanoparticles. That was, the catalytic reduction firstly accelerated with the increase in temperature below the cloud-point temperature and then decelerated with the increase in temperature above the cloud-point temperature of the thermoresponsive colloid-stabilizing Au nanoparticles.     

Fabrication of ultrathin polyelectrolyte fibers and their controlled release properties

Ultrathin fibers comprising 2-weak polyelectrolytes, poly(acrylic acid) (PAA) and poly(allylamine hydrochloride) (PAH) were fabricated using the electrospinning technique. Methylene blue (MB) was used as a model drug to evaluate the potential application of the fibers for drug delivery. The release of MB was controlled in a nonbuffered medium by changing the pH of the solution. The sustained release of MB in a phosphate buffered saline (PBS) solution was achieved by constructing perfluorosilane networks on the fiber surfaces as capping layers. Temperature controlled release of MB was obtained by depositing temperature sensitive PAA/poly(N-isopropylacrylamide) (PNIPAAM) multilayers onto the fiber surfaces. The controlled release of drugs from electrospun fibers have potential applications as drug carriers in biomedical science.     

Synthesis and properties of pH and temperature sensitive P(NIPAAm-co-DMAEMA) hydrogels

In order to investigate the influence of the continuous alkylamide sequence having pH sensitive unit on the temperature sensitivity of poly(N-isopropylacrylamide) (PNIPAAm)-based hydrogel, a monomer, N-(2-(dimethylamino) ethyl)-methacrylamide (DMAEMA), having an ethylamide group as well as an aliphatic tertiary amino group, was designed and synthesized. Hydrogels based on NIPAAm and DMAEMA were prepared via free radical polymerization. The resulted P(NIPAAm-co-DMAEMA) hydrogels were characterized in terms of maximum swelling ratio, swelling kinetics, temperature response kinetics, and effect of pH. The data obtained show that the novel hydrogels have the strong desire to respond to external temperature and pH stimuli. Importantly, because the P(NIPAAm-co-DMAEMA) hydrogels have the continuous alkylamide sequence containing isopropylamide pendant groups from PNIPAAm and ethylamide pendant groups from PDMAEMA, the incorporation of DMAEMA moiety not only provides the pH sensitivity, but also maintains the thermal properties of P(NIPAAm-co-DMAEMA) hydrogels, even as the molar percentage of DMAEMA moiety reaches 14 mol%.     

PEG-grafted chitosan as an injectable thermoreversible hydrogel

PEG-grafted chitosan was formulated such that its solution undergoes a thermally reversed phase transition from an injectable free-flowing solution at low temperature to a gel at body temperature. Aqueous solutions of PEG-grafted chitosan can be prepared at physiological pH values, thereby allowing safe incorporation of bioactive molecules. This injectable thermoreversible hydrogel is potentially suitable for a wide range of biomedical applications, particularly in sustained in vivo drug release and tissue engineering. An aqueous solution of PEG-grafted chitosan polymer is injectable at low temperatures but forms a gel at body temperature.     

聚乙二醇相对分子质量及用量对温敏型PCL-PEG-PCL水凝胶的制备及释药性研究

采用开环聚合法制备PCL-PEG-PCL共聚物,并将其制成温敏性水凝胶,探究了PEG(聚乙二醇)相对分子质量及质量浓度对水凝胶温敏性的影响.水凝胶的相变温度由翻转小瓶法测定.通过FTIR、热分析仪和SEM等技术对其组成及结构进行表征.以疏水性姜黄素(Cur)为模型药物,制备出载Cur PCL-PEG-PCL水凝胶,并研究其体外释药行为.FTIR结果表明:实验制备的共聚物中含有PCL和PEG的链段.热分析结果表明:在25℃~65℃内水凝胶存在相变过程.SEM结果表明:水凝胶剖面具有疏松多孔.体外释药结果表明:PCL-PEG-PCL水凝胶对Cur具有缓释作用,释药机理符合Higuchi骨架溶蚀模型.     

Study on the rapid deswelling mechanism of comb-type N-isopropylacrylamide gels

The shrinking mechanism of comb-type grafted poly(N-isopropylacrylamide) gel was investigated by fluorescence spectroscopy and small-angle X-ray Scattering (SAXS). The SAXS reveals that the microdomain structure with characteristic dimension of 460 Å is developed in the comb-type grafted poly(N-isopropylacrylamide) gel during the shrinking process. Fluorescence spectroscopy together with SAXS observation suggests that the freely mobile characteristics of the grafted chains are expected to show the rapid dehydration to make tightly packed globules with temperature, followed by the subsequent hydrophobic intermolecular aggregation of the dehydrated graft chains. The dehydrated grafted chains created the hydrophobic cores, which enhance the hydrophobic aggregation of the networks. These aggregations of the NIPA chains contribute to an increase in void volume, which allow the gel having a pathway of water molecules by the phase separation.     

A study on the deswelling behaviour of a thermo-responsive hydrogel prepared by radiation polymerization

A new kind of thermo-responsive hydrogel, poly(methacryloyl-DL-alanie methyl ester), was synthesized by means of radiation polymerization. The swelling and deswelling were reversible. The deswelling kinetics changes with the variation of temperature. It was found that a rigid membrane was formed during deswelling at 40°C. In the case of deswelling at 20°C, no skin was found. The hydrogel deswelled uniformly.     

Small-angle neutron scattering study on microstructure of poly(N-isopropylacrylamide)-block-poly(ethylene glycol) in water

By employing small-angle neutron scattering (SANS), we investigated the microstructures of, poly(N-isopropylacrylamide) (PNIPA)-block-poly(ethylene glycol) (PEG) (NE) in deuterated water D₂O, as related to macroscopic behaviors of fluidity, turbidity and synerisis. SANS revealed following results: (i) microphase separation occurs at around above 17 °C in a temperature range of transparent sol below 30 °C. In the microdomain appeared in the transparent sol state, both block chains of PNIPA and PEG are swollen by water; (ii) for the NE solution of polymer concentration W_p > 3.5% (w/v), corresponding to opaque gel above 30 °C, a percolated structure, i.e., network-like domain is formed by NE as a result of macrophase separation due to dehydration of the PNIPA chains. As the temperature increases toward 40 °C, the network domain is squeezed along a direction parallel to the NE interface, which leads to increase of the interfacial thickness given by swollen PEG chains and to the macroscopic synerisis behavior.     

Microporous poly(vinyl methyl ether) hydrogels prepared by γ-ray irradiation at different heating rates

We prepared thermoresponsive and microporous polymer hydrogels by γ-ray irradiation of aqueous solutions poly(vinyl methyl ether) (PVME) at different heating rates. Under all temperature programs, opaque and heterogeneous PVME gels formed, which swelled at temperatures below the lower critical solution temperature and shrank at temperatures above it. All of the samples contained porous and phase-separated structures. The shape and size of the gel pores varied depending on the temperature programs. Gels having a sponge-like continuous porous structure formed only when the radiation-induced crosslinking was carried out at an optimum heating rate, which we found to be 0.11–0.13°C min⁻¹. For temperature changes between 10°C and 40°C, gels with this structure showed rapid volume transitions on a time scale of about a minute.     

Preparation of poly(N-isopropylacrylamide) emulsion gels and their drug release behaviors

Stimuli-sensitive drug delivery systems (DDSs) have attracted considerable attention in medical and pharmaceutical fields; thermosensitive DDS dealing with poly(N-isopropylacrylamide) (poly(NIPA)) have been widely studied. Novel NIPA emulsion gels, i.e., NIPA hydrogels containing distributed oil (oleyl alcohol) microdroplets, were synthesized by means of an emulsion-gelation method in which the polymerization of hydrogels in an aqueous phase in an oil-in-water (O/W) emulsion and the loading of a lipophilic drug (indomethacin) dissolved in an oil phase were accomplished simultaneously. The pulsatile (on-off) drug release from the NIPA emulsion gel loading indomethacin to a phosphate buffered saline (PBS) solution was successfully controlled by a temperature swing between 25 degrees C (release off) and 40 degrees C (release on). The mechanism of the pulsatile drug release was discussed in relation to the diffusion rate, distribution ratio, solvent exchange of NIPA hydrogels, and drug release from an NIPA organogel. The mechanism was as follows: the solvent exchange occurred within the NIPA emulsion gel (the NIPA gel-network absorbed oleyl alcohol with indomethacin) at temperatures above the LCST, and the diffusion rate of indomethacin through the solvent-exchanged gel was higher at 40 degrees C than at 25 degrees C.     

温敏性纤维素/聚N-异丙基丙烯酰胺复合水凝胶的固体核磁共振表征及动力学研究

利用半互穿网络方法将具有温度响应的高分子聚N-异丙基丙烯酰胺(PNIPAM)与天然纤维素复合得到温敏性水凝胶. 通过固体核磁共振的 ¹H, ¹³C CP/MAS(交叉极化/魔角旋转)和QCP(定量交叉极化)等实验手段对复合凝胶的结构进行了定性及定量研究, 并利用固体静态变温核磁共振实验和偶极滤波-自旋扩散实验研究了复合凝胶中PNIPAM分子链段的动力学行为.     

Preparation and properties of poly(N‐isopropylacrylamide)/poly(N‐isopropylacrylamide) interpenetrating polymer networks for drug delivery

A novel poly(N‐isopropylacrylamide) (PNIPA)/PNIPA interpenetrating polymer network (IPN) was synthesized and characterized. In comparison with conventional PNIPA hydrogels, the shrinking rate of the IPN hydrogel increased when gels, swollen at 20 °C, were immersed in 50 °C water. The phase‐transition temperature of the IPN gel remained unchangeable because of the same chemical constituent in the PNIPA gel. The reswelling kinetics were slower than those of the PNIPA hydrogel because of the higher crosslinking density of the IPN hydrogel. The IPN hydrogel had better mechanical strength because of its higher crosslinking density and polymer volume fraction. The release behavior of 5‐fluorouracil (5‐Fu) from the IPN hydrogel showed that, at a lower temperature, the release of 5‐Fu was controlled by the diffusion of water molecules in the gel network. At a higher temperature, 5‐Fu inside the gel could not diffuse into the medium after a burst release caused by the release of the drug on the surface of the gel. © 2004 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 42: 1249–1254, 2004     

Effects of hectorite content on the temperature-sensitivity of PNIPAM microgels

A new method, adopting inorganic clay (synthetic hectorite) as a physical cross-linker, was used to prepare poly(N-isopropylacrylamide) (PNIPAM) microgels via surfactant-free emulsion polymerization. The effect of hectorite content on the temperature-sensitivity of PNIPAM microgels was investigated by means of DLS, UV/Vis and DSC. It was found that, in the absence of surfactant, with increasing hectorite content, the particle size tends to decrease to 300 nm at room temperature, while increases as weight ratio (WR) of hectorite and N-isopropylacrylamide (NIPAM) exceeds 21%. Furthermore, with increasing WR from 7% to 21%, the volume phase transition temperature of PNIPAM microgels has little shift, while decreases slightly when WR increases up to 28%.     

Self-healing mineralized hydrogel scaffolds for stretch-triggered dye release

Hydrogels, with self-healing properties that can self-repair spontaneously when subjected to mechanical stress, are gaining popularity in the biomedical field. Numerous attempts have been made to create distinctive hydrogels with self-healing properties, along with stimuli-responsiveness and biocompatibility. Several techniques exist for fabricating hydrogels, including physical and chemical crosslinking via the creation of covalent bonds, and so on. Here, we prepared self-healing, stimuli-responsive, mineralized hydrogel by simply dissolving Kollidon 90-F, sodium chloride (NaCl), and potassium carbonate (K₂CO₃) in an aqueous solution. The dissociated CO₃²⁻ replaces the water molecules from the Kollidon 90-F polymer backbone and facilitates the cross-linking of the polymer chain, resulting in hydrogel formation. In addition, the in-situ produced sodium carbonate (Na₂CO₃) strengthens the hydrogel network. We optimized the mineralized hydrogels by taking various metal salts and different concentrations of K₂CO₃. The optimized hydrogel showed good stability over a period of time, was able to maintain viscoelastic properties, possessed good self-healing ability, and showed a shape retention ability. The shear-thinning property demonstrated by the optimized hydrogel could open a ray of hope in the bioprinting or 3D printing industry. Further, the stretch-responsive release of dye from the Self-healing mineralized hydrogel (SHMH) matrix confirms the mechanoresponsive behavior of the hydrogel. Overall, the findings could be utilized in the future to fabricate a stable drug delivery system that can autonomously release the drug molecules when stretched by daily processes such as joint movements.     

Closure characteristics of a thermally responsive single ion-track pore determined by size exclusion method

Cross-linked poly(N-isopropylacrylamide) (NIPAAm) gel was grafted on the wall of a single ion-track pore in poly(ethylene terephthalate) (PET). The opening and closing of the pore is controlled by temperature and observed by electric conductivity. In the shrunken state of the gel, ions and molecules can penetrate the membrane through the free volume of the pore. In the swollen state, the gel clogs the pore. Using mixtures of polyethylene glycol (PEG) of various molecular weights and 0.1 N potassium chloride, it was demonstrated that the responsive pore acts as a thermally controllable valve preventing the passage of PEG molecules larger than 2 nm. The mean value of the hydrogel mesh size is estimated to be (1.3±0.05) nm.     

Temperature dependence of free volume of polyacrylamide gels studied by positron lifetime measurements

Changes of positronium (Ps) cavity radii in polyacrylamide and poly(N-isopropylacrylamide) gels were studied from 120 to 300 K by positron lifetime technique and it has been shown that the Ps cavity radius in the hydrogels changes by three or four stages. Temperature dependence of the Ps cavity radius exhibits variations similar to common polymers around the glass transition temperature. Hydrophilicity of the polymer chains significantly affects the Ps cavity radius just below 273 K. These results suggest an important role of free volume on the state of water in hydrogels.