粒径和孔径可控的多孔交联聚苯乙烯微球的制备

采用悬浮聚合方法合成了多孔交联聚苯乙烯微球,研究发现微球的粒径与分散剂含量、水油比、搅拌速度和成孔剂有关,而微球的孔径与成孔剂的种类和含量有关。 增加分散剂的用量,提高水油比和加快搅拌速度都能导致微球的粒径减小。 微球的孔径和粒径均随着成孔剂与聚合物溶度参数差值变大而增加。通过改变以上条件得到粒径为100~300 μm和孔径为8~36 nm的交联度为27%的多孔交联聚苯乙烯微球,并利用光学显微镜、场发射扫描电子显微镜(SEM)和氮气吸附解吸法对微球进行了相应的表征。 得到的微球在固相合成载体中有一定的应用前景。     

Thermosensitive Microparticles Based on Unsaturated Esters of some Poly- and Oligosaccharides: Preparation,Characterization, Drug Inclusion and Release

Summary: The paper concerns the preparation and characterization of hydrogel microparticles based on exopolysaccharide (Gellan, Xanthan) unsaturated derivatives and respectively on cyclodextrin as well as their application for some hydrosoluble and liposoluble drugs inclusion. In the first step the polysaccharide and cyclodextrin unsaturated esters (maleate, acrylate) were synthesized and their hydrogel forming capacity was tested using a grafting-crosslinking free-radical reaction with N-isopropyl acrylamide (NIPAm), at room temperature. For a better control of the crosslinking degree N,N' methylene-bis-acrylamide (BIS), replaced by cyclodextrin tri-acrylate (A-CD) in a few experiments, was used. The microparticles were obtained by using the method in w/o emulsion, in which the dispersed aqueous phase is the reaction mixture and the oil phase is hexane. The particles containing polysaccharide esters showed an average diameter around 100 µm when crosslinking was achieved with BIS. They were smaller than those crosslinked with A-CD, which are in the range of 200-300 µm; the particles based on Xanthan maleate were smaller than Gellan maleate based ones. Even much smaller particles (2-2.5 µm in diameter) were obtained by starting from A-CD grafted-crosslinked systems. The synthesized microparticles are able to include chloramphenicol, as well as progesterone; the drug is slowly released according to diffusion controlled kinetics. The application of these microparticles in emergency ophthalmic treatments is possible as a result of their thermal sensitivity; they can collapse and release the drug instantly when placed in contact with the human eye, at 37 °C.     

Preparation of Monodispersed Polymer Microspheres by SPG Membrane Emulsification‐Solvent Evaporation Technology

The membrane emulsification coupled with solvent evaporation was adopted to prepare monodispersed polystyrene (PS) microspheres. Firstly, stable oil‐in‐water emulsion has been successfully obtained by pressing PS solution through SPG membrane into continuous phase at appropriate pressures. Then monodispersed PS microspheres with size of 2–20 µm were obtained following the removal of solvent. The size of the PS microspheres was strongly dependent on the mean pore size of SPG membrane and concentration of PS solution. Furthermore, the effect of emulsion stability, operation pressure and emulsifier on the size and size distribution of microspheres were systemically investigated. Finally, the surface character of PS microspheres was examined via SEM.     

Polymer Structure‐Guided Self‐Assisted Preparation of Poly(ester‐thioether)‐Based Hollow Porous Microspheres and Hierarchically Interconnected Microcages for Drug Release

Porous polymer microspheres (PPMs) have been widely applied in various biomedical fields. Herein, the self‐assisted preparation of poly(ester‐thioether)‐based porous microspheres and hierarchical microcages, whose pore sizes can be controlled by varying the polymer structures, is reported. Poly(ester‐thioether)s with alkyl side chains (carbon atom numbers were 2, 4, and 8) can generate hollow porous microspheres; the longer alkyl chain length, the larger pore size of microspheres. The allyl‐modified poly(ester‐thioether) (PHBDT‐g‐C₃) can form highly open, hierarchically interconnected microcages. A formation mechanism of these PPMs is proposed; the hydrophobic side chains‐mediated stabilization of oil droplets dictate the droplet aggregation and following solvent evaporation, which is the key to the formation of PPMs. The hierarchically interconnected microcages of PHBDT‐g‐C₃ are due to the partially crosslinking of polymers. Pore sizes of PPMs can be further tuned by a simple mixing strategy of poly(ester‐thioether)s with different pore‐forming abilities. The potential application of these PPMs as H₂O₂‐responsive vehicles for delivery of hydrophobic (Nile Red) and hydrophilic (doxorubicin hydrochloride) cargos is also investigated. The microspheres with larger pore sizes show faster in vitro drug release. The poly(ester‐thioether)‐based polymer microspheres can open a new avenue for the design of PPMs and provide a H₂O₂‐responsive drug delivery platform.     

Characterization of polysuccinate and hydroxyapatite‐based nanocomposites containing poly(ester‐anhydride) microspheres

Repair and regeneration of bone defects with particular shape may be enhanced by in situ forming biomaterials which can be used in minimal invasive surgery. This study is aimed to prepare novel in situ forming biodegradable nanocomposites based on poly(3‐allyloxy‐1,2‐propylene) succinate (PSAGE) and nanosized hydroxyapatite (HA). These nanocomposite materials contain poly(ester‐anhydride) (PEA) microspheres embedded in a polyester matrix prepared by crosslinking PSAGE with oligo(1,2‐propylene maleate) and methacrylic monomers. Methyl methacrylate and one of hydrophilic oligo(ethylene glycol) methacrylates with different functionality and various length of oligooxyethylene chains were used as polymerizable diluents. Incorporation of microspheres which degrade faster than crosslinked polyester matrices enables formation of porous structure in situ. The obtained materials are liquid before curing and harden in several minutes with moderate exothermic effect. The effect of the composition of nanocomposite materials on selected properties, such as water sorption, mechanical strength, porosity and hydrolytic degradation process, was investigated. Rheological behavior and injectability of liquid formulations were studied. Analysis by energy dispersive spectroscopy confirmed the presence of characteristic features of HA in the nanocomposite materials. The morphology of the cured nanocomposites subjected to hydrolytic degradation was evaluated by scanning electron microscopy. The MTS cytotoxicity assay was carried out for extracts from crosslinked materials using hFOB1.19 cells. It was found that the extracts exhibit a dose‐dependent cytotoxic response. Copyright © 2014 John Wiley & Sons, Ltd.     

Preparation of porous polylactide microspheres by emulsion‐solvent evaporation based on solution induced phase separation

Porous polylactide (PLA) microspheres were fabricated by an emulsion‐solvent evaporation method based on solution induced phase separation. Scanning electron microscopy (SEM) observations confirmed the porous structure of the microspheres with good connectivity. The pore size was in the range of decade micrometers. Besides large cavities as similarly existed on non‐porous microspheres, small pores were found on surfaces of the porous microspheres. The apparent density of the porous microspheres was much smaller than that of non‐porous microspheres. Fabrication conditions such as stirring rate, good solvent/non‐solvent ratio, PLA concentration and dispersant (polyvinyl alcohol, PVA) concentration had an important influence on both the particle size and size distribution and the pore size within the microspheres. A larger pore size was achieved at a slower stirring rate, lower good solvent/non‐solvent ratio or lower PLA concentration due to longer coalescence time. Copyright © 2005 John Wiley & Sons, Ltd.     

聚己二酸丁二酯纳米纤维构建的微球的制备

建立了采用异相成核和可控水解相结合的方法制备由纳米纤维构建的聚合物微球的新方法.根据多取代卞叉山梨醇(TM6)对聚己二酸丁二酯(PBA)的异相成核作用以及结晶形态的影响,采用两种乳液溶剂挥发法、并在聚合物溶液中加入成核剂TM6制备了PBA微球,研究了成核剂含量对PBA微球在酶促降解之后形态变化的影响.研究结果表明,二次乳液溶剂挥发法可以制备具有多孔结构的PBA微球,这种多孔结构有利于酶溶液进入到微球内部,促进PBA微球的均匀水解,最终获得由PBA纳米纤维构建的微球.当TM6的含量为3 wt%时,采用二次乳液溶剂挥发法制备的PBA微球,经过5 h酶促降解处理,可以得到表面和内部由PBA纳米纤维均匀组成的微球.进一步的细胞实验表明,微球的纳米纤维结构,有利于MG-63细胞在聚合物微球上的黏附、铺展和向内生长.     

Effect of method of preparation and process variables on controlled release of insoluble drug from chitosan microspheres

An inexpensive and simple method was adopted for the preparation of chitosan microspheres, crosslinked with glutaraldehyde (GA), for the controlled release of an insoluble drug‐ibuprofen, which is a commonly used NSAID (non‐steroidal anti‐inflammatory drug). The chitosan microspheres were prepared by different methods and varying the process conditions such as rate of stirring, concentration of crosslinking agent, and drug:polymer ratio in order to optimize these process variables on microsphere size, size distribution, degree of swelling, drug entrapment efficiency, and release rates. The absence of any chemical interaction between drug, polymer, and the crosslinking agent was confirmed by Fourier transform infrared (FTIR) spectroscopy, differential scanning calorimetry (DSC), and thermogravimetric analyses (TGA) techniques. The microspheres were characterized by optical microscopy, which indicated that the particles were in the size range of 30–200 µm and scanning electron microscopy (SEM) studies revealed a smooth surface and spherical shape of microspheres. The microsphere size/size distributions were increased with the decreased stirring rates as well as GA concentration in the suspension medium. Decreasing the concentration of crosslinker increased the swelling ratio whereas extended crosslinking exhibited lowered entrapment efficiency. The in vitro drug release was controlled and extended up to 10 hr. Copyright © 2007 John Wiley & Sons, Ltd.     

Highly porous poly(lactide‐co‐glycolide) microparticles for sustained tiotropium release

In this study, porous poly(lactide‐co‐glycolide) (PLGA) microparticles with low mass density and large particle size were developed for chronic obstructive pulmonary disease treatment using anticholinergic drug (tiotropium). The porous PLGA microparticles were prepared by the water‐in‐oil‐in‐water (W₁/O/W₂) multi‐emulsion method using PLGA polymer and ammonium bicarbonate (as a porogen). Herein, soluble starch was incorporated in porous PLGA microparticles for long‐term tiotropium release. In vitro drug release studies determined that the rapid release of tiotropium from porous PLGA microparticles was reduced because of the high viscosity of the incorporated starch. Tiotropium release from porous PLGA microparticles continued up to 3 days. Furthermore, the inhaled microparticles showed longer drug residence in in vivo lung epithelium. Copyright © 2013 John Wiley & Sons, Ltd.     

不同溶剂制备的聚乳酸多孔微球的形成机理

利用改进的双乳液溶剂挥发法制备了多孔聚乳酸( PLA)微球.通过采用具有不同沸点和水溶性的有机溶剂制备得到不同多孔结构的PLA微球.结果发现以二氯甲烷、氯仿和甲苯为溶剂制备的微球具有相似的均匀多孔结构,而以乙酸乙酯制备的微球却具有中空结构和多孔的壳层.通过进一步的实验研究了溶剂种类对于微球多孔结构的影响.结果表明溶剂的...     

Synthesis of fast-swelling superabsorbent hydrogels: effect of crosslinker type and concentration on porosity and absorption rate

Fast-swelling highly porous superabsorbent hydrogels were synthesized through a rapid solution polymerization of concentrated partially neutralized acrylic acid under normal atmospheric conditions. Acetone and sodium bicarbonate were used as porosity generators (porogens) during polymerization process for porosity generation. N,N^′-methylenebisacrylamide (MBA) and 1,4-butanedioldiacrylate were used as the water- and the oil-soluble crosslinkers, respectively. The temperature changing of the reaction mixture during polymerization and foam formation process was monitored and investigated in details. Time and sequence of addition of the porogens and gelation time were recognized to be important to increase efficiency of the porogens. The concentration of the crosslinkers on gelation time was optimized to achieve highly porous products. It was found that higher crosslinker concentration, especially in the case of MBA, causes decreased gelation times. Shorter gelation time resulted in more porogen bubbles trapped in the viscose reaction mixture led to products with higher porosity. The effect of type and concentration of the crosslinking agents on the process and swelling behavior of the hydrogels (in water and saline solutions) were investigated. Power law relationships were found for the variation of swelling in terms of either crosslinker or saline concentration. Less sensitivity to the change of salinity was achieved by employing higher amount of crosslinker.     

Drug release behaviors of a pH/thermo-responsive porous hydrogel from poly(N-acryloylglycinate) and sodium alginate

A pH/thermo-responsive hydrogel with porous structure (HME), composed of poly(N-acryloylglycine methyl ester), poly(N-acryloylglycine ethyl ester) and sodium alginate (SA) was prepared for the controllable drug carrier. The resultants, CO₂ and CaCl₂ from the reaction of CaCO₃ particles and HCl act as pore-forming and crosslinking of SA, respectively. The porous HME was characterized by differential scanning calorimetry, scanning electron microscopy (SEM), Fourier transform infrared spectroscopy and surface area and porosity analysis. The sheet, porous structure was clearly observed by the SEM measurement and the specific surface area of HME was evidently increased with an increase of CaCO₃ content. At pH 2.1 phosphate buffered saline (PBS), the release amount of caffeine at room temperature was only 7.2 % within 600 min, while this value approached to 65.3 % at pH 7.4 PBS. Additionally, the cumulative release at 37 °C is much higher than that at room temperature due to the thermo-sensitivity of HME. The experimental results indicated that porous HME has a potential to be used as the promising release-controlled drug carrier in the biomedical fields.     

Synthesis and copolymerization of oligo(lactic acid) derived norbornene macromonomers with amino acid derived norbornene monomer: Formation of the 3D macroporous scaffold

Norbornene macromonomers 2 and 3 bearing 10‐ and 20‐mers of lactide were synthesized by ring‐opening polymerization of lactide using 5‐norbornene‐2, 3‐exo‐exo‐dimethanol as an initiator and DBU as a catalyst. Macromonomers 2 and 3 were copolymerized with amino acid derived norbornene monomer 1 , using the Grubbs 2nd generation ruthenium catalyst. The random and block copolymers with M_n's ranging from 28,000 to 180,000 were obtained almost quantitatively where the M_n's of the block copolymers were higher than those of the random ones. Three‐dimensional macroporous structure polymers with average pore size of 10 µm could be found in poly( 1 ) and the block co‐polymer of 1 and 2 or 1 and 3 at the high ratio of 1 . Meanwhile, poly( 2 ) and poly( 3 ) along with block and random copolymers with low ratio of 1 exhibit much larger pores in the range of 50–300 µm. The porosity increased with increase in the unit ratio of 1 . The compressive strength of the porous structure of poly( 2 ) and poly( 3 ) was improved by the copolymerization with 1 . © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2015 , 53, 1660–1670     

Monodisperse porous polymer particles: Formation of the porous structure

Monodisperse porous styrene-divinylbenzene copolymer particles were prepared via seeded emulsion polymerization using a mixture of linear polymer (polystyrene seed) and non-solvent as inert diluent. Experimental evidence was presented to describe the mechanism of formation of porous polymer particles during the copolymerization and solvent extraction stages, in which porosity was a consequence of phase separation in the presence of diluents. Pore structure formation was investigated by changes in copolymerization kinetics, gel content, crosslinking density, particle morphology, surface area, pore volume, and pore size distribution. The process of copolymerization was presented, based on the concepts of production, agglomeration, and fixation of the interior gel microspheres of polymer particles. A portion of linear polymer used as diluent was found to participate in the network structure while the porous matrix was built-up. The influence of the removal of the linear polymer from the matrix pores during the solvent extraction process on the porous structure was also discussed.     

Synthesis of porous poly(styrene-co-acrylic acid) microspheres through one-step soap-free emulsion polymerization: whys and wherefores

Synthesis of porous poly(styrene-co-acrylic acid) (PS-co-PAA) microspheres through one-step soap-free emulsion polymerization is reported. Various porous PS-co-PAA microspheres with the particle size ranging from 150 to 240 nm and with the pore size ranging from 4 to 25 nm are fabricated. The porous structure of the microspheres is confirmed by the transmission electron microscopy measurement and Brunauer-Emmett-Teller (BET) analysis. The reason for synthesis of the porous PS-co-PAA microspheres is discussed, and the phase separation between the encapsulated hydrophilic poly(acrylic acid) segment and the hydrophobic polystyrene domain within the PS-co-PAA microspheres is ascribed to the pore formation. The present synthesis of the porous PS-co-PAA microspheres is anticipated to be a new and convenient way to fabricate porous polymeric particles.     

Fabrication of poly(lactide‐co‐glycolide) scaffold embedded spatially with hydroxyapatite particles on pore walls for bone tissue engineering

Poly(lactide‐co‐glycolide) (PLGA) scaffolds embedded spatially with hydroxyapatite (HA) particles on the pore walls (PLGA/HA‐S) were fabricated by using HA‐coated paraffin spheres as porogens, which were prepared by Pickering emulsion. For comparisons, PLGA scaffolds loaded with same amount of HA particles (2%) in the matrix (PLGA/HA‐M) and pure PLGA scaffolds were prepared by using pure paraffin spheres as porogens. Although the three types of scaffolds had same pore size (450–600 µm) and similar porosity (90%–93%), the PLGA/HA‐S showed the highest compression modulus. The embedment of the HA particles on the pore walls endow the PLGA/HA‐S scaffold with a stronger ability of protein adsorption and mineralization as well as a larger mechanical strength against compression. In vitro culture of rat bone marrow stem cells revealed that cell morphology and proliferation ability were similar on all the scaffolds. However, the alkaline phosphatase activity was significantly improved for the cells cultured on the PLGA/HA‐S scaffolds. Therefore, the method for fabricating scaffolds with spatially embedded nanoparticles provides a new way to obtain the bioactive scaffolds for tissue engineering. Copyright © 2011 John Wiley & Sons, Ltd.     

Investigation of the thermal behavior of 4-vinylpyridine–trimethylolpropane trimethacrylate copolymeric microspheres

The study describes the thermal properties of porous microspheres synthesized with functional monomer 4-vinylpyridine (4VP) and crosslinking agent trimethylolpropane trimethacrylate (TRIM). Polymeric 4VP–TRIM microspheres were prepared via seed polymerization, using polystyrene microbeads as a shape template. The resulting 4VP–TRIM microspheres were in the range of 9–12 μm, with specific surface area of about 200 m² g^?1. The thermal properties of 4VP–TRIM materials were evaluated by thermogravimetry and differential scanning calorimetry. By TG/FTIR/MS, it was observed that new porous materials exhibited multi-staged decomposition patterns, different from poly(TRIM) microspheres. DSC and TG experiments showed that water molecules were absorbed on the materials’ surface. The synthesized 4VP–TRIM microspheres exhibited rather high thermal stability. Their initial decomposition temperature was about 300 °C. During the microspheres’ decomposition, an evolution of carbon dioxide, water, and carbon monoxide as main gases, as well as of pyridine and aliphatic compounds, was observed. It was confirmed that the evolved pyridine accelerated the degradation of copolymeric network.     

Fabrication of Porous Silica Microspheres Under the Assistance of Solid Template

Spherical porous silica microparticles were synthesized by a sol-gel process in the presence of porous CaCO₃ particles, followed by removal of the carbonate templates. The resulting silica particles had very high porosity and wide pore size distribution, whose surface area and pore volume reached up to 367.3 m²/g and 0.72 mL/g, respectively. With a larger amount of the tetraethyl orthosilicate used, hollow silica microspheres were further obtained. Characterization was made to confirm the chemical and physical structures and purity of the silica microspheres. Spontaneous deposition of tetramethyl rhodamine isothiocyanate labeled dextran into the microspheres was also observed due to the charge attraction.     

p-Nitrophenol permeability and temperature characteristics of an acryloyl-L-proline methyl ester-based porous gel membrane

Thermoresponsive porous gel membranes were synthesized by a simultaneously occurring process consisting of radiation-induced polymerization and crosslinking in aqueous solutions at various concentrations of acryloyl-L -proline methyl ester(A-ProOMe) without a crosslinker. Permeation of p-nitrophenol (PNP) through a thermoresponsive porous gel membrane obtained at a monomer concentration of 80% (w/w) drastically reduced around 14°C, the lower critical solution temperature (LCST) of linear poly(A-ProOMe) in water, from 0.60 × 10⁻³ cm/min at 10°C to no permeation at 18°C, accompanied by changes in both size and shape of pores associated with gel shrinkage. Moreover, it was found that porous gel membranes with a porosity of approximately 60% had a greater PNP permeability constant through porous gel membranes with mutually connected pores obtained at a monomer concentration of 50% (w/w) than individually supported pores obtained at a monomer concentration of 70% (w/w). © 1998 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 36: 1495–1500, 1998     

Infrared spectroscopy studies of the cyclic anhydride as the intermediate for the ester crosslinking of cotton cellulose by polycarboxylic acids. III. Molecular weight of a crosslinking agent

Polycarboxylic acids have been used as nonformaldehyde crosslinking agents for cotton fabrics to replace the traditional N-methylol reagents. In this research, we compared 1,2,3,4-butanetetracarboxylic acid (BTCA) with poly(maleic acid) (PMA) as crosslinking agents for cotton cellulose. BTCA and PMA have similar molecular structures with carboxyl groups bonded to their molecular backbones, and both form five-membered cyclic anhydride intermediates during a curing process. However, BTCA is a more effective crosslinking agent for cotton cellulose than PMA. This is mainly attributed to the differences in the mobility of the anhydride intermediates to access the cellulosic hydroxyl groups during a curing process. The mobility of the anhydride intermediate of PMA is reduced due to its molecular size and multiple bonding between a PMA molecule and cellulose. Consequently, more anhydride and less ester are detected on the cotton fabric treated with PMA than on the fabric treated with BTCA. The amount of the unreacted anhydride intermediate on the fabric treated with PMA is reduced whereas the amount of ester is increased when another hydroxyl-containing compound of low molecular weight is present. Thus, the infrared spectroscopy data show a clear link between the molecular weight of a polycarboxylic acid and its effectiveness for crosslinking cotton cellulose. © 1997 John Wiley & Sons, Inc.