膜乳化-溶剂挥发法制备表面羧基功能化苯乙烯-马来酸酐共聚物微球

以苯乙烯-马来酸酐共聚物(PSMA)为原料,利用膜乳化-溶剂挥发法,成功制备了表面光滑、尺寸均一的表面羧基功能化聚合物微球.研究表明:将膜乳化法和溶剂挥发法相结合,可以有效提高微球粒径的均一性,乳化剂种类及浓度、连续相流速、分散相中聚合物浓度等参数对微球粒径及粒径分布有显著影响.此外,利用盐酸使微球酸酐基团水解,可以得...     

微米级单分散共聚物微球的制备

用分散聚合法制备了苯乙烯 甲基丙烯酸甲酯微米级单分散共聚物微球 ,粒径为 5 4 μm .将分散聚合体系与乳液聚合体系进行了比较 ,并对共聚物微球的形貌、粒径分布及共聚情况进行了表征研究 .     

Preparation of hollow PPy (HPPy) microspheres via template methods with characterization of properties

Template-synthesis method was one of the important methods for the preparation of hollow microspheres. In present work, polystyrene (PS) microspheres were initially synthesized and effects of reaction conditions on the particle size and distribution of PS microspheres were studied. Then sulfonated PS (SPS) microspheres and spherical core (PS) /shell (polypyrrole, PPy) were synthesized by sulfonated and template method respectively. The method was that pyrrole (Py) on the surface of SPS microspheres were polymerized. Then PS (core)-PPy (shell) microspheres by dissolving PS inner core in N, N-Dimethylformamide (DMF), and hollow polypyrrole (HPPy) microspheres were obtained (Figure 1). Thereafter, HPPy microspheres were characterized by fourier transform infrared spectroscopy, X-ray diffraction, particle size analyzer, scanning electron microscope, thermal gravimetric analysis and KDY-4 four-probe resistance meter. The results showed that the size range of PS microspheres were 200～300 nm. HPPy microspheres have been successfully synthesized with good electrical conductivity and excellent thermal stability.     

单分散聚苯乙烯微球的制备及表征

应用膜乳化-液中干燥法成功制备出粒径为2～20μm的单分散聚苯乙烯(PS)微球.PS微球的粒径主要由膜孔径决定,其值约为膜孔径的2倍;PS溶液的浓度对其也有一定的影响.膜乳化过程中的压力对微球粒径的分散性有很大的影响,在一定压力范围内,粒径呈单分散.在分散相中加入致孔剂,制备出表面多孔的PS微球.采用复乳-液中干燥法制备出中空PS微球.     

反应原料组成对单分散苯乙烯微球粒径及其分布的影响

采用分散聚合工艺制备微米级单分散聚苯乙烯微球，并对分散聚合反应的内部影响因素(分散稳定剂、助稳定剂、单体、引发剂)进行了研究．结果表明，随着分散稳定剂和助稳定剂用量的增加，聚苯乙烯微球的粒径减小；随着单体和引发剂用量的增加，聚苯乙烯微球的粒径增大．分散稳定剂和单体用量是影响聚苯乙烯微球粒径分布的两个主要内部因素．     

原子转移自由基聚合法制备超大孔聚合物微球

以甲基丙烯酸缩水甘油酯为单体(GMA)、乙二醇二甲基丙烯酸酯(EDMA)为交联剂,采用原子转移自由基聚合法(ATRP)制备了PGMA-EDMA大孔聚合物微球,采用傅里叶变换红外光谱、扫描电子显微镜及压汞法对PGMA-EDMA微球进行了表征.研究结果表明,原子转移自由基聚合法制备的PGMA-EDMA微球的孔径尺寸及比表面积均大于普通自由基聚合法(CFRP)制备的PGMA-EDMA;ATRP法制备的PGMAEDMA微球的颗粒尺寸(100~400 nm)明显小于CFRP法制备的PGMA-EDMA微球的颗粒尺寸(1000 nm).PGMA-EDMA(ATRP)的微球粒径尺寸分布优于PGMA-EDMA(CFRP).因此PGMA-EDMA(APRP)微球在快速蛋白分离纯化方面有潜在的应用前景.     

反应条件对聚合物微球粒径及其分布影响

采用分散聚合的工艺制备出了微米级单分散聚苯乙烯微球，并对分散聚合反应的外部影响因素(反应介质极性、反应体系温度、搅拌速度)进行了研究，研究结果表明：随着反应介质极性的增加，聚苯乙烯微球的粒径战小，粒径分布变化不大；随着反应体系温度的增加，聚苯乙烯微球的粒径增大，粒径分布变化不大，在满足粒径和粒径分布要求的前提下，搅拌速度以低速为宜。     

膜乳化-液中干燥法制备单分散高分子微球

粒径可控的单分散高分子微球,在分析化学中可用作高效液相色谱填料^[1,2];在化学工业中可用作催化剂载体;在生物领域中用于药物释放、癌症与肝炎等临床诊断、细胞标记与识别等^[3].高分子微球的制备方法大致可分为两类,一是利用由单体出发的聚合反应或缩聚反应形成微球,二是高分子溶液经物理或物理化学手段处理后形成微球^[4]     

聚苯乙烯微球表面接枝丙烯腈的研究

采用分散聚合法制备出平均粒径为3.85 μm的窄分布聚苯乙烯微球， 并在此基础上引入第二单体丙烯腈进行共聚反应， 制备出平均粒径为4.02 μm的窄分布苯乙烯-丙烯腈共聚物微球. 对聚苯乙烯微球和苯乙烯-丙烯腈共聚物微球进行了形貌及粒径、红外光谱、差示扫描量热法(DSC)分析， 结果表明丙烯腈基团均匀分布在聚苯乙烯微球表面， 提高了聚苯乙烯微球表面的极性.     

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.     

Influence of manufacturing parameters on development of contraceptive steroid loaded injectable microspheres

The main objective of this work was to develop a system consisting of polymeric microspheres loaded with steroid drugs. The drugs were encapsulated using biodegradable poly(lactide-co-glycolide) (PLG) and poly(epsilon-caprolactone) (PCL) by double emulsion solvent evaporation method. The lipophilic drugs, levonorgestrel and ethinylestradiol were made soluble by adding ethanol/water mixture. The effects of parameters like polymer concentration and stabilizer concentration were studied on the size, size distribution, surface properties and loading efficiencies of microspheres. The formulated microspheres were smooth, spherical and uniform in shape and size. Fourier transformed infrared spectroscopy and differential scanning calorimetry studies seemed to confirm the absence of chemical interaction between the drugs and the polymers, while the drugs were dispersed in the polymer. The increase in polymer concentrations increased the size as well as the loading efficiency of microspheres. Data obtained in this study demonstrated that the PLG/PCL microspheres may be a suitable polymeric carrier for long acting injectable drug delivery.     

INVESTIGATION OF POLYDL-LACTIDE-b-POLY（ETHYLENE GLYCOL）-b-POLYDL-LACTIDE MICROSPHERES CONTAINING PLASMID DNA

PolyDL-lactide (PDLLA) and the block copolymer, polyDL-lactide-b-poly(ethylene glycol)-b-polyDL-lactide (PELA) were used as the microsphere matrix to encapsulate plasmid DNA. The PDLLA, PELA, pBR322-1oaded PDLLA and pBR322-1oaded PELA microspheres were prepared by solvent extraction method based on the formation of multiple w1/o/w2 emulsion. The microspheres were characterized by surface morphology, mean particle size, particle size distribution and loading efficiency. The integrity of DNA molecules after being extracted from microspheres was determined by agarose gel electrophoresis. The result suggested that plasmid DNA molecules could retain their integrity after being encapsulated by PELA. The PELA microspheres could prevent plasmid DNA from being digested by DNase. The in vitro degradation and release profiles of plasmid DNA-loaded microspheres were measured in pH - 7.4 buffer solution at 37℃. The in vitro degradation profiles of the microspheres were evaluated by the deterioration in microspheres surface morphology, the molecular weight reduction of polymer, the mass loss of microspheres, the changes of pH values of degradation medium, and the changes of particle size. The in vitro release profiles of the microspheres were assessed by measurement of the amount of DNA presented in the release medium at determined intervals. The release profiles were correlation with the degradation profiles. The release of plasmid DNA from PELA microspheres showed a similar biphasic trend, that is, an initial burst release was followed by a slow, but sustained release.     

两亲磁性高分子微球的合成与表征

在Fe3O4磁流体存在下 ,通过苯乙烯与聚氧乙烯大分子单体 (MPEO)分散共聚制备两亲磁性高分子微球 .研究了聚氧乙烯大分子单体对微球粒径的影响 .用扫描电子显微镜 (SEM)、原子力显微镜 (AFM)表征了磁性微球的粒径、表面形貌以及表面粗糙度 ,用傅立叶红外光谱 (FTIR)鉴定了共聚物的结构 .随着聚合物中聚氧乙烯大分子单体含量的增加 ,微球表面的粗糙度增加 ,通过改变共聚物中MPEO的含量 ,可以得到含有 0 4～ 3 5mg g羟值的两亲磁性高分子微球     

沉淀聚合法制备右旋邻氯扁桃酸分子印迹聚合物微球

以右旋邻氯扁桃酸为模板,丙烯酰胺、乙二醇二甲基丙烯酸酯分别为功能单体和交联剂,采用沉淀聚合法制备了分子印迹聚合物微球,讨论了反应介质用量、聚合温度、引发剂的种类和用量对印迹微球的影响。实验表明：分子印迹微球与传统本体聚合法制备的聚合物相比具有更高的特异识别能力,通过Scatchard分析研究了聚合物的选择结合性能,结果表明分子印迹聚合物微球在识别右旋邻氯扁桃酸分子的过程中存枉两类结合位点,而空白聚合物微球只存在一类结合位点。     

Graft copolymers having hydrophobic backbone and hydrophilic branches. XI. Preparation and thermosensitive properties of polystyrene microspheres having poly (N-isopropylacrylamide) branches on their surfaces

Thermosensitive microspheres with 0.4–1.2 μm diameter consisting of a polystyrene core and poly(N-isopropylacrylamide) (polyNIPAAm) branches on their surfaces were prepared by the free radical polymerization of a polyNIPAAm macromonomer and styrene in ethanol. Electron spectroscopy for chemical analysis (ESCA) of the microsphere surface suggested that polyNIPAAm chains were favorably located on the surface of the microspheres. The morphology of the microspheres was observed by transmission electron micrograph (TEM) and the particle size of was estimated by submicron particle analyzer. The molecular weight of the polyNIPAAm macromonomer, the ratio of the macromonomer and styrene, and the polymerization temperature affected the particle size. Thermosensitive properties of polyNIPAAm-coated polystyrene microspheres were evaluated by the turbidity of their dispersion solutions and the hydrodynamic size of the miocrospheres. The transmittance in dispersion solutions changed clearly, similar to oligoNIPAAm and polyNIPAAm macromonomers. In addition, the particle size of microspheres decreased with rising temperature. These results were explained by the thermosensitivity of polyNIPAAm branches on the microsphere surface. © 1996 John Wiley & Sons, Inc.     

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.     

聚二乙烯基苯微球的合成及其表征研究

采用分散聚合方法制备了聚二乙烯基苯微球 ,研究了引发剂、稳定剂、单体 溶剂比例和溶剂种类对微球粒径及其分布的影响 ,在适当的条件下可以得到平均粒径较大、粒径分布较窄的微球 .用红外光谱法研究了聚合物微球内稳定剂、悬挂双键以及对位和间位二乙烯基苯含量随聚合过程的进行发生的变化 .测得的微球TG曲线表明 ,聚合物微球具有良好的热稳定性 .     

Controlling morphology and particle size of hollow poly(styrene-divinylbenzene) microspheres fabricated by template-based method

Hollow poly(styrene–divinylbenzene) (P(S-DVB)) microspheres were fabricated via template-based method including synthesis of silica particles by sol-gel method, preparation of silica/P(S-DVB) particles by dispersion polymerization and chemical etching of silica cores by NaOH solution. TEM, FTIR and TG analyses confirmed that the hollow P(S-DVB) microspheres were successfully obtained. The morphology of hollow P(S-DVB) microspheres could be controlled by adjusting the amounts of DVB, AIBN and VTES, and the round-ball-like hollow P(S-DVB) microspheres were fabricated when the amount of DVB, AIBN and VTES was 30.0?wt%, 5.0?wt% and 30.0?vol% respectively. Both the size of silica particles and amount of monomers were regarded as the two key factors to control the particle size of the round-ball-like hollow P(S-DVB) microspheres.     

Preparation and characterization of biodegradable microspheres containing hepatitis B surface antigen

Poly-DL-lactide-poly(ethylene glycol) (PELA) microspheres containing Hepatitis B surface antigen (HBsAg) were elaborated by a solvent extraction method based on the formation of a double water/oil/water (w/o/w) emulsion. Microspheres were characterized in terms of morphology, size and size distribution, encapsulation efficiency, and the efficiency of microsphere formation (EMF). Transmission electron microscopy (TEM) and polyacrylamide gel electrophoresis (PAGE) were used to investigate the structural integrality of HBsAg encapsulated in PELA microspheres. The release profile was investigated by the measurement of antigen present in the release medium at various intervals. The PELA-10 microspheres displayed the highest antigen encapsulation efficiency (about 80%), and antigen molecules could be stabilized in the PELA-10 microspheres during the preparation process. It suggested that the PELA microspheres had a great potential as a new polymer adjuvant for HBsAg. The release of Hepatitis B surface antigen from poly-DL-lactide-poly(ethylene glycol) microspheres.     

The influence of chitosan on in vitro properties of Eudragit RS microspheres

Eudragit RS microspheres containing chitosan hydrochloride were prepared by the solvent evaporation method using acetone/liquid paraffin solvent system and their properties were compared with Eudragit RS microspheres without chitosan, prepared in our previous study. Different stirring rates were applied (400-1200 rpm) and drug content, Higuchi dissolution rate constant, surface and structure characteristics of the microspheres were determined for each size fraction. An increase in average particle size with a reduction of stirring rate appeared in limited interval in both series. The average particle size of microspheres without chitosan, prepared at the same stirring rate, was smaller. Pipemidic acid content increased with increasing fraction particle size, but not with increasing stirring rate as it was observed for microspheres without chitosan. We presume that high pipemidic acid content in larger microspheres is a consequence of cumulation of undissolved pipemidic acid particles in larger droplets during microspheres preparation procedure. Pipemidic acid release was faster from microspheres with chitosan and no correlation between Higuchi dissolution rate constant and stirring rate or fraction particle size was found, though it existed in the system without chitosan. Structure and surface characteristics of microspheres observed by scanning electron microscope (SEM) were not changed significantly by incorporation of chitosan. But in contrast with microspheres without chitosan, the surface of chitosan microspheres was more porous after three hours of dissolution. It is supposed that the influence of particle size fraction and stirring rate on release characteristics is expressed to a great extent through porosity and indirectly through total effective surface area, but the incorporation of highly soluble component i.e. chitosan salt hides these effects on drug release. In conclusion, changes in biopharmaceutical properties due to varying stirring rate and fraction particle size exhibited the same direction as those reported for the microspheres without chitosan, although they are less expressed because of increased experimental variability, likely caused by chitosan.