温度敏感性P(MEO2MA-co-OEGMA)共聚物的合成与性质

利用原子转移自由基聚合(ATRP)方法合成了组成递变的2-甲基-2-丙烯酸-2-(2-甲氧基乙氧基)乙酯(MEO₂MA)与寡聚乙二醇甲醚甲基丙烯酸酯(OEGMA)共聚物P(MEO₂MA-co-OEGMA). 核磁共振氢谱(¹HNMR)和凝胶渗透色谱(GPC)表征了聚合物的结构、分子量及其分布. 通过测定透光率、粘度、激光粒度分析了共聚物组成对共聚物低临界溶解温度(LCST)的影响, 考察了共聚物组成、浓度、盐浓度、盐种类、温度对其溶液相行为的影响. 结果表明: 所合成的共聚物具有温度敏感性, 其LCST 可以通过合成时共聚单体MEO₂MA与OEGMA投料比的改变来调控, 随着OEGMA量的增加共聚物的LCST升高, 共聚物溶液浓度升高其LCST减小, 随盐溶液浓度的增大共聚物的LCST降低, 共聚物的LCST降低主要受盐溶液中阴离子价数的影响; HCl的引入使共聚物水溶液的LCST降低; NaOH的引入使共聚物水溶液的LCST升高.     

温度/pH敏感性嵌段共聚物P(HEMA-co-DEAEMA)-b-PDEAM-b-P(DEAEMA-co-HEMA)的合成与性质研究

利用原子转移自由基聚合方法(ATRP)合成了组成递变的嵌段共聚物P(HEMA-co-DEAEMA)-b-PDEAM-b- P(DEAEMA-co-HEMA). 用FTIR, ¹H NMR和GPC技术表征了聚合物的组成、结构、分子量及其分布. 通过透光率测定、粘度、激光粒度分析和透射电镜研究了共聚物组成、温度及溶液pH对其溶液相行为和胶束化作用的影响. 结果表明: 所合成的嵌段共聚物具有温度和pH敏感性, 共聚物水溶液的低临界溶解温度(LCST)随HEMA量的增加而降低, 临界相变pH随HEMA量的增加而降低, 温度和pH诱导均可实现嵌段共聚物的胶束化. 控制HEMA量可以调控嵌段共聚物的LCST和pK_a.     

温敏性共聚物P(DMA-co-DAAM)的合成与热缔合行为研究

以N,N-二甲基丙烯酰胺(DMA)和双丙酮丙烯酰胺(DAAM)为共聚单体,在水溶液中采用常规自由基聚合以K_2S_2O_8-Na_2SO_3双氧化还原体系为引发剂,合成了一系列具有最低临界溶解温度(LCST)的温敏性聚合物P(DMA-co-DAAM).采用紫外可见分光光度计、动态光散射、芘荧光探针法和变温核磁共振氢谱等多种手段研究共聚物在不同温度下的溶液结构,结果表明共聚物P(DMA-co-DAAM)具有明显的热致缔合行为,在低温下聚合物以单链形式溶解,温度升高超过LCST之后由于P(DMA-co-DAAM)分子链上DAAM侧基发生亲水-疏水性变化,部分疏水链段缔合形成微相分离的胶束聚集体.进一步的研究还表明通过改变共聚物组成和溶液浓度能够有效调节共聚物溶液的缔合转变温度,共聚物P(DMA-co-DAAM)的LCST值与DAAM含量成很好的线性关系,DAAM含量越高LCST温度越低.采用常规自由基聚合所带来的链间异质性以及分子量的多分散性等特点并没有显著影响共聚物P(DMA-co-DAAM)的温敏性.     

P(MMA-co-MAh)-g-mPEG的合成及环境敏感性

采用偶合接枝法在甲基丙烯酸甲酯(MMA)和马来酸酐(MAh)无规共聚物上接枝不同含量的聚乙二醇单甲醚(mPEG), 合成具有pH敏感和温度敏感的两亲接枝共聚物P(MMA-co-MAh)-g-mPEG, 并对其进行了红外光谱和核磁共振波谱表征. 通过紫外-可见分光光度计测量了接枝共聚物水溶液的透光率, 结果表明, 接枝聚合物的水溶液呈现低临界溶解温度(LCST), 其LCST值对环境pH值和无机盐等因素敏感, 并可通过控制亲水侧链含量来调节.     

温度敏感性PNIPAM-b-PZLL-b-mPEG三嵌段共聚物的合成与自组装研究

通过大分子引发剂引发ε-苄氧羰基-L-赖氨酸-N-羧酸酐(Lys-NCA)开环聚合和大分子缩合的方法合成了聚(N-异丙基丙烯酰胺)-b-聚(ε-苄氧羰基-L-赖氨酸)-b-聚乙二醇单甲醚三嵌段共聚物(PNIPAM-b-PZLL-b-mPEG).用GPC和1H-NMR对其结构进行了表征.用芘荧光探针法证明了该三嵌段聚合物形成胶束的性质并测定了临界胶束浓度(CMC).动态光散射(DLS)研究表明,在固定PNIPAM-b-PZLL链段长度的情况下,mPEG分子量为2000时,胶束在温度高于临界溶解温度(LCST)时发生聚集,mPEG分子量为5000时,胶束在LCST以上没有发生聚集.     

含环糊精的温度敏感性聚合物的合成及自组装

合成了侧基含环糊精的聚异丙基丙烯酰胺(PnipamCD), 该聚合物在水溶液中具有较高的最低临界溶解温度(LCST). 快速升温到溶液的LCST以上可形成球形胶束, 慢速升温到LCST以上可形成空心囊泡. 在PNIPAM的选择性溶剂中, PnipamCD形成棒状组装体.     

温敏性含氟两亲接枝共聚物的制备及胶束化行为

以聚乙二醇单甲醚甲基丙烯酸酯(MPEGMA)为大分子单体, 甲基丙烯酸六氟丁酯(HFMA)为含氟单体, N-异丙基丙烯酰胺(NIPAAm)为功能性单体, 采用大分子单体接枝共聚法, 制备了一种温敏性含氟两亲接枝共聚物P(NIPAAm-co-HFMA)-g-PEG. 利用FTIR, ¹H NMR, ¹⁹F NMR和GPC对共聚物的结构进行表征; 采用紫外-可见分光光度计测定了共聚物的低临界溶解温度(LCST)约为38.9 ℃, 高于人体正常的生理温度; 利用荧光探针技术测定了共聚物的临界胶束浓度(cmc), 结果表明, 当共聚物溶液温度高于LCST时, 其cmc明显变小; 利用激光光散射粒度仪(LLS)测定了共聚物胶束的水合粒径及其分布, 当温度达到LCST时, 胶束粒径明显变小, 温度过高时, 粒径又有所增大; 利用透射电子显微镜(TEM)研究了共聚物胶束的形貌, 结果表明, P(NIPAAm-co-HFMA)-g-PEG在水溶液中可自组装成球状胶束粒子, 随着温度的升高, 共聚物胶束由松散的核壳结构转变成更加紧凑的球状结构, 且粒径明显变小.     

N-异丙基丙烯酰胺/丙烯酸胆甾醇酯共聚物研究

合成和表征了N 异丙基丙烯酰胺 (NIPAM)与丙烯酸胆甾醇酯 (CHA)的共聚物 .利用表面张力和荧光探针法研究了共聚物水溶液的表面活性性能 ,确定了其临界胶束浓度 (CMC) .利用浊度法和荧光探针法测定了共聚物的最低临界溶液温度 (LCST) .研究发现 ,在聚N 异丙基丙烯酰胺 (PNIPAM)分子链中引入疏水结构单元CHA会使其LCST下降 ;且随着共聚物中CHA含量的增加 ,LCST下降幅度增加 .在PNIPAM链段中引入少量的CHA就会使其表现出明显的两亲性 ,共聚物在水中能形成有壳核结构的稳定胶束 .通过将疏水化合物胆甾醇作为模拟药物包埋在胶束的疏水核中的研究 ,证实所得的胶束能包埋疏水药物 ,且随着包埋胆甾醇含量的增加 ,胶束平均粒径增大 .     

温敏性嵌段共聚物纳米胶束的制备及其稳定性

通过N-异丙基丙烯酰胺(NIPAAm)和N,N-二甲基丙烯酰胺(DMAAm)在链转移剂巯基乙醇存在下的自由基共聚,制备了具有端羟基的共聚物P(NIPAAm-co-DMAAm).利用其端羟基在异辛酸亚锡催化下引发己内酯开环聚合,得到了两亲性嵌段共聚物P(NIPAAm-co-DMAAm)-b-PCL,并在聚己内酯(PCL)链末端引入可光催化反应的不饱和双键.通过1H-NMR、GPC和相转变温度(LCST)等方法对聚合物进行了结构表征,测定了嵌段共聚物形成胶束的临界胶束浓度和胶束粒径,比较了核交联前后胶束的粒径和稳定性.结果表明:通过调节共聚物的组成,可获得LCST在40℃附近的胶束,胶束经核交联后,粒径有所减小,但稳定性明显提高,可用于对药物的温敏控制释放.     

梳状P(MMA-co-MAh)-g-PEGME共聚物的合成及结构与性能

用自制的甲基丙烯酸甲酯和马来酸酐的共聚物P(MMA-co-MAh)为反应物,聚乙二醇单甲醚(PEGME)为接枝单体,合成了梳状P(MMA-co-MAh)共聚物多缩乙二醇酯(P(MMA-co-MAh)-g-MPEG).采用傅立叶红外光谱(FTIR)、核磁共振(NMR)13C谱、1H谱以及H,C-COSP谱对所合成的梳状共聚物结构进行表征;热失重分析(TGA)和示差扫描量热法(DSC)对所合成的共聚物的物理性能进行了分析.FTIR及NMR结果表明,聚乙二醇单甲醚通过酯化反应接枝到P(MMA-co-MAh)共聚物上,形成以MMA/MAh共聚物为主链,聚乙二醇单甲醚为侧链的梳状共聚物,其在马来酸酐上的接枝率大约为20%;热性能分析结果表明,合成的梳状共聚物热分解温度与共聚物P(MMA-co-MAh)的分解温度相差不大,接枝后的梳状共聚物也具有高的热稳定性,起始热分解温度在325.9℃左右,且该梳状共聚物具有两个玻璃化转变温度,一个是由于侧链的玻璃化转变引起的,温度为32℃左右;一个是主链的玻璃化转变引起的,温度为120℃左右.在主链玻璃化转变温度以下,侧链是可以移动的,有利于电活性物质和离子等在聚合物基体中的扩散和迁移.     

Thermo and pH Dual-Responsive Micelles of N-phthaloylchitosan-g-Poly(N-isopropylacrylamide) and Poly(acrylic acid-co-tert-butyl acrylate) for Drug Delivery

A novel amphiphilic copolymer N-phthaloylchitosan graft poly(N-isopropylacrylamide) and poly(acrylic acid-co-tert-butyl acrylate) (PHCS-g-PNIPAAm&P(AA-co-tBA)) was synthesized. The graft copolymer could form micelles in aqueous medium, and the critical micelle concentration (CMC) of the copolymer was 7.5 × 10^{? 3}mg/mL. The lower critical solution temperature (LCST) of the micelles was measured to be 30°C. Transmission electron microscopy (TEM) image showed that the micelles exhibited a regular spherical shape, and the mean diameter of the micelles was 94.1 ± 0.8 nm as determined by dynamic light scattering (DLS). The potential usefulness of the micelles as drug delivery systems was investigated using anti-inflammation drug prednisone acetate as the model. The drug loading capacity of the micelles was measured to be 22.86 wt%, and the DLS results showed that the mean diameter of the drug-loaded micelles was 133.3 ± 2.4 nm. In vitro drug release studies indicated that the micelles exhibited thermo and pH dual-responsive release profiles.     

Physicochemical characterization of polymeric micelles constructed from novel amphiphilic polyphosphazene with poly(N-isopropylacrylamide) and ethyl 4-aminobenzoate as side groups

An amphiphilic graft polyphosphazene (PNIPAm/EAB-PPP) composed of oligo-poly(N-isopropylacrylamide) (PNIPAm) as hydrophilic segments and ethyl 4-aminobenzoate (EAB) as hydrophobic groups was synthesized via ring-opening polymerization and subsequent substitution reaction. The molar ratio of the PNIPAm segment to EAB group was 1.85:0.15. The lower critical solution temperature (LCST) of copolymer was 32.6 degrees C as determined by turbidity method. Micellization behavior of PNIPAm/EAB-PPP in an aqueous phase was characterized by fluorescence technique, 1H NMR, dynamic light scattering (DLS) and transmission electron microscopy (TEM). The critical micelle concentration (CMC) of the graft copolymer in aqueous solution was 0.1mg/ml. The number-averaged particle size of spherical micelles was 80 nm at 25 degrees C with a narrow distribution. TEM also revealed that inter-micellar aggregation was induced in the micelle solution at temperature above LCST of graft copolymer. The thermosensitive PNIPAm/EAB-PPP micelles may be of help to regulate the loading and release of hydrophobic drugs.     

P(DEAM-co-NAS)的合成及其温敏性的环境效应

采用自由基溶液聚合法合成聚(N,N-二乙基丙烯酰胺-co-N-丙烯酸琥珀酰亚胺)(P(DEAM-co-NAS))共聚比为7.9∶1、3.5∶1、2.5∶1、2∶1、1.5∶1的五组共聚物.利用傅里叶变换红外(FTIR)光谱和核磁共振(1HNMR)谱对P(DEAM-co-NAS)结构进行表征.共聚物组成和介质性质对P(DEAM-co-NAS)水溶液温敏性有显著影响.结果表明:随着NAS含量增加,共聚物水溶液的低临界溶解温度(LCST)逐渐升高,温敏性降低;盐的引入使P(DEAM-co-NAS)水溶液的LCST降低,所引入盐的阴离子价数越高,影响程度越大;有机酸的引入使P(DEAM-co-NAS)水溶液的LCST降低;NaOH、乙二胺、丁二胺的引入使P(DEAM-co-NAS)水溶液的LCST升高,二胺对P(DEAM-co-NAS)水溶液温敏性影响程度要大于NaOH.     

荧光探针法对N-异丙基丙烯酰胺-丙烯酰胺共聚物水溶液相变的研究

合成了多种不同配比的N 异丙基丙烯酰胺 (NIPAM )与丙烯酰胺 (AM )的共聚物 .用荧光探针法研究了共聚物溶液荧光光谱随温度升高而引起的变化 .研究表明 :共聚物的最低临界溶液温度 (LCST)取决于AM与NIPAM的组成比 .AM的比例越大 .LCST就越高 ,且有较好的正比关系 .通过以共价键连接于共聚物的荧光探针法 (标记法 )和以小分子探针混入共聚物水溶液的方法 (混入法 )测定上述体系LCST的结果比较 ,发现标记探针法具有较高的灵敏度 ,更适宜用来研究共聚物水相体系的相变问题 .     

全亲水无规共聚物P(NIPAM-co-AA)的pH和温度双重刺激响应性水相自组装

从N-异丙基丙烯酰胺(NIPAM)和丙烯酸(AA)单体合成了一种全亲水无规共聚物P(NIPAM-co-AA),实验发现该聚合物在水相中可以产生pH或温度双重刺激响应性自组装.采用透射电子显微镜(TEM)观察了自组装体的形貌,采用动态光散射(DLS)和静态光散射(SLS)观察了其粒径及粒径分布.测定了该聚合物水溶液的最低临界溶解温度(LCST)及其zeta电位随pH的变化,通过分析NIPAM和AA两种链节的质子化状态随温度和pH变化的趋势,阐释了其在水相中产生双重响应性自组装的推动力;并结合傅里叶红外(FT-IR)光谱测定自组装体表面富集基团的结果,进一步阐释了不同环境下自组装体的微结构.这类全亲水无规共聚物的合成方法简单,具有pH和温度双重响应性,其全水相中的刺激响应性自组装行为在药物释放等方面具有潜在的应用价值.     

全亲水无规共聚物P(NIPAM-co-AA)的pH和温度双重刺激响应性水相自组装

从N-异丙基丙烯酰胺（NIPAM）和丙烯酸（AA）单体合成了一种全亲水无规共聚物P（NIPAM-co-AA）,实验发现该聚合物在水相中可以产生pH或温度双重刺激响应性自组装. 采用透射电子显微镜（TEM）观察了自组装体的形貌,采用动态光散射（DLS）和静态光散射（SLS）观察了其粒径及粒径分布. 测定了该聚合物水溶液的最低临界溶解温度（LCST）及其zeta 电位随pH的变化,通过分析NIPAM和AA两种链节的质子化状态随温度和pH变化的趋势,阐释了其在水相中产生双重响应性自组装的推动力;并结合傅里叶红外（FT-IR）光谱测定自组装体表面富集基团的结果,进一步阐释了不同环境下自组装体的微结构. 这类全亲水无规共聚物的合成方法简单,具有pH和温度双重响应性,其全水相中的刺激响应性自组装行为在药物释放等方面具有潜在的应用价值.     

Synthesis and micelle formation of triblock copolymers of poly(methyl methacrylate)-b-poly(ethylene oxide)-b-poly(methyl methacrylate) in aqueous solution

Amphiphilic triblock copolymers of poly(methyl methacrylate)-b-poly(ethylene oxide)-b-poly(methyl methacrylate) (PMMA-b-PEO-b-PMMA) with well-defined structure were synthesized via atom transfer radical polymerization (ATRP) of methyl methacrylate (MMA) initiated by the PEO macroinitiator. The macroinitiator and triblock copolymer with different PMMA and/or PEO block lengths were characterized with ¹H and ¹³C NMR and gel permeation chromatography (GPC). The micelle formed by these triblock copolymers in aqueous solutions was detected by fluorescence excitation and emission spectra of pyrene probe. The critical micelle concentration (CMC) ranged from 0.0019 to 0.016 mg/mL and increased with increasing PMMA block length, while the PEO block length had less effect on the CMC. The partition constant K_v for pyrene in the micelle and in aqueous solution was about 10⁵. The triblock copolymer appeared to form the micelles with hydrophobic PMMA core and hydrophilic PEO loop chain corona. The hydrodynamic radius R_h,app of the micelle measured with dynamic light scattering (DLS) ranged from 17.3 to 24.0 nm and increased with increasing PEO block length to form thicker corona. The spherical shape of the micelle of the triblock copolymers was observed with an atomic force microscope (AFM). Increasing hydrophobic PMMA block length effectively promoted the micelle formation in aqueous solutions, but the micelles were stable even only with short PMMA blocks.     

Novel thermo‐responsive self‐assembly micelles from a double brush‐shaped PNIPAM‐g‐(PA‐b‐PEG‐b‐PA)‐g‐PNIPAM block copolymer with PNIPAM polymers as side chains

A novel double brush‐shaped copolymer with amphiphilic polyacrylate‐b‐poly(ethylene glycol)‐b‐poly acrylate copolymer (PA‐b‐PEG‐b‐PA) as a backbone and thermosensitive poly(N‐isopropylacrylamide) (PNIPAM) long side chains at both ends of the PEG was synthesized via an atom transfer radical polymerization (ATRP) route, and the structure was confirmed by FTIR, ¹H NMR, and SEC. The thermosensitive self‐assembly behavior was examined via UV‐vis, TEM, DLS, and surface tension measurements, etc. The self‐assembled micelles, with low critical solution temperatures (LCST) of 34–38 ^°C, form irregular fusiform and/or spherical morphologies with single, double, and petaling cores in aqueous solution at room temperature, while above the LCST the micelles took on more regular and smooth spherical shapes with diameter ranges from 45 to 100 nm. The micelle exhibits high stabilities even in simulated physiological media, with low critical micellization concentration (CMC) up to 5.50, 4.89, and 5.05 mg L^?1 in aqueous solution, pH 1.4 and 7.4 PBS solutions, respectively. The TEM and DLS determination reveled that the copolymer micelle had broad size distribution below its LCST while it produces narrow and homogeneous size above the LCST. The cytotoxicity was investigated by MTT assays to elucidate the application potential of the as‐prepared block polymer brushes as drug controlled release vehicles. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012