不饱和端基超支化聚合物/丙烯酸酯共聚乳液的研究

利用Si—H加成反应制得了以CC为端基的超支化含硅聚合物,并将其与丙烯酸酯类单体进行乳液共聚,对聚合反应机理及所得聚合物的性能进行了测试分析.结果表明,含有大量CC端基的超支化含硅聚合物能与丙烯酸酯类单体稳定聚合,制得了平均粒径小于100nm高度交联的乳胶粒子.共聚物的红外光谱证实,超支化聚合物的不饱和端基已全部反应,形成了以超支化聚合物为多臂交联点的交联型乳胶粒子.随聚合体系中超支化聚合物用量的增加,乳液聚合反应速率增大,乳胶粒粒径减小,共聚物热稳定性显著提高.     

通过A2+B3反应制备超支化聚芳醚酮荧光材料

用3-二甲氨基苯酚与超支化聚芳醚酮(HPETFDEK-F)的末端氟发生反应,制得荧光超支化聚芳醚酮(FHPETFDEK).采用1HNMR,FTIR,DSC和TGA等方法对所得到的聚合物结构和热性能进行了表征.研究了FHPETFDEK的紫外吸收及荧光发射光谱,发现其具有荧光行为.     

基于炔类单体的点击聚合制备超支化聚合物

超支化聚合物由于其独特的树枝状结构和物理化学性质,已经得到了广泛关注及应用.而基于炔类单体的点击聚合作为一类简单、高效的聚合反应已被广泛用于超支化聚合物的制备.本文对近5年利用叠氮-炔和巯基-炔点击聚合制备超支化聚合物的工作进行了简要综述.其中,Cu(I)催化的叠氮-炔点击聚合可制备1?4-立构规整的超支化聚三唑;Ru(II)催化的叠氮-炔点击聚合可制备1?5-立构规整的超支化聚三唑;活化的炔类单体和叠氮单体的无金属催化点击聚合可得到1?4-异构体含量高(高达91.7%)的超支化聚合物;而光引发?热引发及自发的巯基-炔点击聚合可制备含硫的超支化聚合物.此外,对所制备的超支化聚合物的功能和应用进行了简单介绍,最后还简单讨论了点击聚合制备超支化聚合物方面的可能发展方向.     

含香豆素基团超支化星形聚合物的合成与表征

设计并合成了含有香豆素基团的自引发单体, 与2-(2-甲氧基乙氧基)乙基甲基丙烯酸酯(MEO₂MA)进行自缩合乙烯基共聚合后得到超支化聚合物H-PMEO₂MA. 以其作为大分子引发剂, 进行二甲氨基乙基甲基丙烯酸酯(DMAEMA)的原子转移自由基聚合, 合成了具有温度响应性的超支化星形聚合物H-PMEO₂MA-star-PDMAEMA. 将此超支化星形聚合物在水中自组装成胶束后, 利用支化点处香豆素基团的光二聚性能, 在λ=320 nm的紫外光照射下进行香豆素间的光交联反应, 形成核交联胶束. 此核交联胶束在254 nm紫外光照射下则会发生解交联反应. 采用尼罗红作为模型药物, 将其装载到超支化星形聚合物胶束中, 研究了不同条件下的药物释放行为.     

新型含磷和氟聚芳醚的制备、表征及性能

通过分子设计, 成功合成了一种含有三苯基膦结构的二氟单体--4,4’-二氟二苯苯磷氧(BFPPO). 在碱催化条件下, BFPPO与2-双-(4-羟苯基)六氟丙烷(六氟双酚A)缩聚得到一种新型含三苯基膦结构的聚芳醚材料(6F-PAEPO). 使用FTIR,1H NMR, 31P NMR, 和16F NMR等表征手段确定了聚合物的结构, 聚合物表现出良好的热稳定性、有机可溶性、机械性能和光透过性能, 其中聚合物的玻璃化转变温度高达211℃, 空气气氛和氮气气氛下5%热失重温度分别为512℃和523℃, 聚合物薄膜的最大光透过率超过80%. 尤其, 聚合物由于主链中三苯基磷氧结构的存在, 表现出了优异的阻燃性能, 有限氧指数(LOI)达到39.9%.     

超支化梯形共轭聚合物的合成与表征

采用"A2+B2+B3"方法,通过Pd(0)催化的Suzuki聚合反应制备了一系列的超支化梯形共轭聚合物.所制备的聚合物荧光发射均在蓝光发射区.随着支化度的增加,聚合物的荧光发射和紫外吸收均有蓝移的趋势.超支化结构在一定程度上抑制分子间的聚集,使得聚合物在薄膜中的发射和吸收相对于溶液中的发射和吸收红移比较小.所制备的聚合物都表现出了良好的热稳定性,热分解温度都在320℃以上,DSC二次加热曲线在35～300℃之间没有玻璃化转变和其它的热力学过程.超支化共轭聚合物有望成为一种良好的蓝光材料.     

端基结构对超支化聚合物静电吸附自组装行为的影响

研究了3种具有相同骨架结构、不同端基的超支化聚合物与线型聚阳离子(PDAC)的静电吸附自组装.结果表明,超支化聚合物的组装过程与线型弱酸聚合物相似,都受溶液pH值与无机盐浓度的影响,但影响程度随端基结构不同而变化.此外,对以超支化聚合物为最外层的不同自组装膜的表面形貌及接触角进行了表征,其表面形貌及亲水性随端基结构的不同而不同.     

两亲性全季铵盐超支化聚合物的设计与合成及主-客体超分子着色应用研究

采用高效的巯基-炔点击化学与Menschutkin季铵化反应,合成了一种带有1个叠氮基、2个炔基和2个季铵盐基团的AB2型季铵盐单体,通过核磁共振、红外光谱、质谱等方法对单体结构进行了确认.将所得单体进行点击聚合,得到全季铵盐超支化聚合物,并用端叠氮基的长链烷烃封端,得到核亲水-壳憎水的两亲性超支化聚季铵盐.研究所得两亲性超支化聚合物对染料的装载性能,结果表明所合成的带正电荷两亲性聚合物对多种带负电荷的水性染料装载效果好,平均相转移率高达95%.进一步将装载染料的主-客体超分子复合物用于聚合物制品着色,发现其对SBS及PMMA等聚合物有很好的着色效果,着色均匀且不掉色,着色的膜色泽鲜艳透明.     

两亲性超支化聚合物的研究进展

两亲性超支化聚合物作为一种新型功能性材料.近年来引起了人们的广泛关注.两亲性超支化聚合物的合成丰要是利用不同亲水性的链段对超支化聚合物端基进行改性,或者首先在超支化聚合物末端产生活性位点,再利用超支化分f作为大分子引发剂引发烯类单体进行斤环聚合、原子转移自由基聚合等得到以超支化聚合物为核的两亲性超支化共聚物;这些分子由...     

新型超支化聚芳烃的合成与性能研究

3,6-二乙炔基-9-(三苯胺基)-咔唑、4,4′-二乙炔基-4″-(咔唑基)-三苯胺双炔和1-辛炔单炔在CpCo(CO)2-hν催化的条件下合成了新型超支化聚芳烃.所得的聚合物都溶于普通溶剂(甲苯、THF、氯仿、二氯甲烷等).在光激发的条件下,聚合物在428 nm左右发射蓝光,其荧光量子效率达到62%.所有超支化聚合物都表现出优异的热稳定性,它们的起始分解温度高达484℃.     

由聚丙二醇二缩水甘油醚和甘油制备温敏性超支化聚合物

由聚丙二醇二缩水甘油醚和甘油通过质子转移聚合(proton transfer polymerization)一步法制备了端羟基的温敏性超支化聚醚.聚合产物的分子量(Mn)在1.76×104~2.43×104之间,玻璃化转变温度(Tg)在-31.5~-26.7℃之间,热分解温度(Td)在367~376℃之间.通过控制聚丙二醇二缩水甘油醚和甘油的投料比,实现了对温敏性超支化聚醚最低临界溶解温度(LCST)的调节,LCST可控制在28.3~39.6℃之间.     

多重响应性超支化星形聚合物的合成与组装以及控制释放研究

含二硫键的自引发单体与2-(2-甲氧基乙氧基)乙基甲基丙烯酸酯(MEO₂MA)进行自缩合乙烯基共聚合得到超支化PMEO₂MA(H-PMEO₂MA). 以它作大分子引发剂, 引发二甲氨基乙基甲基丙烯酸酯(DMAEMA)进行原子转移自由基聚合, 合成了具有温度、pH以及氧化还原多重响应性的超支化星形聚合物H-PMEO₂MA-star-PDMAEMA. 证明了H-PMEO₂MA有低临界溶液温度(LCST); 研究了PDMAEMA 链段的长度和溶液的pH值对超支化星形聚合物的LCST的影响. 当H-PMEO₂MA-star-PDMAEMA水溶液温度从2 ℃升高至室温, H-PMEO₂MA变成疏水性而发生聚集, 形成以H-PMEO₂MA为核, PDMAEMA为壳的胶束. 在胶束形成过程中, 将尼罗红装载到这种聚合物胶束中, 形成释药系统, 研究了pH、氧化还原响应性释药性能.     

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.     

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.     

Synthesis and supramolecular self‐assembly of thermosensitive amphiphilic star copolymers based on a hyperbranched polyether core

A novel amphiphilic thermosensitive star copolymer with a hydrophobic hyperbranched poly (3‐ethyl‐3‐(hydroxymethyl)oxetane) (HBPO) core and many hydrophilic poly(2‐(dimethylamino) ethyl methacrylate) (PDMAEMA) arms was synthesized and used as the precursor for the aqueous solution self‐assembly. All the copolymers directly aggregated into core–shell unimolecular micelles (around 10 nm) and size‐controllable large multimolecular micelles (around 100 nm) in water at room temperature, according to pyrene probe fluorescence spectrometry and ¹H NMR, TEM, and DLS measurements. The star copolymers also underwent sharp, thermosensitive phase transitions at a lower critical solution temperature (LCST), which were proved to be originated from the secondary aggregation of the large micelles driven by increasing hydrophobic interaction due to the dehydration of PDMAEMA shells on heating. A quantitative variable temperature NMR analysis method was designed by using potassium hydrogen phthalate as an external standard and displayed great potential to evaluate the LCST transition at the molecular level. The drug loading and temperature‐dependent release properties of HBPO‐star‐PDMAEMA micelles were also investigated by using indomethacin as a model drug. The indomethacin‐loaded micelles displayed a rapid drug release at a temperature around LCST. © 2007 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 46: 668–681, 2008     

Temperature‐responsive “tadpole‐shaped” protein–polymer hybrids and their self‐assembly behavior

The temperature‐responsive poly (N, N‐diethylacrylamide) (pDEAAm) with narrower molecular weight distribution was prepared by the atom transfer radical polymerization and characterized by ¹HNMR and gel permeation chromatography. The temperature‐responsive “tadpole‐shaped” BSA–pDEAAm hybrids were fabricated via a free Cys‐34 residue of bovine serum albumin (BSA) site specifically binding to the end group disulfide bonds of pDEAAm and characterized by native‐polyacrylamide gel electrophoresis (Native‐PAGE) and matrix‐assisted laser desorption/ionization time of flight mass spectrometry. Their temperature‐responsive behaviors were measured by ultraviolet‐visible spectra (UV‐Vis). The lower critical solution temperature (LCST) of the pDEAAm was identified as 28°C, and the LCST of BSA–pDEAAm hybrids was identified as 31°C. The morphologies of BSA–pDEAAm hybrids self‐assembled in the aqueous solutions with two different temperatures at 25 °C and 40°C were investigated by transmission electron microscopy. Below the LCST of BSA–pDEAAm hybrids, the separate spherical nanoparticles were observed. In contrast, bundles and clusters were observed above the LCST of BSA–pDEAAm hybrids. The results suggested that the self‐assembly morphology of BSA–pDEAAm hybrids depended upon the pDEAAm block in BSA–pDEAAm hybrids, and the morphology transitions were effected by the LCST of BSA–pDEAAm hybrids. It would be expected to be used in biomedicine and materials science. Copyright © 2016 John Wiley & Sons, Ltd.     

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.     

Phase transition behavior of unimolecular micelles with thermoresponsive poly(N-isopropylacrylamide) coronas

This paper describes the double phase transition behavior of a thermoresponsive poly(N-isopropylacrylamide) (PNIPAM) brush at the surface of a hydrophobic core. Reversible addition-fragmentation transfer (RAFT) polymerization of N-isopropylacrylamide (NIPAM) was conducted by using a hyperbranched polyester (Boltorn H40) based macroRAFT agent. The resultant multiarm star block copolymer (H40-PNIPAM) exists as unimolecular micelles with hydrophobic H40 as the core, densely grafted PNIPAM brush as the shell. A combination of laser light scattering (LLS) and microdifferential scanning calorimetry (micro-DSC) studies of H40-PNIPAM in aqueous solution reveals double phase transitions of the PNIPAM corona, which is in contrast to the fact that free PNIPAM homopolymer in aqueous solution exhibits a lower critical solution temperature (LCST) at approximately 32 degrees C. The first phase transition takes place in the broad temperature range 20-30 degrees C, which can be tentatively ascribed to the n-cluster-induced collapse of the inner region of the PNIPAM brush close to the H40 core; the second phase transition occurs above 30 degrees C, which can be ascribed to the outer region of PNIPAM brush. Employing the RAFT chain extension technique, the inner and outer part of PNIPAM brush were then selectively labeled with pyrene derivatives, respectively; temperature-dependent excimer fluorescence measurements further support the conclusion that the inner part of PNIPAM brush collapses first at lower temperatures, followed by the collapse of the outer part at higher temperatures.     

Phase Transition and Micellization of Temperature Responsive Dextran—graft—poly（N—isopropylacrylamide）Polymers

Phase behavior and micellization of dextran-graft-poly(N-isopropylacrylamide)(PNIPAAm)polymers in aqueous solution are investigated in this paper using DSC and AFM methods.It is found that with the increase of grafting(G%) of the copolymers the endothermic enthalpy during the phase transition increases significantly and the transition temperature decreases slightly.The phase transition behavior of the copolymers is scanning rate dependent.Micelles are formed whenever the solution temperature is raised above the LCST of the copolymers.It is proposed that by using this thermal responsive property of the copolymers,drugs could be incorporated into the micelles without employing any organic solvent.     

Controlled aggregation behavior of thermoresponsive polymeric micelles by introducing hydrophilic segments as corona components

Poly[N‐isopropylacrylamide‐co‐N‐(3‐methoxypropyl)acrylamide]‐b‐poly(D,L‐lactide) (P(IPAAm‐co‐MPAAm)‐b‐PLA) as a thermoresponsive block copolymer and PMPAAm‐b‐PLA as a nonthermoresponsive block copolymer were co‐assembled into thermoresponsive polymeric micelles in water. In addition, PMPAAm‐b‐P(IPAAm‐co‐MPAAm)‐b‐PLA triblock copolymer was assembled to form thermoresponsive micelles with a hydrophilic layer on the outermost surface of the thermoresponsive corona. Using both micelles, we investigated the effects of introducing hydrophilic polymer segments on micellar aggregation behavior at temperatures above the lower critical solution temperature (LCST) of the thermoresponsive micelles. Despite the external hydrophilic PMPAAm layer on PMPAAm‐b‐P(IPAAm‐co‐MPAAm)‐b‐PLA micelles, aggregation following dehydration of the thermoresponsive segments was not significantly suppressed at temperatures above the LCST due to the instability of the core‐corona state. In contrast, intermicellar aggregation was successfully controlled by blending P(IPAAm‐co‐MPAAm) and PMPAAm in the thermoresponsive corona region, even above the LCST. In particular, PMPAAm chains longer than the P(IPAAm‐co‐MPAAm) chains could regulate the hydrodynamic diameter of micellar aggregates at temperatures above the LCST. The micelles showed enhanced drug release rates in response to temperature changes above the LCST without precipitating from solution. These results indicated that a side‐by‐side structure of hydrophilic/thermoresponsive chains in the corona region could effectively control the micellar aggregation state after a thermal phase transition. © 2018 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2018 , 56, 1695–1704