PU/PGMA同步互穿网络的力学性能

目的 研究影响高增塑聚氨酯 ( PU) /聚甲基丙烯酸缩水甘油酯 ( PGMA)同步互穿网络 ( SIN)力学性能的因素 ,寻求最佳力学性能配方 .方法 制备不同配方的样品 ,对其进行拉伸试验以及动态力学分析 .结果与结论 改变 PU与 PGMA的组成比 ,SIN的拉伸强度和延伸率呈非单调变化 ,在 PU含量为 60 %附近时出现极大值 .在体系中引入 PGMA组分的交联剂及引入网间接枝剂均使体系的交联密度上升 ,导致抗张强度升高 。

PU/PGMA同步互穿网络的固化反应动力学

目的 研究各种动力学因素对同步互穿网络 ( SIN)形成的影响 .方法 用傅里叶红外光谱法 ( FTIR)跟踪聚氨酯 ( PU)中 NCO基团及甲基丙烯酸缩水甘油酯 ( GMA)中C C基团特征吸收峰的变化 ,分别得到其转化率与时间曲线 .结果与结论 研究了互穿网络中各组分与纯组分反应情况的差异 ;SIN中 PU和 PGMA反应均为二级动力学反应 ,其反应活化能分别为 2 8.1和 3 5 .6k J/ mol;当改变 PU催化剂时 ,根据红外跟踪得到转化率曲线 。

PGMA预浸润石英纤维增强PMMA基托树脂的抗折性能和界面结合性能

目的:探索一种新型增强材料聚甲基丙烯酸甘油酯(polyglycidyl methacrylate,PGMA)预浸润石英纤维网的界面结合性能和机械性能。方法:采用"三明治"埋入法制作PGMA预浸润石英纤维网(1层、2层、3层)、电解钴铬合金网、"喷砂+表面处理剂"预处理钴铬合金网增强的基托树脂标准实验模块,大小为40 mm×15 mm×2 mm,采用三点弯曲实验和扫描电镜对其抗折裂性能和界面结合性能进行研究。结果:3层PGMA预浸润石英纤维网增强基托树脂表现出最大的弹性模量(6 406 MPa)和弯曲强度(227 MPa),1层和2层PGMA预浸润石英纤维网增强效果并不明显。钴铬合金网具有增强效果,表面改性后增强效果更加明显。表面预处理钴铬合金网和PGMA预浸润石英纤维网与聚甲基丙烯酸甲酯(polymethyl methacrylate,PMMA)具有更好的界面结合性能。结论:PGMA预浸润石英纤维增强材料可以改进与PMMA的界面结合性能,并随着纤维层数的增多,其机械性能得到更大的改善。

表面引发AGET ATRP原位聚合法制备Fe_3O_4/PGMA复合纳米粒子

以多元醇还原法制备亲水性超顺磁四氧化三铁（Fe3O4）纳米粒子,并利用表面引发电子活化再生原子转移自由基聚合（SI-AGET ATRP）法,制备了Fe3O4/聚甲基丙烯酸缩水甘油酯（Fe3O4/PGMA）磁性复合纳米粒子。研究了原位聚合过程中还原剂异辛酸亚锡（Sn（EH）2）用量对PGMA接枝量和复合纳米粒子磁性能的影响。结果表明：Sn（EH）2在0.005-0.03 mmol时,聚合物接枝量随着Sn（EH）2用量的增大而增加;当Sn（EH）2用量大于0.15 mmol时,PGMA接枝量先增大后减少。磁性能研究表明,复合纳米粒子在室温下具有超顺磁特性,其饱和磁化强度从改性前的Ms=73 emu·g^-1降低到Ms=1 emu·g^-1。

不同蛋白A亲和色谱填料的制备工艺比较及性能评价

蛋白A亲和色谱填料由于能够和免疫球蛋白G(IgG)特异性作用,已广泛应用于临床医学、生物医药领域。采用不同结构和形貌的基质,通过不同的表面修饰方法得到的填料性能差别很大。研究分别以常用的琼脂糖和聚甲基丙烯酸缩水甘油酯(PGMA)小球为基质,通过多功能环氧基定向固定蛋白A制得琼脂糖基质亲和色谱填料(A-S)和PGMA基质亲和色谱填料(P-S)。通过马来酰亚氨基定向固定蛋白A制得琼脂糖基质亲和色谱填料(A-R)和PGMA基质亲和色谱填料(P-R)。通过对蛋白A的键合工艺加以优化,研究了基质种类、基质粒径以及蛋白A含量等条件对材料性能的影响,提高了材料对IgG的吸附性能。结果表明,尽管所制备的4类材料对IgG都有一定的吸附选择性,但P-R的性能明显更加优异,可在较低的蛋白A配基密度下达到较高的动态载量。制备了不同配基密度的亲和色谱填料,其中配基密度为15.71 mg/mL的P-R对牛免疫球蛋白的动态载量为32.23 mg/mL,对人免疫球蛋白的动态载量达到54.41 mg/mL,且在碱处理160个循环后动态载量仍为初始值的94.6%。耐压测试结果表明P-R的机械强度远高于同等条件下制得的琼脂糖基质的亲和材料A-R,当流速到达80 mL/min时,PGMA基质色谱柱的流速与压力仍保持较好的线性关系,P-R的耐压性能好,可以在更高的流速下进行分离纯化。以上结果说明以马来酰亚氨基在PGMA上固定蛋白A的工艺更适宜于蛋白A亲和色谱填料的工程化生产,所发展的方法有望在固定蛋白和免疫吸附材料合成领域发挥更大的作用。

聚甲基丙烯酸缩水甘油酯为主链的咪唑型螯合树脂的合成、表征及吸附性能研究

用分散聚合法合成了聚甲基丙烯酸缩水甘油酯(PGMA),然后引入咪唑功能基合成了螯合树脂(PGMA-Imi),用傅立叶变换红外光谱(FTIR)与扫描电镜(SEM)研究了其结构与粒子表面形态,元素分析测定功能基含量,并对Cu2+等离子进行了吸附研究。结果表明所得PGMA微球为微米级、单分散性很好,所得螯合树脂(PGMA-Imi)对Cu2+的吸附效果最好。

侧基键合有锌酞菁的聚甲基丙烯酸缩水甘油酯的制备及其光谱性质

首先通过开环反应,将2,9,16,23-四氨基取代的锌酞菁(ZnTAPc)键合在聚甲基丙烯酸缩水甘油酯(PGMA)的侧基上,制得键合有氨基锌酞菁(ZnAPc)的聚合物ZnAPc-PGMA。然后使ZnAPc-PGMA侧基上的氨基与对二甲氨基苯甲醛(DMAB)发生席夫碱反应,制得侧基含芳环席夫碱基团的锌酞菁(ZnABPc)的聚合物ZnABPc-PGMA。通过测定氨基锌酞菁在PGMA上的键合度,重点研究了反应时间、温度和催化剂种类对ZnTAPc在PGMA上键合过程的影响。测定了ZnAPc-PGMA和ZnABPc-PGMA的紫外-可见吸收光谱及荧光发射光谱,考察了其光物理学行为。结果表明,所制备的ZnAPc-PGMA和ZnABPc-PGMA均具有ZnTAPc的特征电子吸收光谱与荧光发射光谱,同时也显示出锌酞菁键合到聚合物上的特征。ZnTAPc键合到PGMA上后,有效地减弱了其聚集性。此外,随着ZnAPc在PGMA上键合度的增大,荧光吸收光谱强度增强。同时,ZnAPc-PGMA的荧光光谱还显现了一定的高分子效应,随着ZnAPc-PGMA中ZnAPc键合度的增大,ZnAPc侧链单元间会发生能量转移,使荧光发射强度减弱。

Preparation and Characterization of Non-porous Superparamagnetic Microspheres with Epoxy Groups by Dispersion Polymerization

Non-porous superparamagnetic polymer microspheres with epoxy groups were prepared by dispersion polymerization of glycidyl methacrylate (GMA) in the presence of magnetic iron oxide (Fe3O4) nanoparticles coated with oleic acid. The polymerization was carried out in the ethanol/water medium using polyvinylpyrrolidone (PVP) and 2,2’-azobisisobutyronitrile (AIBN) as stabilizer and initiator, respectively. The magnetic microspheres obtained were characterized with scanning electron microscopy (SEM), vibrating sample magnetometry (VSM) and Fourier transform infrared spectroscopy (FTIR). The results showed that the magnetic microspheres had an average size of-1μm with superparamagnetic characteristics. The saturation magnetization was found to be 4.5emu.g-1. There was abundance of epoxy groups with density of 0.028 mmol·g^-1 in microspheres. The magnetic PGMA microspheres have extensive potential uses in magnetic bioseparation and biotechnology.

Synthesis and characterization of monosize magnetic poly(glycidyl methacrylate) beads

Monosize, 1.6 μm, magnetic beads of poly（glycidyl methacrylate） [M-poly（GMA）], were prepared by dispersion polymerization in the presence of Fe3O4 nano-powder. Monosize M-poly（GMA） beads were characterized by swelling tests, density measurements, electron spin resonance （ESR）, vibrating sample magnetometer （VSM） and scanning electron microscopy （SEM）. The characteristic functional groups of M-poly（GMA） beads were analyzed by Fourier transform infrared spectrometer （FTIR）. The M-poly（GMA） beads are highly uniform in size and have a spherical shape and non-porous structure. Polydispersity index （PDI） of M-poly（GMA） beads was calculated to be around 1.008. The hydrated density of the M-poly（GMA） beads measured at 25 ℃ was 1.14 g/cm^3. The content of oxirane groups on the surface of the M-poly（GMA） sample was found to be 3.46 mmol/g by using perchloric acid titration. The specific surface area of the M-poly（GMA） beads was determined to be 3.2 m^2/g. The equilibrium swelling ratio was 52%. The volume fraction of magnetite nanopowder in the M-poly（GMA） beads was found to be 4.5%. The g factor, that can be considered as a quantity characteristic of the molecules in which the unpaired electrons are located, was found to be 2.28 for M-poly（GMA）. The external magnetic field at resonance was calculated to be 2055 Gs which was found sufficient to excite all of the dipole moments present in 1.0 g of M-poly（GMA） sample.

SiO2同步合成与固载酞菁的制备及可见光催化性能

首先通过对羟基苯甲酸和8-羟基喹啉分别与4-硝基邻苯二腈反应制备了羧基苯氧基邻苯二腈(CPPN)和喹啉氧基邻苯二腈(QPN),然后利用开环反应将CPPN键合到聚甲基丙烯酸缩水甘油酯改性的硅胶(PGMA/SiO2)表面,得到键合有邻苯二腈的硅胶CPPN-PGMA/SiO2,再通过“同步合成与固载”的方法在PGMA/SiO2表面固载喹啉氧酞菁(QPc)或金属喹啉氧酞菁(MQPc),制备了固载化的酞菁QPc-PGMA/SiO2或CoQPc-PGMA/SiO2。通过红外光谱、扫描电镜、热重分析、紫外-可见漫反射光谱等对其结构、形貌和酞菁键合量进行表征和测定。考察了催化剂DBU用量对“同步合成与固载”酞菁过程的影响。最后以亚甲基蓝(MB)和苯酚为目标降解物,研究所制得的固载化酞菁催化剂QPc-PGMA/SiO2或CoQPc-PGMA/SiO2的可见光催化活性。结果表明,借助“同步合成与固载”的方法能够成功在PGMA/SiO2表面固载喹啉氧酞菁(QPc)或金属喹啉氧酞菁(CoQPc),得到固载化酞菁QPc-PGMA/SiO2或CoQPc-PGMA/SiO2。在可见光照射下,QPc-PGMA/SiO2和CoQPc-PGMA/SiO2均具有较好的光催化活性。较低浓度时,CoQPc-PGMA/SiO2催化降解亚甲基蓝的效果优于QPc-PGMA/SiO2;碱性条件有利于CoQPc-PGMA/SiO2光催化降解MB性能的发挥,在pH值为10.0时,0.2g/L的CoQPc-PGMA/SiO2能使MB的降解率高达97%以上。固载化金属酞菁周边取代基的性质对其光催化降解苯酚有一定的影响,有供电子共轭效应的CoQPc-PGMA/SiO2对苯酚的光降解效果最优,5min内苯酚的降解率达58%,2h内苯酚的降解率高达100%。此外,固载化金属酞菁还具有良好的重复使用性。

β-(N,N-二甲胺基乙氧基)酞菁锌在硅胶表面的固载及其光催化活性

通过4-硝基邻苯二腈分别与对羟基苯甲酸和N,N-二甲基乙醇胺反应制备了4-(4-羧基苯氧基)邻苯二腈(CPPN)和4-(N,N-二甲胺基乙氧基)邻苯二腈(ePN),然后利用开环反应将CPPN键合到聚甲基丙烯酸缩水甘油酯改性的硅胶(PGMA/SiO2)表面,得到键合有邻苯二腈的硅胶CPPN-PGMA/SiO2。在“分子碎片”ePN和催化剂1,8-二氮杂双环[5.4.0]十一碳-7-烯(DBU)作用下,通过“同步合成与固载”的方法在PGMA/SiO2表面固载金属酞菁(β-(N,N-二甲胺基乙氧基)酞菁锌,ePcZn)或无金属酞菁(ePc),从而制备了固载化的酞菁ePcZn-PGMA/SiO2或ePc-PGMA/SiO2。通过FT-IR、紫外-可见光谱、TG等对其结构和酞菁键合量进行表征和测定。考察了DBU的用量对“同步合成与固载”酞菁过程的影响。以亚甲基蓝(MB)为目标降解物,研究所制得的固载化酞菁催化剂ePc-PGMA/SiO2或ePcZn-PGMA/SiO2的可见光催化活性。结果表明,借助“同步合成与固载”的方法能够成功在PGMA/SiO2表面固载ePc或ePcZn,得到固载化酞菁光催化剂ePc-PGMA/SiO2或ePcZn-PGMA/SiO2,它们均具有较好的可见光催化活性。在可见光照射下,ePcZn-PGMA/SiO2和ePc-PGMA/SiO2在较低的质量浓度下凭借吸附-光催化耦合协同作用均能有效降解MB,且随催化剂用量的增大,MB的降解率增大,0.03 g的ePcZn-PGMA/SiO2能使MB的降解率高达92%。催化剂重复使用5次后仍具有较好的光催化稳定性。

Facile synthesis of wormlike quantum dots-encapsulated nanoparticles and their controlled surface functionalization for effective bioapplications

Semiconductor quantum dots (QDs) are considered as ideal fluorescent probes owing to their intrinsic optical properties. It has been demonstrated that the size and shape of nanoparticles significantly influence their behaviors in biological systems. In particular, one-dimensional (1D) nanoparticles with larger aspect ratios are desirable for cellular uptake. Here, we explore a facile and green method to prepare novel 1D wormlike QDs@SiO2nanoparticles with controlled aspect ratios, wherein multiple QDs are arranged in the centerline of the nanoparticles. Then, an excellent cationic gene carrier, ethanolamine-functionalized poly(glycidyl methacrylate) (denoted by BUCT-PGEA), was in-situ produced via atom transfer radical polymerization on the surface of the QDs@SiO2nanoparticles to achieve stable surfaces (QDs@SiO2-PGEA) for effective bioapplications. We found that the wormlike QDs@SiO2-PGEA nanoparticles demonstrated much higher gene transfection performance than ordinary spherical counterparts. In addition, the wormlike nanoparticles with larger aspect ratio performed better than those with smaller ratio. Furthermore, the gene delivery processes including cell entry and plasmid DNA (pDNA) escape and transport were also tracked in real time by the QDs@SiO2-PGEA/pDNA complexes. This work realized the integration of efficient gene delivery and real-time imaging within one controlled 1D nanostructure. These constructs will likely provide useful information regarding the interaction of nanoparticles with biological systems. [Figure not available: see fulltext.] © 2016, Tsinghua University Press and Springer-Verlag Berlin Heidelberg.