三聚氰胺-甲醛树脂包裹环氧树脂微胶囊的制备及表征

针对环氧树脂基材料的自修复,选取四氢邻苯二甲酸二缩水甘油酯作为芯材,采用三聚氰胺-甲醛树脂为壁材,对其进行微胶囊化包裹.结果表明,制得的具有单囊结构的环氧树脂微胶囊,胶囊粒径较小(约6.7μm)、囊壁较薄(约0.2μm)、芯含量较高(83.2 wt%),囊壁内、外表面光滑致密,胶囊具有良好的密闭性和耐热性;在微胶囊化过程中,三聚氰胺-甲醛树脂的缩聚反应动力学起关键作用,芯材没有参与囊壁形成的交联反应;包裹后的芯材活性保持不变,胶囊被复合到材料过程中囊芯活性也保持不变;胶囊的强度较高,能承受与基体材料复合过程中的外力作用,且与基体材料间粘结良好,在裂纹形成过程中能够随基体同时开裂.     

共缩聚聚酰胺胶囊的制备及其性质的研究

界面缩聚法是制备微胶囊的常用办法之一,在医药、农药、生物工程等各个领域得到了广泛的研究与应用.此法制备聚酰胺胶囊具有制备方法简单、缩聚速度快、囊壁孔隙大等优点.在制备胶囊时,一般以一种二元胺或多元胺作为水溶性单体,制备的微胶囊存在很大的缺陷.当用二元胺作为水溶性单体时,得到具有线型结构的聚酰胺胶囊,囊壁的机械强度差.采用多元胺作为水溶性单体时,反应深度小,制备的胶囊囊壁薄、孔隙小.我们采用二元胺和多元胺的混合物作为水溶性单体,得到了不规则缩聚的共缩聚胶囊.改变二元胺与多元胺的比例,改善囊壁的机械强度和对KCl 的渗透系数,从而制备出具有较高机械强度和较大渗透系数的胶囊,以适应实际应用中对芯材控制释放的要求.     

芯材结构及组成对天然香料液体纳米胶囊形成能力的影响

本文以壳聚糖为壁材、CO-40/Span-80/1,2-丙二醇为乳化体系,考察不同芯材结构及组成对液体纳米胶囊形成能力的影响.本文所选用的芯材为乙酸芳樟酯、柠檬香茅醛、芳樟醇、香叶醇、香茅醇和苎烯等芳香小分子,以及薰衣草香料、柠檬香料及香茅香料3种天然香料.首先,以这些芳香小分子作为芯材制备纳米胶囊并绘制相关伪三元相图,考察芳香小分子结构对液体纳米胶囊形成能力的影响.其次,将这些芳香小分子按照不同的比例进行复配用作芯材制备液体纳微胶囊,并与以天然香料为芯材所制得的液体纳米胶囊性能进行对比,归纳出制备小粒径、窄分布且透明的天然香料液体纳米胶囊的一般规律.结果表明,芯材的亲水部分结构中含有以下官能团时,它们形成透明液体纳米胶囊的能力依次为:酯基羰基羟基,且芯材疏水部分体积越大形成透明液体纳米胶囊的能力越小;复合组分用作芯材时,其组分比例与天然香料组成比例相近时,所获得液体纳米胶囊性能相似;复合组分中含量最高的组分决定了其最终液体纳米胶囊的性质.     

聚[2-(甲基丙烯酰氧)乙基三甲基氯化铵]/阿拉伯胶复凝聚法十二醇微胶囊的制备

将聚[2-(甲基丙烯酰氧)乙基三甲基氯化铵](PMTC)和阿拉伯胶(GA)在一定条件下进行了复凝聚,并对影响复凝聚实验的壁材配比、壁材浓度、离子强度等因素进行了考察.实验结果表明,PMTC与GA配比为1/3.22,壁材总浓度为4%时复凝聚效率最高;体系中不同浓度的氯化钠的存在会对复凝聚起到不同程度的抑制作用.在实验确定的最佳复凝聚条件下以有机小分子化合物十二醇作为芯材进行了包覆,制备了不同壁芯比例的微胶囊.对微胶囊的包覆率及载药量进行了测量,并对它们的释放行为进行了考察.包覆有十二醇的复合微胶囊大小一般在几微米.随着壁材与芯材比例的增大,胶囊载药量逐渐降低,微胶囊释放十二醇的速率明显变小,但包覆率却无明显变化规律.     

以CdS-ZnS核-壳量子点/聚酰胺-胺(PAMAM)树形分子纳米复合材料自组装制备发光超薄膜

制备了表面带负电荷的CdS-ZnS核-壳结构量子点/聚酰胺-胺(PAMAM)树形分子纳米复合材料, 并以其为阴离子, 以聚二甲基二丙烯基氯化铵(PDDA)为聚阳离子自组装制备了光致发光(PL)超薄膜. 对膜的生长均匀性、表面平整性及发光性能进行表征, 发现膜的UV-Vis吸收强度和PL强度随层数增加呈线性增大, 表明每层膜均匀生长; AFM照片表明单个复合层膜非常平整, 10层膜仍具有良好的平整度, 并发出明亮的蓝绿色光.     

含浸P204胶囊的芯材缓释与功能性研究

对于含浸10个碳以上双链型表面活性剂的微胶囊体系,已得到了受温度、电场、pH值、化学反应及光控制的功能性胶囊~[1～3].功能性胶囊对芯材的缓释及控制释放作用,在医药、生化等方面的应用具有广阔的前景.但是一般认为对于含浸的双键型表面活性剂的较短链链长不能小于10个碳,对含浸链长小于10个碳的表面活性剂的功能性微胶囊体系未见报道.     

十二甲基六元瓜环包结1,4-二烷噁的晶体结构

合成了全甲基取代六元瓜环(Me_(12)Q[6])与1,4-二噁烷的包结配合物并生长了晶体,通过单晶X-射线衍射方法进行了表征;该配合物形成了以Me_(12)Q[6]为"胶囊体"、1,4-二噁烷为"胶囊"芯材、水分子为"胶囊盖"的"分子胶囊"结构,"分子胶囊"通过氢键自组装形成一维超分子链,而一维的超分子链通过Me_(12)Q[6]端口的羰基氧原子与水分子之间的氢键作用横竖交错组成二维具有空洞结构的分子网.     

丙烯酸共聚物囊壁的正十八烷微胶囊的制备和性能表征

以二丙烯酸1,4-丁二醇酯为交联剂, 成功制备了甲基丙烯酸甲酯-甲基丙烯酸共聚物为壁材, 正十八烷为囊芯的相变材料微胶囊. 采用扫描电子显微镜(SEM)、差示扫描量热仪(DSC)和热重分析仪(TG)分别考察了单体与芯材投料比、单体浓度和交联剂的含量对微胶囊形貌、相变热性能、热稳定性能的影响. 实验结果表明: 随着单体与芯材投料比或单体浓度的增加, 微胶囊表面均变得致密, 壁厚增加; 随着交联剂含量的增加, 微胶囊的表面变得更加致密光滑, 热稳定性显著增强; 随着单体与芯材投料比的增大, 微胶囊热焓值减小, 被包裹的囊芯含量减少.     

单凝聚与复凝聚法制备昆虫激素十二醇微胶囊及其释放行为

通过向明胶溶液中加入硫酸钠溶液的单凝聚方法以及将明胶溶液加入到阿拉伯胶溶液的复凝聚方法,制备了聚合物包覆昆虫激素十二醇的水分散体系微胶囊.通过对凝聚过程中ζ电位与透光率跟踪测试确定了单凝聚中加入硫酸钠的最佳用量以及复凝聚中明胶与阿拉伯胶的相对量.在壁材浓度大于或等于3%条件下制备的复凝聚胶囊的尺寸大于单凝聚微胶囊,但后者的大小分布更均一.除非在2%壁材浓度下,其他条件下复凝聚制备的胶囊的十二醇包覆率明显高于单凝聚胶囊.对胶囊中十二醇在恒湿恒温条件下的释放研究表明,单凝聚胶囊中十二醇很快释放完毕,变化壁材浓度不明显改变其释放行为.相比之下复凝聚胶囊中十二醇的释放对壁材浓度有明显的依赖性.2%壁材浓度制备的胶囊其释放行为类似于单凝聚胶囊;但3%到5%壁材浓度制备的胶囊中十二醇的释放明显分为3个区间,即较快的初始释放、较长时间的恒速释放以及最后阶段释放速率的再次提高直至释放完毕.复凝聚胶囊中十二醇的释放表现出了明显的可控性.文中亦对该体系中昆虫激素十二醇的释放机理作了初步讨论.     

花生酸-钌有机螯合物Ru(phen)2 3+的单分子膜和LB膜中分子聚集行为的研究

以功能性的钌有机螯合物Ru(phen)2 3+作为亚相离子,花生酸在亚相表面上形成稳定的单分子膜.π-A等温线和动态弹性测量表明,此膜因花生酸与钌螯离子发生了静电相互作用而有更大的可压缩性,并在固态区发生了分子聚集.用垂直法成功地制备了嵌有Ru(phen)2 3+离子的超薄有序Y-型LB膜.光谱实验表明,所得LB膜是稳定、均匀的层状三明治结构,在层面内Ru(phen)23+与花生酸结合成相对稳定的分子基团并形成了J-聚体.     

Asymmetric insertion of membrane proteins in lipid bilayers by solid-state NMR paramagnetic relaxation enhancement: a cell-penetrating Peptide example

A novel solid-state NMR technique for identifying the asymmetric insertion depths of membrane proteins in lipid bilayers is introduced. By applying Mn (2+) ions on the outer but not the inner leaflet of lipid bilayers, the sidedness of protein residues in the lipid bilayer can be determined through paramagnetic relaxation enhancement (PRE) effects. Protein-free lipid membranes with one-side Mn (2+)-bound surfaces exhibit significant residual (31)P and lipid headgroup (13)C intensities, in contrast to two-side Mn (2+)-bound membranes, where lipid headgroup signals are mostly suppressed. Applying this method to a cell-penetrating peptide, penetratin, we found that at low peptide concentrations, penetratin is distributed in both leaflets of the bilayer, in contrast to the prediction of the electroporation model, which predicts that penetratin binds to only the outer lipid leaflet at low peptide concentrations to cause an electric field that drives subsequent peptide translocation. The invalidation of the electroporation model suggests an alternative mechanism for intracellular import of penetratin, which may involve guanidinium-phosphate complexation between the peptide and the lipids.     

Assembly of polymeric micelles into hollow microcapsules with extraordinary stability against extreme pH conditions

Hollow microcapsules containing polymeric micelles in their walls were fabricated by alternating assembly of poly(allylamine hydrochloride) (PAH) and poly(styrene- b-acrylic acid) (PS- b-PAA) micelles on MnCO(3) microparticles followed by sacrificing the templates in acid solution. The successful formation of PAH/micelle multilayers on both planar and curved substrates was confirmed by UV-vis spectroscopy, ellipsometry, and xi-potential measurements. The PS- b-PAA micelles retained their structure during the whole assembly process. The as-prepared microcapsules showed extraordinary stability against concentrated HCl (37%) and 0.1 M NaOH solutions. No variation in capsule size or shape was observed in acidic solution, while slight swelling and distortion of the capsules took place in alkaline solution. However, these capsules completely recovered their original size and morphology after being incubated in acidic solution again. The microcapsules, in which large voids exist between the micelle grains on the walls, were totally permeable to fluorescein-tagged dextran with an M(w) of 2000 kDa. Assembly of additional PAH/poly(sodium 4-styrenesulfonate) multilayers could substantially reduce the permeation of the same molecules. These multicompartmental capsules combine polymeric micelles with multilayer polyelectrolyte microcapsules and could possibly be imparted with multifunctions, thus possibly finding diverse applications in the fields of drug delivery, biosensing, and nanobiotechnology.     

超离子导体CaF2中的Ca2+亚晶格和F-亚晶格

CaF_2在熔化以前为超离子导体相。一些实验和理论的研究表明,在超离子导体相中,Ca~(2+)仍维持原有的面心立方骨架,而F~-则在Ca~(2+)骨架中运动。早期的分子动力学模拟结果表明Ca~(2+)的均方根位移仅约0.3A,而F~-的扩散系数可达2.6×10~(-5)cm·s~(-1),已是熔盐扩散系数量级。近年来的中子散射实验表明在扩散离子和近邻离子间存在着某种动力学相关。为解释这些事实,新近Gillan的分子动力学模拟表明扩散离子伴随着F~-亚晶格变形,而Kaneko和Ueda的分子动力学模拟则表明扩散离子伴随着近邻离子在同一运动方向的相关运动。进一步的研究尚待进行。八十年代初,Nelson等人提出了描述晶体、非晶和液态中键取向的键球谐函数方法。     

Nanopore formation and phosphatidylserine externalization in a phospholipid bilayer at high transmembrane potential

Atomic-resolution molecular dynamics simulations of lipid bilayers containing 7% phosphatidylserine (PS) on one leaflet are consistent with experimental observations of membrane poration and PS externalization in living cells exposed to nanosecond, megavolt-per-meter electric pulses. Nanometer-diameter aqueous pores develop within nanoseconds after application of an electric field of 450 mV/nm, and electrophoretic transport of the anionic PS headgroup along the newly constructed hydrophilic pore surface commences even while pore formation is still in progress.     

Bilayer-coated capsule membranes. IV. : Control of NaCl permeability by phase transition of synthetic bilayer coatings,depending on their hydrophilic head groups

Ultrathin nylon capsule membranes coated with synthetic bilayers, the hydrophilic head groups of which had cationic, anionic, zwitterionic and nonionic charges, were prepared. Permeation of NaCl trapped in the inner aqueous phase was reduced by a factor of 10-1000 relative to that of the uncoated, semipermeable capsules, and drastically changed at the phase transition temperature, T_c, of the coating bilayers, depending on the charge of their hydrophilic head group. In the case of capsules coated with positively or negatively charged bilayers, NaCl permeation was enhanced at temperatures above the T_c of the coating bilayers, as expected. On the other hand, NaCl release of capsules coated with neutral charged (nonionic and zwitterionic) bilayers was largely reduced at temperatures above the T_c. From activation energy data of Arrhenius plots, the permeation mechanism of NaCl, depending on the membrane surface charge, below and above the T_c was discussed.     

新型钙荧光探针在H2O2对HL-60胞浆钙影响研究中的应用

采用H2O2、黄嘌呤和黄嘌呤氧化酶、H2O2/抗坏血酸/Fe^2＋（或H2O2/Fe^＋）、H2O2和辣根过氧化酶（HRP）等不同活性氧产生体系,对自行合成的胞浆特异性钙荧光探针STDIn的活性氧耐受性进行了考察.以STDIn-AM为探针标记HL-60细胞,激光共聚焦技术检测单细胞内Ca^2＋-STDIn荧光强度的变化;探讨了不同浓度的H2O2对胞内Ca^2＋浓度变化的影响,从膜结构和生物信号传导的角度研究了氧自由基对培养细胞的生物效应.     

Ca2+、Ba2+对光敏热成像材料照相性能和稳定性的影响

以常用的硬脂酸银为银源,异位AgBr为光敏元以及亲水型PVA为粘合剂,分别考察了Ca2+和Ba2+对光敏热成像(PTG)材料照相性能以及老化稳定性的影响.实验结果表明:涂布前乳液中加入Ca2+或Ba2+后,PTG材料的感光度和灰雾均出现不同程度的降低,并且随着加入量的增加,感光度下降更快.另外,含有Ca2+或Ba2+的PTG材料随着老化时间的增加,其感光度和灰雾的变化趋势并不相同.     

Molecular dynamics study of the effect of calcium ions on the monolayer of SDC and SDSn surfactants at the vapor/liquid interface

The effect of Ca(2+) ions on the hydration shell of sodium dodecyl carboxylate (SDC) and sodium dodecyl sulfonate (SDSn) monolayer at vapor/liquid interfaces was studied using molecular dynamics simulations. For each surfactant, two different surface concentrations were used to perform the simulations, and the aggregation morphologies and structural details have been reported. The results showed that the aggregation structures relate to both the surface coverage and the calcium ions. The divalent ions can screen the interaction between the polar head and Na(+) ions. Thus, Ca(2+) ions locate near the vapor/liquid interface to bind to the headgroup, making the aggregations much more compact via the salt bridge. The potential of mean force (PMF) between Ca(2+) and the headgroups shows that the interaction is decided by a stabilizing solvent-separated minimum in the PMF. To bind to the headgroup, Ca(2+) should overcome the energy barrier. Among contributions to the PMF, the major repulsive interaction was due to the rearrangement of the hydration shell after the calcium ions entered into the hydration shell of the headgroup. The PMFs between the headgroup and Ca(2+) in the SDSn systems showed higher energy barriers than those in the SDC systems. This result indicated that SDSn binds the divalent ions with more difficulty compared with SDC, so the ions have a strong effect on the hydration shell of SDC. That is why sulfonate surfactants have better efficiency in salt solutions with Ca(2+) ions for enhanced oil recovery.