分子内环化对溶胶凝胶分配的影响(Ⅰ)——A_a-B_b型缩聚反应

本文用概率方法推导出包括溶胶中分子内环化反应的溶胶凝胶分配方程。由此方程计算出的理论值同实验值符合很好。     

聚乙烯醇/壳聚糖复合水凝胶的物理化学性质

测定了聚乙烯醇(PVA)和壳聚糖(CS)复合水凝胶的平衡含水量、熔融焓、等温溶胀动力学和非等温失水动力学等性质,讨论了水凝胶的组成和制备参数对这些性质的影响.结果显示:PVA/CS复合水凝胶具有适宜于软骨修复替代材料的网络结构和平衡含水量.CS与PVA复合减弱了凝胶的结晶度,但却增强了水与凝胶支架的相互作用.尽管水凝胶力学拉伸强度有所降低,但却优化了凝胶的生物相容性和降解能力.PVA/CS复合水凝胶是一种潜在的软骨修复材料,作为一种理论研究的模型体系,它将促进热力学在复杂医用材料方面的应用.     

交联聚乙烯醇水凝胶对胆红素的吸附性能研究

本文采用反相聚合的方法以戊二醛为交联剂合成了珠状交联聚乙烯醇凝胶，并研究了它对胆红素的吸附性能。结果表明交联聚乙烯醇对胆红素的体外吸附率受到吸附剂的交联度、颗粒直径、溶液中白蛋白的浓度、吸附温度及离子强度的影响。该类吸附剂对胆红素具有良好的吸附动力学性能。     

聚乙烯醇水凝胶溶胀特性研究

在前文对聚乙烯醇水溶液冰冻凝胶化浓度依赖性研究基础上，对接触浓度（Ｃ）以上聚乙烯醇水溶液通过冰冻－融化处理，制得了一种含水率高达９５～９８％的水凝胶．系统研究了该水凝胶在蒸馏水中的溶胀及溶解特性．得到了一个与实验结果相吻合的溶胀动力学方程：Ｑ１＝Ｑｅ－（Ｑｅ－ＱＯ）／ｅｋｔ，及平衡溶胀比Ｑｅ与浓度之间的定量关系：Ｑｅ＝６０．３－４．４５×１０２Ｃ．发现当冰冻－融化次数Ｎ≤５时，平衡溶胀比Ｑｅ及溶解量Ｗ与冰冻－融化次数（Ｎ）间满足幂函数关系：Ｑｅ。Ｗ通过对聚乙烯醇水凝胶平衡溶胀比与经冰冻处理的聚乙烯醇水溶液特性粘数进行比较，发现反映链间氢键凝聚缠结效应与反映链内氢键凝聚缠结效应的定量指标具有等效性．     

含内环化A—Bb,Cc缩聚反应的溶胶—凝胶分配

结合Ａａ－Ｂｂ，Ｃｃ型缩聚反应，给出了溶胶中含内环化的溶胶－凝胶分配公式及凝胶化条件。     

聚乙烯醇缩酮化度的定量表征

本文在不同条件下制备出聚乙烯醇（ＰＶＡ）与丙酮的缩酮化产物ＰＶＫＴ。进一步利用核磁共振（＾１Ｈ－ＮＭＲ，＾１３Ｃ－ＮＭＲ）、红外光谱（ＩＲ）、紫外光谱（ＵＶ）三种测试手段建立了表征缩酮化度的方法，从不同角度分析了上述方法在表征缩酮化度的准确性。     

含内环化A_a－B_b，C_c缩聚反应的溶胶－凝胶分配

结合Ａａ－Ｂｂ，Ｃｃ型缩聚反应，给出了溶胶中含内环化的溶胶－凝胶分配公式及凝胶化条件。     

壳聚糖/聚乙烯醇/三聚磷酸钠三元复合微球的制备及表征

由壳聚糖（ＣＳ）、聚乙烯醇（ＰＶＡ）和三聚磷酸钠（ＴＰＰ）制备了壳聚糖／聚乙烯醇／三聚磷酸钠三元复 合微球,探讨了体系中壳聚糖含量对复合微球的影响,以及离子种类及浓度和ｐＨ值对复合微球溶胀度的影 响。采用ＸＲＤ、ＦＴＩＲ和ＳＥＭ等测试技术对微球的组分、结构和形貌进行了表征。结果表明,ＣＳ和ＰＶＡ具有良好的相容性,随着ＣＳ含量的增加,ＰＶＡ的结晶性逐渐降低,复合微球的粒径约为４００～９５０ μｍ,表面较为粗糙;随着ＣＳ添加量的增加,凝胶平衡溶胀度先增大再减小,ＣＳ／ＰＶＡ／ＴＰＰ复合微球在ｐＨ值为３～8的溶胀度最大,且在同一种溶液中,随着离子浓度的增加,其溶胀度明显降低;复合微球具有溶胀 收缩可逆性,显示ＣＳ／ＰＶＡ／ＴＰＰ复合微球是ｐＨ／离子敏感型凝胶,可为药物缓释系统提供实验和理论依据。     

聚乙烯醇磷酸酯水凝胶电刺激响应行为的研究

以脲为催化剂,将聚乙烯醇(PVA)磷酸酯化制成聚乙烯醇磷酸酯,再经戊二醛交联制备了一种新型的聚乙烯醇磷酸酯水凝胶.研究了水凝胶的溶胀性能,力学性能和电刺激响应行为.结果表明,该凝胶在NaCl水溶液中其平衡溶胀率随NaCl溶液的离子强度增大而减小.在离子强度为0~0.2的NaCl水溶液中,其弹性模量为0.300~0.356 MPa,抗张强度为91.5~137.8 kPa,断裂伸长率为32.0%~37.5%,且均随离子强度的增大而增大.在去离子水和NaCl水溶液中于非接触直流电场作用下,凝胶向电场负极弯曲,弯曲速度和应变随外加电压的增大而增大,并随NaCl离子强度的增大于0.005处出现极大值.在循环电场作用下,聚乙烯醇磷酸酯水凝胶的电刺激响应行为具有良好的可逆性.     

利用聚乙烯醇结晶辅助制备多重交联的高强度聚丙烯酰胺水凝胶

在表面带有C=C双键的乙烯基杂化二氧化硅纳米颗粒(vinyl hybrid silica nanoparticle,VSNP)上接枝丙烯酰胺(AM),所得到的纳米刷状凝胶因子通过聚丙烯酰胺(PAM)间的氢键形成物理交联点,则多官能化的VSNP可作为拟共价交联点构筑双重交联的单一网络纳米复合物理水凝胶(nanocomposite physical hydrogel,NCP gel),表现出较高的强度和超拉伸性.为了进一步提高凝胶的强度和韧性,将少量PVA和PAM/VSNP纳米刷混合制成凝胶,通过冷冻-融化处理,使与PAM分子链相互缠绕并形成氢键作用的PVA结晶,形成新的交联点进一步交联PAM NCP gel,得到多交联的PAM NCP gel体系.通过拉曼光谱和示差扫描量热分析,证明凝胶中的PVA通过氢键既可以与PAM相互作用,又形成微晶为新交联点,大大增强了NCP gel的力学性能,与PAM NCP gel相比,凝胶的拉伸强度和断裂能分别从313 k Pa和1.41×104 J/m~2提高到了557k Pa和4.65×104 J/m~2.     

Palladium‐Catalyzed Chemoselective Intramolecular Cyclization of 2‐Bromoaryl Alkenenitriles

The chemoselectivity in the palladium‐catalyzed intramolecular cyclization of 2‐(o‐bromoaryl)‐alkenenitriles depends on the nature of α‐substitutents. 2‐(o‐Bromoanilino)alkenenitriles attacked the cyano group, followed by the cyano group transposition and hydrolysis, to give o‐(methylamino)benzonitrile. 2‐(o‐Bromobenzyl)alkenenitriles, 2‐(o‐bromophenylthio)alkenenitriles and 2‐(o‐bromophenoxy)‐alkenenitriles attacked the olefinic double bonds and led to l‐vinyl‐2‐indancecarbonitrile, 1,2,3,4‐tetrahydronaphthalene‐2‐carbonitriles, 3,4‐dihydro‐2H‐benzo[b]thiine‐2‐carbonitriles, and 3,4‐dihydro‐2H‐benzo[b]oxine‐2‐carbonitriles. A general mechanism for the palladium‐catalyzed arylations is proposed.     

One Pot Spiropyrazoline Synthesis via Intramolecular Cyclization/Methylation

Regioisomeric spiropyrazolines were synthesized through a tandem intramolecular cyclization/methylation reaction of a functionalized 5,5-disubstituted pyrazoline in one reaction vessel. The 5,5-pyrazolines were constructed through a 1,3-dipolar cycloaddition reaction of aromatic ring containing nitrile imines and a disubstituted geminal alkene. An evaluation of the relative location of the nucleophilic and electrophilic functional groups on the pyrazoline was performed in order to ascertain the best pyrazoline system for the intramolecular cyclization/methylation reaction. Higher spiropyrazoline isolated yields were realized from pyrazolines with the electrophilic ester located further away from the pyrazoline when compared to pyrazolines with a directly bonded ester.     

Synthesis of Highly Substituted N-Hydroxy Piperidine via Intramolecular Reductive Cyclization of 1-Keto-5-ketoxime

Abstract

Diasteroselective synthesis of highly substituted N-hydroxypiperidine was achieved by an intramolecular reductive cyclization of monoxime (2) of the 1,5-diketone (1), generated from 2-(cyclohexylthio)-1-phenylethanone and arylaldehyde, using NaBH₃CN. The major product N-hydroxypiperidine (3) has been found to be racemate of a single diastereomer.     

Studies of Intramolecular Cyclization of 4-Arylpyridines. II Syntheses of Condensed Tricyclic Pyridines

A convenient method for the synthesis of condensed tricyclic pyridines using intramolecular cyclization of 4-arylpyridines is reported. The tricyclic compounds, 2-azafluorenone (9), 2-azafluorenone (10), 2-azafluorenol (11), lactones 12 and 13, and anhydride 14 have been prepared.     

Intramolecular Cyclization of 1-Benzyl-2-(nitromethylene)pyrrolidines in Triflic Acid

1-Benzyl-2-(nitromethylene)pyrrolidines in triflic acid undergo intramolecular cyclization to afford the corresponding 2,3-dihydro-1H-pyrrolo[1,2-b]isoquinolinium triflates and/or 10-amino-2,3-dihydro-1H-pyrrolo[1,2-b]isoquinolinium triflates, depending on the nature of the aromatic substituent. Structures of products and reaction mechanisms are discussed.     

Total Synthesis of Spirotryprostatins through Organomediated Intramolecular Umpolung Cyclization

Cyclodipeptide 2,5-diketopiperazines (DKP) are privileged structural units present in drugs and natural alkaloids. This work reports a new method for the synthesis of biologically important DKP scaffolds based on an intramolecular nucleophilic α-addition of general amides towards an alkynamide system. The utility of this umpolung cyclization mediated by trimethyl phosphine and l -glutamic acid is highlighted by its application to the concise total syntheses of 6-methoxyspirotryprostatin B (the first total synthesis), spirotryprostatin A, and spirotryprostatin B.     

Intramolecular cyclization and subsequent rearrangements of alkyne-tethered N-heterocyclic carbenes

Alkyne-tethered imidazole and 1,2,4-triazole-based N-heterocyclic carbene precursors have been prepared and studies of the intramolecular reactions of carbenes are performed. Products consistent with intramolecular cyclizations and subsequent rearrangements were observed. Mechanistic studies using crossover experiments showed that the products did arise from intramolecular carbene additions. The reactions are proposed to go through vinylogous diaminocarbene intermediates similar to vinylogous dialkoxycarbenes formed during Boger cycloaddition reactions. Imidazole substituted dienes were observed to be the major products of tandem cyclization and elimination reactions that were observed for imidazole-based N-heterocyclic carbenes.     

P（DMAA-co—AM）水凝胶制备及其固定a-淀粉酶研究

采用氧化还原引发体系,水溶液聚合法制备P（DMAA-co-AM）水凝胶,并以其作为载体固定a-淀粉酶。采用单一变量法研究交联剂（N,N＇-亚甲基双丙烯酰胺）用量、引发剂（过硫酸铵）用量、单体浓度和单体配比对凝胶性能的影响。以水凝胶的最大平衡溶胀度为指标,得出制备P（DMAA-co-AM）水凝胶的优化条件：交联剂用量为0．3％,引发剂用量为0．6％,单体浓度为20％,N,N’-二甲基丙烯酰胺与丙烯酰胺的摩尔比为2：1。在优化条件下,采用原位聚合法固定a-淀粉酶,测定不同单体配比的P（DMAA-co-AM）水凝胶固定化a-淀粉酶的活性。     

Synthesis of Benzazepinones via Intramolecular Cyclization Involving Ketene Iminium Intermediates

Herein, we describe a very straightforward and metal free method for the synthesis of benzazepinones through an intramolecular cyclization. This involves an ortho‐vinyl‐anilino‐amide as starting material which is converted to a keteniminium intermediate that spontaneously cyclize to form a 7‐membered ring iminium. Under slightly basic hydrolysis conditions, this latter is ultimately converted to the desired benzazepinone. Control experiments on the electron density of the nitrogen constituting the aniline were performed to support our proposed mechanism and rationalize the selectivity of the reaction.