全甲基及其多胺修饰环糊精与牛血清白蛋白的相互作用

制备了两个多胺修饰全甲基化环糊精, 即单-[6-(乙二胺)-6-脱氧]-七-(2,3,6-三甲氧基)-β-环糊精(4)和单-[6-(二乙烯三胺)-6-脱氧]-七-(2,3,6-三甲氧基)-β-环糊精(5), 并采用荧光和紫外-可见光谱方法测定了全甲基化环糊精及其多胺修饰衍生物在磷酸缓冲溶液中(25 ℃, pH=7.2)与牛血清白蛋白形成化学计量比为8∶1的超分子配合物的稳定常数. 结果表明, 全甲基化环糊精对牛血清白蛋白具有强于天然环糊精和部分甲基化环糊精的分子键合能力, 而经过多胺修饰的全甲基化环糊精衍生物则显示了更强的键合能力, 这些强的键合能力源于疏水作用、静电作用和氢键作用的协同效应.     

聚酰胺-胺树状分子接枝到方法修饰多壁碳纳米管

采用聚酰胺-胺树状分子(PAMAM)“接枝到”这一温和而简单易行的方法修饰多壁碳纳米管(MWCNTs),制备了一种树状分子/碳纳米管(MWCNTs-g-PAMAM)纳米复合材料。在水、甲醇和乙醇等极性溶剂中,该复合材料具有很好的分散性。通过傅立叶变换红外光谱(FTIR)、X-射线光电子能谱(XPS)、热重分析(TGA)和透射电子显微镜(TEM)等对MWCNTs-g-PAMAM纳米复合材料进行了表征。FTIR表明接枝修饰是PAMAM与MWCNTs的共价键结合,TGA数据表明PAMAM成功修饰于MWCNTs侧壁,且接枝到MWCNTs上PAMAM的量随其代数(G1.0～G4.0)的不同而不同,具体顺序为G2.0＞G1.0≈G3.0＞G4.0.     

聚酰胺-胺(PAMAM)树状大分子对甲氨蝶呤的包合及缓释研究

以甲氨蝶呤(MTX)为模型药物,研究了G5.0PAMAM树状大分子对其包合和释放,并用13^CNMR对PAMAM-MTX包合物进行了表征.UV-Vis研究结果表明,1个G5.0PAMAM树状大分子能包合27个MTX分子,体外释放研究表明,在37℃,pH=7.4的10mmol/LTris-HCl缓冲溶液中G5.0PAMAM树状大分子对MTX具有明显的缓释作用.     

不同代PAMAM树状大分子与牛血清白蛋白的相互作用研究

采用发散法合成了以乙二胺为核的聚酰胺-胺型(PAMAM)树状大分子,并应用荧光光谱法研究了生理条件下(pH=7.4)3.0代(G3.0)、3.5代(G3.5)和4.0代(G4.0)PAMAM树状大分子与牛血清白蛋白(BSA)的相互作用.结果表明,三种PAMAM树状大分子都能引起牛血清白蛋白荧光猝灭,其程度主要取决于各自末端基团的性质,猝灭机制属于静态猝灭.G4.0PAMAM,G3.5PAMAM和G3.0PAMAM与BSA的猝灭常数分别为2.73,1.69,1.55L·mmol-1.同时考察了体系pH值及离子强度的变化对PAMAM与BSA相互作用的影响.此外,同步荧光和紫外光谱法(UV)以及红边激发荧光位移(REES)等方法的研究结果表明,PAMAM树状大分子的存在改变了BSA的构象.     

喹啉修饰β-环糊精键合胆酸客体的热力学研究

采用微量热滴定、核磁共振和分子模拟等方法研究了三唑基喹啉修饰β-环糊精(1)和羟基喹啉基修饰β-环糊精(2)同胆酸(CA)、脱氧胆酸(DCA)、甘胆酸(GCA)和牛磺胆酸(TCA)的键合行为.二维核磁和分子模拟研究表明胆酸客体分子的尾链和D环部分从大口端进入了环糊精空腔.微量热滴定研究表明两种喹啉基修饰环糊精键合胆酸客体的过程由焓驱动,并且伴随着明显的熵损失,说明主-客体间键合的驱动力主要来自于氢键和范德华相互作用.与天然环糊精相比,喹啉基修饰环糊精对胆酸客体的键合有着更为有利的焓变和更为不利的熵变.     

树状大分子PAMAM(1G)-FCD的合成及荧光性能

合成了外围由小分子2-芴醛修饰的树状大分子PAMAM(1G)-FCD, 用IR, 1H NMR, MALDI-TOF-MS等手段表征了其结构, 并对其荧光性能及Sn2+对该性能的影响进行了研究, 结果表明, Sn2+能使化合物荧光显著增强. 紫外光谱表明, 随着PAMAM(1G)-FCD溶液中Sn2+浓度的增加, 体系在360 nm处出现了新的吸收峰, 表明二者之间存在化学反应. 故该树状分子有望作为难得的蓝光区荧光材料及金属-树状大分子杂化材料.     

以枝形大分子聚酰胺-胺(PAMAM)为键合固定相的开管毛细管电色谱柱的制备及评价

用3-氨丙基三乙氧基硅烷(KH550)作偶联剂, 在毛细管内壁上逐步合成树枝形大分子聚酰胺-胺(PAMAM), 制得了1, 2和3代PAMAM键合的开管毛细管电色谱柱, 并对其性能进行了研究. 结果表明, 随着大分子代数的增加, 毛细管电渗流(EOF)逐步下降. 利用制得的1, 2和3代PAMAM修饰的开管毛细管电色谱柱对丙氨酸和脯氨酸的分离进行对比, 结果显示, 随着大分子PAMAM代数的增加, 分离度逐步增大, 丙氨酸和脯氨酸可在3代树枝状大分子PAMAM修饰的开管毛细管电色谱柱上达到基线分离. 采用非衍生化法和3代PAMAM修饰的开管毛细管电色谱柱成功地分析了精氨酸、 丙氨酸、 脯氨酸、 甲硫氨酸和组氨酸. 结果表明, 键合毛细管柱具有良好的重现性和稳定性.     

Cu2+对联苯甲醛修饰的树状大分子聚酰胺-胺荧光性能的影响

采用小分子联苯甲醛(BPA)分别修饰第一和第二代树状大分子聚酰胺-胺(PAMAM), 合成了2种PAMAM的修饰产物G1-BPA4和G1-BPA8. 利用IR, 1H NMR及MALDI-TOF MS等手段表征了2种产物的结构, 研究了Cu2+浓度对其荧光性能的影响. 结果表明, 在一定的浓度范围内, 作为常见荧光猝灭剂的Cu2+能使2种产物的荧光均显著增强.     

(聚酰胺-胺)树状大分子对甲氨蝶呤的复合和释放研究

以甲氨蝶呤(MTX)为模型药物,研究了PAMAM与MTX的复合及体外释放.1H-,13C-NMR数据表明MTX与PAMAM树状大分子形成复合物是由于MTX羧基和PAMAM树状大分子外端氨基之间的相互作用.该复合物在pH=7.4,10 mmol/L Tris-HCl中非常稳定,表现出明显的缓释效果.当溶液中的离子强度增加时,会破坏PAMAM-MTX复合物的稳定性,缓释作用部分或全部失去,说明PAMAM树状大分子与MTX之间的相互作用属于静电作用.UV测得每个G5.0 PAMAM、G4.0 PAMAM树状大分子分别能复合271、4个MTX分子.     

超分子体系中的分子识别研究(一)──氨基酸修饰β-环糊精对客体分子TNS的包结配位研究

近年来 ,环糊精作为一类重要的分子受体 (主体 )选择性结合底物 (客体 )形成超分子配合物已经成为化学和生物化学等领域的研究热点之一 .在β-环糊精分子中引入特定的官能团 ,可以扩展对客体分子的识别能力 .因此 ,许多工作都致力于环糊精的化学修饰研究 [1～ 3] .我们曾报道的由亲电或亲核试剂修饰后的β-环糊精 ,不仅改变了主体原有的分子键合能力 ,而且扩展了主体对一些模型底物的分子识别能力 [4 ,5] .有关氨基酸修饰β-环糊精的报道尚不多见 .最近 ,我们应用紫外和圆二色谱等手段研究了色氨酸修饰的β-环糊精对客体分子的配位包结作用 …     

Synthesis of conjugates of β-cyclodextrin with polyamidoamine dendrimers and their molecular inclusion interaction with levofloxacin lactate

Polyamidoamine (PAMAM) dendrimers of different generations (G2 and G4) conjugated with β-cyclodextrin (β-CD), PAMAM (G2, G4)-CD, were synthesized using substitution reaction from mono-6-iodine-β-cyclodextrin and PAMAM dendrimers. The resulting molecular structures were characterized by NMR, IR. The molecular interaction between various dendrimers and levofloxacin lactate (LFL) were investigated by monitoring the fluorescence of LFL in the presence of dendrimers in buffer solution (pH 7.4) at 25?°C. It was found that the PAMAM (G2, G4)-CD possesses higher sensitizing ability than that of the corresponding parent dendrimers and natural β-CD, and increases concomitantly with the increases of generation and content of β-CD, suggesting that the PAMAM (G2, G4)-CD possesses stronger inclusion ability with LFL. The possible interaction mechanism between PAMAM-CD and LFL was proposed by ¹H NMR analysis and theoretical calculation. The results show that the LFL molecule is located at the amine end of dendrimer molecule and along the side of cyclodextrin cavities to form supramolecular complexes. Furthermore, results indicate that the main driving force of the complex could be attributed to the electrostatic interactions and hydrogen bonding between LFL and PAMAM-CD, as well as the synergistic effect of intermolecular forces.     

Prilocaine-cyclodextrin-liposome: effect of pH variations on the encapsulation and topology of a ternary complex using 1H NMR

A better comprehension of the prilocaine (PLC)-β-cyclodextrin (β-CD) complex liberation to membranes was provided by studying the architectural supramolecular arrangements of PLC, β-CD and egg phosphatidylcholine (EPC) liposomes, a membrane model. The topologies and possible interactions of mixtures of PLC, β-CD and EPC liposomes were investigated by nuclear magnetic resonances combining experimental (1)H-NMR (1D ROESY, STD and DOSY) at different pHs. The results indicate that in the mixture PLC/β-CD/EPC at pH 10 the PLC molecules are almost totally embedded into the liposomes and little interaction was observed between PLC and β-CD. However, at pH 5.5 not only was PLC imbedded in the EPC bilayer, but PLC was also interacting with β-CD. These results were rationalized as a spontaneous PLC release from β-CD to liposomes vesicles, whereas the PLC/EPC complex formation was higher at pH 10 than pH 5.5.     

Effect of Norfloxacin Complexation with β-Cyclodextrin on the in Vitro Dissolution Behaviour and its Interaction with Mg2+ and Al3+

Interaction between norfloxacin and β-cyclodextrin (β-CD) in solution was characterized by immersion calorimetry studies and nuclear magnetic resonance. ¹H-NMR studies suggest that the pyperazine group of norfloxacin is the part of the molecule bound inside the β-CD cavity. Solid inclusion complexes of norfloxacin with β-cyclodextrin were prepared by freeze-drying in two different molar ratios, 1:1 and 1:2, and characterized by X-ray diffractometry and differential scanning calorimetry. Drug dissolution rate was improved by inclusion complexation and norfloxacin incompatibility with metal cations (Mg²⁺, Al³⁺) was reduced.     

Fluorescent detection of cholesterol using β-cyclodextrin functionalized graphene

A fluorescence based cholesterol detection method has been developed using competitive host-guest interaction between graphene bound β-cyclodextrin (β-CD) with rhodamine 6G (R6G) and cholesterol. Fluorescence of β-CD incorporated R6G is quenched by graphene but is 'turned on' by cholesterol as it replaces R6G from the β-CD host.     

竞争包结法研究β-环糊精及其两种衍生物对一些手性脂肪族客体分子的识别作用

以酚酞作为光谱探针 ,采用紫外 可见光谱滴定法测定了 β 环糊精 (β CD)、单 (6 氧 α 麦芽糖 ) β 环糊精 (6 G2 β CD )和单 [2 氧 (2 羟丙基 ) ] β 环糊精 (2 HP β CD )在 2 5℃时 ,pH =10 5缓冲液中(0 0 2 5mol/L)与几种脂肪族手性客体分子所形成超分子配合物的稳定常数 .结果表明 ,多种弱相互作用力协同作用于环糊精的配位过程 ,主 客体间的尺寸匹配决定所形成配合物的稳定性 .环糊精衍生物的取代基影响主体的配位能力 ,对于尺寸较小的客体分子配位能力的大小一般为 2 HP β CD >β CD >6 G2 β CD .另一方面 ,3种环糊精主体化合物对一些脂肪族客体分子也表现出一定的手性识别能力 ,对 (+ ) 异构体给出相对较强的键合能力 ,其中 ,2 HP β CD对 (+ ) /(- ) 樟脑的配位选择性为 1 2 5 .     

Strong guest binding by cyclodextrin hosts in competing nonpolar solvents and the unique crystalline structure

6-O-Modified β-cyclodextrins, such as heptakis(6-O-triisopropylsilyl)-β-cyclodextrin (TIPS-β-CD) and heptakis(6-O-tert-butyldimethylsilyl)-β-cyclodextrin (TBDMS-β-CD), formed 2:1 inclusion complexes with pyrene in benzene and cyclohexane with high association constants. The X-ray crystalline structure of the TIPS-β-CD-pyrene complex obtained from the benzene solution showed that one pyrene molecule was incorporated in the form of a sandwich-type complex with two benzene molecules within the cavity of the dimer formed by two TIPS-β-CD molecules.     

Inclusion complexes of ortho-anisidine and β-cyclodextrin: A quantum mechanical calculation

The structural aspects for the complexation of ortho-anisidine (O-AN)/β-cyclodextrin were explored by using PM6, density function theory B3LYP/6-31G*, M05-2X/6-31G*, B3PW91/6-31G*, MPW1PW91/6-31G*, HF/6-31G* methods and several combinations of ONIOM2 hybrid calculations. Calculations were performed upon the inclusion complexation of β-cyclodextrin (β-CD) with neutral (O-AN1) and cationic (O-AN2) species of ortho-anisidine. The obtained results with PM6 method clearly indicate that the formed complexes are energetically favored, the complex of O-AN2/β-CD in B orientation is significantly more favorable than the others energetically. The structures show the presence of several intermolecular hydrogen bond interactions that were studied on the basis of natural bonding orbital (NBO) analysis, employed to quantify the donor–acceptor interactions between ortho-anisidine and β-CD.     

Formation of 3Pseudorotaxanes from β-cyclodextrin and a Series of Dicarboxylic Acids with Their Corresponding α,ω-alkanedicarboxylate Anions

Inclusion complexes between β-cyclodextrin (β-CD) and a series of dicarboxylic acids (DAn, n=11-15) were prepared by co-grinding and co-precipitation methods and the 3pseudorotaxane structure of them was eluci-dated by FTIR, DTA and XRD characterizations. Inclusion complexes of β-CD and α,w-alkanedicarboxylate anions (DAn2-) were acquired by neutralizing β-CD/DAn different inclusion complexes with sodium hydrox-ide and the structure was also proved to be a pseudorotaxane structure by 1H-NMR spectra and NOESY spectrum. Both the inclusion complexes of β-CD/DAn and β-CD/DAn2- adopt the 3pseudorotaxane structure with β-CD arranged in dimers threaded onto one aliphatic chain and the binding mode of 1:1 inclusion complex was excluded based on the consideration of chain conformations     

Study on the Supramolecular System of TAPP and Cyclodextrins by Spectroscopy

The ability of β-cyclodextrin (β-CD), γ-CD, hydroxypropyl-β-CD (HP-β-CD), trimethyl-β-CD (TM-β-CD), sulfurbutylether-β-CD (SBE-β-CD) and carboxymethyl-β-cyclodextrin (CM-β-CD) to break the aggregate of the meso-tetrakis(4-N-trimethylaminobenzyl)porphyrin (TAPP) and to form 2:1 inclusion complexes has been studied by absorption and fluorescence spectroscopy. The formation constants are calculated, respectively, by fluorimetry, from which the inclusion capacity of different CDs is compared and the inclusion mechanism of charged-β-CD (SBE-β-CD and CM-β-CD) is quite different from that of the parent β-CD. At lower pH, the complexation between TM-β-CD and H²TAPP²⁺ (the form of the diprotonated TAPP) hampers the continuous protonation of the pyrrole nitrogen of TAPP and the hydrophobic cavity may prefer to bind an apolar neutral porphyrin molecule. ¹HNMR data support the inclusion conformation of the porphyrin–cyclodextrin supramolecular system, indicating the interaction of the meso-phenyl groups of TAPP with the cavity of CDs. For this host–guest inclusion model, cyclodextrin being regarded as the protein component, which acts as a carrier enveloping the active site of heme prosthetic group within its hydrophobic environment, provides a protective sheath for the porphyrin, creating artificial analogues of heme-containing proteins. However, for TAPP, encapsulated within this saccharide-coated barrier, its photophysical and photochemical properties changed strongly.     

β-环糊精交联聚丙烯酸水凝胶的合成及其药物控制释放研究

采用1,3-二环己基碳化二亚胺(DCC)为缩合剂,通过β环糊精与丙烯酸的酯化反应合成了不同取代度的丙烯酸β环糊精酯(βCD6A),以此为单体与丙烯酸通过氧化还原自由基引发聚合,合成出了不同交联密度和不同环糊精含量的新型水凝胶(AAβCD6A).溶胀实验表明,该类水凝胶均具有pH敏感性,溶胀动力学实验进一步对其机理进行了探讨.选择苯丁酸氮芥(CHL)作为模型药物,考察了不同pH下AAβCD6A水凝胶对药物释放行为的影响.结果表明,pH=6.8时药物释放率均大于pH=2.0时药物释放率,环糊精的存在表现出促释作用.