环糊精的实际应用进展

综述近年环糊精在药物、食品工业、环境保护、除臭剂、生物医学、化妆品以及电化学方面的应用。     

现代仪器分析技术在纺织品及皮革分析中的应用

现代分析技术以仪器分析为主,大量先进的现代仪器分析技术已经广泛地应用于纺织品及皮革分析。介绍了气相色谱（GC）、液相色谱（LC）、色谱质谱联用（GC-MS、LC-MS）、原子吸收（AAS）、电感耦合等离子发射光谱（ICP-OES）等现代仪器分析技术在纺织品及皮革分析中的研究进展与应用。     

基于环糊精的荧光传感器*

基于环糊精的荧光传感器研究倍受人们关注,近年来得到了迅速发展。本文阐述了环糊精络合物的形成以及它们的分子识别机理,在此基础上详细综述了丹酰、芘、萘等荧光基团修饰的环糊精单体及含多个主体的荧光传感器的制备及应用研究现状。此外,对基于环糊精超分子络合物的荧光传感器2003年以后的发展也进行了介绍,同时展望了该领域的发展趋势。     

基于环糊精的分子印迹技术

基于环糊精的分子印迹技术综合了超分子化学、高分子化学、分析化学等多学科优势,对人为可控的大型超分子主体化合物的合成有着指导意义,对具有多位点识别人工酶的实现也有巨大的推动作用。本文综述了近年来基于环糊精的分子印迹技术的研究进展：首先介绍了不同种类的基于环糊精的分子印迹产物的合成,包括合成思路、步骤、方法以及识别机理探讨;然后着重叙述了该体系的应用研究进展,包括其在分子识别、色谱分离、电化学传感器以及生物学控制等领域的应用;最后指出目前研究工作存在的不足,并对其发展前景进行了展望。     

Release Characteristics of Iodine Encapsulated in Cyclodextrins

The effect of cyclodextrins (CDs) on water solubility of iodine was investigated. Modified CDs greatly enhanced the solubility of iodine. On the contrary, enhancement by natural CDs was rather moderate whereby the solubility was only doubled at the highest β-CD concentration examined. Desorption experiment of iodine from solution was carried out with addition of various CDs to study the effect of CDs on iodine retention. α-CD was the most efficient in retarding iodine desorption. Later, various concentrations of α-CD were used in the desorption experiment to observe its volatile suppression effect and determine the stability constant of iodine/α-CD complexation. At α-CD concentration of 10.3 mM, no lost of iodine from the solution was detected. A model was developed for desorption of iodine from the solution based on mass transfer theory. The stability constant K given by this model was 3.28×10⁴ M⁻¹ which was in the same order as the value estimated in this study by solubility method and as well those reported by other authors. In release experiments of solid state inclusion complexes, stability of inclusion complex powders decreased in the order of α-CD>β-CD>randomly methylated β-CD (RM-β-CD).     

Effects of Cyclodextrins on Chymotrypsin Action

Inhibition by cyclodextrins ofchymotrypsin-catalysed hydrolysis of N-acetyl-L-tyrosineethyl ester (ATEE) and of N-succinyl-L-phenylalaninep-nitroanilide (SUPHEPA) was measured. Rates ofproteolysis are reduced by a factor of three tofour by a four-molar ratio of cyclodextrin tosubstrate, except for -cyclodextrin andSUPHEPA where the rate reduction is much less.The kinetics of inhibition, as well as NMR andUV measurements, were used to measureassociation constants between the cyclodextrinsand substrates. Agreement between these methodsconfirmed that inhibition by cyclodextrins isdue to steric effects at the substrate, ratherthan direct interaction with the enzyme.     

Intramolecular Inclusion of L-tryptophan within 3-functionalized Cyclodextrins

Abstract

The synthesis of L-tryptophan attached to the C3 group of a β-cyclodextrin through amide linkages with ethylenediamine or propylenediamine is reported. Circular dichroism and fluorescence investigations were carried out showing great differences between the two derivatives. The derivative containing the propylenediamine chain shows clear self-inclusion and exhibits spectral variations upon guest inclusion detected both by circular dichroism or by fluorescence. The difference in conformation of the two derivatives could be explained on the basis of the chain length.     

环糊精及其衍生物在手性识别中的应用

详细地论述了环糊精及其衍生物在手性识别中的应用,并对环糊精超分子体系手性识别中的进一步研究提供了依据。     

环糊精与聚合物的包合作用

本文着重介绍了环糊精及其衍生物与聚合物所形成的各种包合物,并扼要介绍了它们的研究和应用前景。     

Novel Glycolipids Based on Cyclodextrins

Novel amphiphilic cyclodextrins have been prepared by grafting a phospholipid on a modified cyclodextrin through a spacing arm to combine the selectivity in size of cyclodextrins and the transport properties of phospholipids. Synthesis and full characterization by NMR and mass spectrometry have been performed. The aggregation process in water has been characterized by light scattering, DSC and ³¹P NMR. This compound appears to assemble into large objects and displays a very low CMC. The detergent properties of the phospholipidyl-cyclodextrins have been evaluated.     

Energetics of Water/Cyclodextrins Interactions

The heat capacities of solid -CD, 8.1 H₂O and -CD, 6.0 H₂O have been measured between 10 and 300 K by adiabatic calorimetry. Using earlier results obtained in similar experiments with anhydrous cyclodextrins and with -CD, 9.7 H₂O, a comparative analysis has been developed. The energetic behaviours of anhydrous and hydrated cyclodextrins (CDs) have been compared in order to investigate the role of water molecules in the stabilization of the cyclodextrin's rings and on their reactivities. Calculations, based on the additivity of thermodynamic properties, provide the energetic and entropic average contributions of water molecules in each cyclodextrin. From these results, we assumed that the water–water and water–CD interactions are rather different according to the cyclodextrin. In the (-CD, 9.7 H₂O) structure, the water molecules seem to be better organised in a relatively independent network. Concerning hydrated -CD and -CD, stronger water–CD interactions probably prevent an optimal organisation of the water–water bonds network. Differential scanning calorimetry was also used to follow the evolution of the thermal behaviour of -CD, nH₂O versus hydration ratio between 170 and 300 K. Our results indicate that the -CD ring needs at least 1.6 water molecules to be stabilized in the solid state.     

有机相变材料的发展及在纺织领域的应用

相变材料因为其优良的热性能,被广泛应用于纺织品、航空航天、交通运输、农业、国防、建材、太阳能系统和医疗设备等领域。近年来,开发应用新型相变材料已经成为研究热点。本文首先概括介绍了相变材料发展进程,着重介绍了有机相变材料,包括它的分类、性能和应用。详细介绍了有机相变材料在纺织行业的应用,以及对调温纺织品测试手段的研究和建立的相关数学模型的建立。     

Cyclodextrins lessen the membrane damaging effect of nonionic tensides

Nonylphenyl-ethyleneoxide polymers containing 5, 9 and 30 ethyleneoxide groups per molecule build into the hydrophobic fatty acid chains of the cell membrane phospholipid dipalmitoyl-phosphatidylcholine (DPPC) resulting in a decreased main transition temperature, a decreased enthalpy of the main transition and in enhanced potassium permeability of DPPC liposomes. The -, - and -cyclodextrins form inclusion complexes with the tenzides lowering their free concentration. The complex formation lessens or sometimes totally prevents the membrane damaging effect of tensides. The effectivity order of cyclodextrins is CD>CD>CD.Presented at the Fourth International Symposium on Inclusion Phenomena and the Third International Symposium on Cyclodextrins, Lancaster, U.K. 20–25 July 1986.     

Interactions with Charged Cyclodextrins and Chiral Recognition

Anionic N-acetylated -aminoacids (AcTrp^-, AcPhe^-, AcLeu^- and AcVal^-) are bound to protonatedheptakis(6-amino-6-deoxy)--cyclodextrin(per-NH₃ ⁺--CD) by a cooperative work of inclusion and Coulomb interactions.Such complexation occurs enantioselectively ((S)-selective)and is accompanied bypositive entropy changes. Similar (S)-selectivecomplexation occurs in the oppositelycharged system. Namely, cationic -aminoacid methyl esters are enantioselectivelybound to dissociatedheptakis(6-carboxymethylthio-6-deoxy)--cyclodextrin(per-COO^---CD). In order to obtain thegeneral mechanism for complexationof a charged host with an oppositely charged guest,we examined the ¹H NMR spectra oncomplexation of simple carboxylate anions suchas p-methylbenzoate anion andalkanoate anions with per-NH₃ ⁺--CD.Both Coulomb interactions andinclusion are essential to form stable complexesof these carboxylate anions. In allcases, positive entropy changes promote thecomplexation between the carboxylateanions and per-NH₃ ⁺--CD. Dehydrationfrom both charged host and guestis the origin of entropic gains. The mechanism forcomplexation of a charged host withan oppositely charged guest involving the cooperativework of inclusion and Coulombinteractions and positive entropy change due todehydration upon complexation isgenerally applied for related systems such asenantioselective complexation ofRu(phen)₃ ²⁺ with per-COO^---CDand of Ru(phen)₃ ²⁺with DNA.     

Bile Acids-Selective Chemosensors Based on NBD-amine-Modified Cyclodextrins

A new type of fluorescent chemosensor, based on modified cyclodextrins bearing the fluorophore unit NBD-amine, was prepared. One of these new chemosensors, NC0γCD is very sensitive to bile acids, but is not sensitive to other guests (e.g. adamantane and borneol derivatives). The response of the new type of chemosensor to a guest was an increase in the fluorescence intensity and the sensitivity parameter (ΔI/I ₀ ) dose not correlate to the binding affinity of NC0γCD.     

环糊精及其衍生物的超分子晶体结构研究进展

本文对近年来有关环糊精、环糊精衍生物以及它们与各类客体组装成的超分子包合物的晶体结构研究进行的简要概述。     

烷氧基苯基卟啉与环糊精的超分子体系研究

合成了5种非水溶性烷氧基苯基卟啉, 以荧光光谱法、紫外可见分光光度法和1H NMR法研究了其与环糊精相互作用形成的超分子体系. 并以荧光光谱法测定了超分子体系的包结常数和包结比, 对其包结机理进行了初步研究. 在此基础上, 探讨了不同取代位置、不同链长的烷氧基对非水溶性烷氧基苯基卟啉与不同空腔直径的环糊精的超分子体系的影响.     

抗抑郁化合物SIP15838和环糊精分子非共价复合物的研究

报道了用电喷雾电离质谱(ESI-MS),并结合紫外分光光度法及溶解度实验,研究一种新型的具有自主知识产权的抗抑郁化合物SIPI5838与α-环糊精(CD)和β-环糊精(CD)分子生成的非共价复合物.质谱测量结果表明,在溶液中,SIPI5838分子可以与环糊精分子之间生成非共价复合物,且两者之间的配比关系为1:1.这些非共价复合物的形成可以显著地提高这种抗抑郁化合物在水溶液中的溶解度,使得它作为高效的口服或注射药物成为可能.另外,还用紫外分光光度法和溶解度实验对液相中非共价复合物的形成进行了辅助研究,这些结果均显示了非共价复合物的生成.根据溶解度实验结果,计算了SIPI5838和两种环糊精分子在液相中的生成常数.它们分别为SIPI5838-β-环糊精:1.83×103 mol-1·L,SIPI5838-α-环糊精:3.15×101mol-1·L.两种非共价复合物的稳定程度为β-环糊精-SIPI5838>α-环糊精-SIPI5838.     

抗抑郁化合物SIPI5838和环糊精分子非共价复合物的研究

报道了用电喷雾电离质谱(ESI-MS), 并结合紫外分光光度法及溶解度实验, 研究一种新型的具有自主知识产权的抗抑郁化合物SIPI5838与α-环糊精(CD)和β-环糊精(CD)分子生成的非共价复合物. 质谱测量结果表明, 在溶液中, SIPI5838分子可以与环糊精分子之间生成非共价复合物, 且两者之间的配比关系为1∶1. 这些非共价复合物的形成可以显著地提高这种抗抑郁化合物在水溶液中的溶解度, 使得它作为高效的口服或注射药物成为可能. 另外, 还用紫外分光光度法和溶解度实验对液相中非共价复合物的形成进行了辅助研究, 这些结果均显示了非共价复合物的生成. 根据溶解度实验结果, 计算了SIPI5838和两种环糊精分子在液相中的生成常数, 它们分别为SIPI5838-β-环糊精: 1.83×103 mol－1•L, SIPI5838-α-环糊精: 3.15×101 mol－1•L. 两种非共价复合物的稳定程度为β-环糊精-SIPI5838＞α-环糊精-SIPI5838.     

Cyclodextrins and the Biopharmaceutics Classification System of Drugs

Although the biopharmaceutics classification system (BCS) was originally developed for solid oral dosage forms this system can be extended to other types of drug delivery forms. According to the BCS aqueous solubility and permeability are the most important parameters affecting drug bioavailability. Cyclodextrins can enhance the aqueous solubility of lipophilic drugs without changing their intrinsic ability to permeate biological membranes. Thus, through cyclodextrin complexation it is possible to move Class II drugs, and sometimes even Class IV drugs, into Class I. However, cyclodextrins can decrease bioavailability of Class I drugs and will in most cases not improve bioavailability of Class III drugs. Through formation of drug/cyclodextrin/polymer ternary complexes it is possible to enhance the complexation efficacy of cyclodextrins and at the same time improve drug bioavailability from cyclodextrin containing drug formulations.