Tunable Supramolecular Assembly and Photoswitchable Conversion of Cyclodextrin/Diphenylalanine‐Based 1D and 2D Nanostructures

A photocontrolled, interconvertible supramolecular 2D‐nanosheet/1D‐nanotube system was constructed through the supramolecular assembly of adamantanyl‐modified diphenylalanine with azobenzene‐bridged bis(β‐cyclodextrin). The nanosheet exhibited a greater fluorescence enhancement effect than the nanotube. Significantly, these nanosheets and nanotubes could interconvert via the photocontrolled trans/cis isomerization of azobenzene linkers in bis(β‐cyclodextrin), and this photo‐switchable one‐dimensional/two‐dimensional morphological interconversion was reversible and recyclable. This enables convenient routes to highly ordered nanostructures with various morphologies and dimensions that can be controlled by external stimuli.     

联喹啉桥联双环糊精对染料客体分子的协同键合

采用荧光光谱滴定的方法测定了一系列联喹啉桥联双环糊精在磷酸缓冲溶液中(25 ℃, pH＝7.2)与几种染料客体分子形成化学计量比为1∶1的超分子配合物的稳定常数. 结果表明, 拥有刚性和大(电子体系的联喹啉桥联双环糊精比相应的联吡啶桥联双环糊精对三角形的RhB分子和线形的AR分子具有更强的分子键合能力. 二维核磁的研究证实, 桥联双环糊精对客体分子强的键合能力起源于在一个分子内两个环糊精单元的协同键合. 桥联双环糊精对染料客体分子的选择键合能力从主-客体间的尺寸/形状匹配以及几种弱相互作用力的协同效应进行了讨论.     

三嗪基苯胺桥联双环糊精的合成及其对染料分子的选择键合

通过N,N-二乙基-4-(二氯代-1,3,5-三嗪-2-基)苯胺分别与单-[6-(乙二胺基)-6-脱氧]-β-环糊精和单-[6-(二乙烯三胺基)-6-脱氧]-β-环糊精反应合成了两种三嗪基苯胺桥联双环糊精, 采用荧光和紫外光谱滴定方法测定了它们在磷酸缓冲溶液中(25 ℃, pH＝7.2)与几种具有不同形状和电子密度的染料分子包结配位的稳定常数. 结果表明, 三嗪基苯胺桥联双环糊精不但对具有较大电子密度的三角形客体结晶紫给出了6～26倍于天然环糊精的配位稳定常数, 而且对结晶紫/中性红分子对给出了高的分子选择性(K_CV/K_NR＝23～31). 分子力学研究表明, 桥联双环糊精对客体分子的强键合能力主要源于两个环糊精空腔及桥链基团对客体分子的协同键合, 特别是桥链中三嗪基苯胺基团与客体之间的p-p相互作用.     

Supramolecular polymers based on cyclodextrins

Two types of supramolecular polymers based on cyclodextrins were prepared. One was a host–guest type, and the other was a polyrotaxane type. When a guest part was covalently attached to cyclodextrin, they formed supramolecular dimers, a cyclic daisy chain, supramolecular oligomers, and polymers. t-Boc-cinnamamide-α-cyclodextrin was found to form chiral supramolecular polymers in aqueous solutions. Supramolecular poly[2]rotaxane polymers and supramolecular α,β-cyclodextrin copolymers were obtained. Polyrotaxanes containing β-cyclodextrin or γ-cyclodextrin were prepared. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 44: 5113–5119, 2006     

Excitonic coupling interactions in the self-assembly of perylene-bridged bis(β-cyclodextrin)s and porphyrin

A supramolecular self-assembly has been constructed by perylene-bridged bis(β-cyclodextrin)s with water-soluble porphyrin through hydrophobic interactions, showing strong excitonic coupling interactions between perylene backbones and included porphyrins.     

Photocontrolled Reversible Conversion of Nanotube and Nanoparticle Mediated by β‐Cyclodextrin Dimers

A photochemically interconvertible supramolecular nanotube–nanoparticle system was constructed through secondary assembling of self‐aggregates of amphiphilic porphyrin derivatives mediated by trans‐ and cis‐azobenzene‐bridged bis(permethyl‐β‐cyclodextrin). Significantly, these nanotubes and nanoparticles were able to interconvert upon irradiation at different wavelengths, and this photocontrolled morphological conversion is reversible and recyclable for tens of times, which will provide a feasible and convenient way to construct the ordered nanostructure with various morphologies that can be smartly controlled by the environmentally benign external stimulus.     

Synthesis of Cyclodextrin and Sugar-Based Oligomers for the Efavirenz Drug Delivery

Summary: In the present work water-soluble lactose based oligomers of β-cyclodextrin were synthesized by a simple and efficient condensation polymerization process. Proposed water-soluble β-cyclodextrin oligomers were prepared by controlled reaction between β-cyclodextrin and a triazine linker and purification by an ultrafiltration process. Similarly, lactose based β-cyclodextrin oligomers were synthesized for enhanced water solubility. The physical and chemical properties of the synthesized polymers were characterized by FT-IR and ¹H NMR spectroscopy, XRD analysis, thermogravimetric analysis (TGA) and aqueous solubility determination.. Molecular weights of these β-cyclodextrin based oligomers were measured by ESI technique. These β-cyclodextrin based water-soluble oligomers polymers were used as supramolecular carriers for efavirenz (an anti HIV drug), improving the inclusion property and aqueous solubility properties of this drug. These synthesized oligomers were found to improve stability and aqueous solubility of efavirenz on their (1:1) inclusion complex through phase solubility and dissolution studies. Reduced cytotoxicity than the parent β-CD was observed in hemolysis test.     

Surface-up click access to allylimidazolium bridged cyclodextrin dimer phase for efficient enantioseparation

In this work, a novel allylimidazolium-bridged bis(β-cyclodextrin) chiral stationary phase was fabricated via a surface-up thiol-ene click chemistry reaction between 7-SH-β-cyclodextrin and 1-allylimidazole-β-cyclodextrin bonded on a silica surface. The structure of the allylimidazolium-bridged bis(β-cyclodextrin) chiral stationary phase was characterized by Fourier transform infrared spectra, ¹³C nuclear magnetic resonance, thermogravimetric analysis, and elemental analysis. Its chiral chromatographic performances were systematically evaluated by separating 35 racemic analytes including isoxazolines, dansyl-amino acids, and flavanones under reversed-phase high-performance liquid chromatography. Compared with the corresponding bottom and top layer of the β-cyclodextrin stationary phase, the allylimidazolium-bridged bis(β-cyclodextrin) chiral stationary phase afforded significantly accentuated chiral recognition ability due to its abundant hydrogen bond sites, electrostatic interactions, and synergistic inclusion. Furthermore, the allylimidazolium-bridged bis(β-cyclodextrin) chiral stationary phase showed better enantioseparation ability compared to other reported bridged cyclodextrin stationary phases. In particular, Ar-Phs and dansyl-amino acid could be completely separated by allylimidazolium-bridged bis(β-mono-6^A-deoxy-6-allylimidazolium-β-cyclodextrin chiral stationary phase) chiral stationary phase with high resolutions of 1.14–7.20 and 3.16–5.82, respectively. Molecular docking reveals that good enantioseparation ability arises from the different interaction modes and the synergistic effect of allylimidazolium-bridged bis(β-cyclodextrin) chiral stationary phase.     

Molecular Recognition and Cooperative Binding Ability of Fluorescent Dyes by Bridged Bisβ-cyclodextrin)s Tethered with Aromatic Diamine

A novel bridged bis(β-cyclodextrin),m-phenylenediimino-bridged bis(6-imino-6-deoxy-β-cyclodextrin) (2), was synthesized by the reaction of m-phenylenediamine and 6-deoxy-6-formyl-β-cyclodextrin. The inclusion complexation behavior of the novel bridged bis(β-cyclodextrin) 2,as well as native β-cyclodextrin (1),p-phenylenediamino-bridged bis(6-amino-6-deoxy-β-cyclodextrin) (3) and 4,4'-bianilino-bridged bis(6-amino-6-deoxy-β-cyclodextrin) (4) with representative fluorescent dye molecules, i.e., acridine red (AR), neutral red (NR), Rhodamine B (RhB), ammonium 8-anilino-1-naphthalenesulfonate (ANS) and sodium 6-toluidino-2-naphthalenesulfonate (TNS), was investigated at 25 °C in aqueous phosphate buffer solution (pH 7.20) by means of fluorescence, and circular dichroism, as well as 2D NMR spectrometry. The spectrofluorometric titrations have been performed to calculate the complex stability constants (K_S) and Gibbs free energy changes (Δ G°) for the stoichiometric 1 : 1 inclusion complexation of 1–4 with fluorescent dye molecules. The results obtained demonstrated that bis(β-cyclodextrin)s 2–4 showed much higher affinities toward these guest dyesthan native β-cyclodextrin 1. Typically, dimer 2 displayed the highest binding ability upon inclusion complexation with ANS, affording 35 times higher K_S value than native β-cyclodextrin. The significantlyenhanced binding abilities of these bis(β-cyclodextrin)s are discussed from thebinding mode and viewpoints of size/shape-fit concept and multiple recognition mechanism.     

β-cyclodextrin mediated synthesis of indole derivatives: reactions of isatins with 2-amino(or 2-thiole)anilines by supramolecular catalysis in water

An elegant, mild, and straightforward strategy for the synthesis of indole derivatives have been accomplished by the biomimetic catalysis for the first time in water under neutral conditions. This supramolecular catalyst oriented methodology provides a sustainable and green protocol for the synthesis of 6H-indolo[2,3-b]quinoxalines and 3H-spiro[benzo[d]thiazole-2,3’-indolin]-2’-one by the reaction of isatin derivatives with 1,2-difunctionalized benzene using β-cyclodextrin (β-CD) as a recoverable and reusable supramolecular catalyst.     

一种新型芳香二胺桥联β-环糊精对染料的分子识别

以单-(6-对甲苯磺酰基)-β-环糊精和3,3′-亚甲基联苯胺为原料, 合成了一种新型刚性结构的芳香二胺桥联环糊精, 3,3′-亚甲基联苯胺桥联(6-氨基-6-脱氧-β-环糊精)2. 并用荧光光谱和紫外光谱技术分别测定了在25 ℃时, pH为7.20的磷酸缓冲溶液中β-环糊精(1)和新型桥联环糊精(2)与几种染料分子, 如吖定红(AR)、中性红(NR)、2-对甲苯胺基-6-萘磺酸钠(TNS)、1-苯胺基-8-萘磺酸铵(ANS)、罗丹明B(RhB)和亮绿(BG)形成超分子配合物的稳定常数KS. 化学计量比表明, 桥联环糊精2与客体形成了1∶1的超分子配合物, 其对客体的键合能力和分子选择性远远强于母体?茁-环糊精, 如桥联环糊精2对BG的键合能力可以达到母体环糊精的22.2倍. 从主-客体间的尺寸匹配关系和多重识别机理等方面探讨了桥联环糊精对客体分子的协同键合作用.     

Supramolecular polymers formed by cinnamoyl cyclodextrins

6-Cinnamoyl α-cyclodextrin (6-CiO-α-CD) and 6-cinnamoyl β-cyclodextrin (6-CiO-β-CD) were prepared. 6-CiO-α-CD formed intermolecular complexes to give supramolecular oligomers. 6-CiO-β-CD formed insoluble supramolecular complexes in the solid state. The structures of these complexes are discussed. © 2003 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 3519–3523, 2003     

Inclusion complexation of a novel diaminodiphenyl disulphide bridged bis(β-cyclodextrin) with bile salts

A novel 4,4′-diaminodiphenyl disulphide bridged bis(β-cyclodextrin) (β-CD) 2 was synthesised, and its inclusion complexation behaviour with bile salts, i.e. cholate (CA), deoxycholate (DCA), glycocholate (GCA) and taurocholate (TCA) have been determined in phosphate buffer (pH 7.20) at 25°C by the fluorescence and 2D NMR spectroscopy. The stoichiometry of resulting inclusion complexes between bis(β-CD) 2 and bile salts was demonstrated, showing 1?:?1 binding model upon all inclusion complexation. The structures of the inclusion complexes between bile salts and bis(β-CD) 2 were elucidated by 2D NMR experiments, indicating that the D-ring and side-chain of bile salts, penetrate into one CD cavity of 2 from the wide opening deeply, while the phenyl moiety of the CD linker is partially self-included in the other CD cavity to form host-linker-guest binding mode. As compared with the native β-CD 1 upon complexation with bile salts, the bis(β-CD) 2 enhances the binding ability and molecular selectivity.     

Photocontrolled transparent–opaque transition of a thermosensitive homopolymer solution based on an azobenzene–cyclodextrin system

A solution displaying photocontrolled transparent–opaque transition was prepared through combination of a thermosensitive polymer, poly(N-(3-ethoxypropyl)acrylamide) (PEPAAm), with α-cyclodextrin (α-CD) and a water-soluble azobenzene compound, Azo-Py⁺. α-CD increased the cloud point of an aqueous solution of PEPAAm through formation of inclusion complexes between α-CD and the side groups of PEPAAm. After Azo-Py⁺ was added, the cloud point of the solution decreased because most of the α-CD formed complexes with Azo-Py⁺. The concentration of free α-CD was changed by photocontrolled inclusion of Azo-Py⁺ in α-CD or exclusion of Azo-Py⁺ from α-CD, allowing the cloud point of PEPAAm/α-CD/Azo-Py⁺ solution to be changed up and down. Consequently, the transparent–opaque transition of this solution was realised by alternating irradiation with UV and visible light at 38°C.     

Correlation between Thermodynamic Behavior and Structure in the Complexation of Modified β-Cyclodextrins and Bile Salts

Complex stability constants (K _S), standard molar enthalpy changes (ΔH ⁰) and entropy changes (ΔS ⁰) for the inclusion complexation of two cyclodextrin dimers, 6,6′-{2,2′-diselenobis[2-(benzoylamino)ethylamino]}-bridged bis(β-cyclodextrin) (1) and o-phenylenediseleno bridged bis(β-cyclodextrin)s (3), and their monomer analogs, 6-deoxy-6-{[2-(2,3-dihydro-3-oxo-1,2-benzisoselenazol-2-yl)ethyl]amino}-β-cyclodextrin (2) and mono[6-(phenylseleno)-6-deoxy]-β-cyclodextrin (4), with two bile salt guests, sodium cholate (CA) and sodium deoxycholate (DCA), were determined at 25°C in Tris buffer solutions (pH 7.4) at 298.15?K by means of isothermal titration microcalorimetry (ITC). The interactions and binding modes between the host cyclodextrins and the guest bile salts were further studied by ROESY spectroscopy. The thermodynamic parameters obtained, together with the ROESY spectra, were used to examine the correlations between thermodynamic behavior and binding modes of the host–guest complexation. The results indicate that the length, structure and conformation of the tethers linked to the cyclodextrins determine the binding modes and the binding abilities between hosts and guests to a great extent, leading to a reversion in binding ability when comparing the corresponding dimer and its monomer analog.     

超分子体系强的分子识别研究 23: 多胺修饰β-环糊精及其铜 配合物与萘衍生 物的包结配位作用

用荧光光谱滴定法测定了单-[6-(二乙烯三胺)-6-脱氧]-β-环糊精(1)、单-[6-(三乙烯四胺)-6-脱氧]-β-环糊精(2)及其铜配合物(3,4)与一系列萘衍生物在磷酸缓冲溶液(pH7.2,0.1mol.dm^-^3)中,25℃时形成超分子体系的稳定常数,并与母体β-环糊精的配位能力进行了比较。化学计量法表明,四种化学修饰β-环糊精与萘衍生物形成了1:1的超分子配合物。从尺寸适合、几何互补及多点识别等方面讨论了主体化合物对模型底物的分子选择性键合能力。结果表明,疏水相互作用、范德华力、静电相互作用及氢键等多种非共价键弱相互作用协同贡献于超分子配合物的形成,主-客体间的结构匹配在分子受体选择性键合底物形成超分子配合物中起重要作用。     

Supramolecular self-assembly and nanoencapsulation of [60]fullerene by bis-β-cyclodextrin

Bis-β-cyclodextrin connected via ethylene diamine on the primary side of the β-cyclodextrin was synthesized and used for the supramolecular non-covalent inclusion complex with C₆₀ in a mixed solvent system at room temperature. The apparent association constant of the 2:2 inclusion complex determined by combination of UV–Vis absorbance and Benesi–Hildebrand equation was found to be 1.78 × 10⁶ M^?1. The product obtained was highly water-soluble and superior in stability in aqueous medium as compared to previously known β-cyclodextrin/C₆₀ complex. The non-covalent self-assembly of bis-β-cyclodextrin and C₆₀ was characterized and confirmed from FT-IR, UV–Vis, XRD and TGA. The supramolecular aggregation behavior and particle size of the inclusion complex was found from transmission electron microscope and static light scattering measurements. The size of the inclusion complex was found to be ~30 ± 5 nm.     

Supramolecular assemblies of Al3+ complexes with vitamin D3 (cholecalciferol) and phenothiazine. Encapsulation and complexation studies in β-cyclodextrin

Ternary assemblies of β-cyclodextrin with cholecalciferol (or vitamin D₃) or phenothiazine and Al³⁺ ions were studied. The stability constants of aluminium binary complexes with cholecalciferol or phenothiazine and of ternary assemblies (β-cyclodextrin, cholecalciferol or phenothiazine and Al³⁺) were determined using potentiometric titrations at 25 °C (I = 0.100 M). The ¹³C NMR spectra of the supramolecular structures in the solid state showed that ternary supramolecular structures associating β-cyclodextrin, cholecalciferol or phenothiazine and aluminium(III) ions were obtained. Finally, X-ray powder diffraction patterns showed that the ternary assemblies with phenothiazine are channel type inclusion complexes.     

β-环糊精衍生化胰酶的合成及其手性分离性能研究

研究了β-环糊精衍生化胰酶的合成以及作为毛细管电色谱手性选择剂的分离性能. 利用乙二醇二环氧丙烷醚作为交联剂, 将β-环糊精接枝到胰酶蛋白的主链, 得到了β-环糊精衍生化胰酶. 将其通过化学键合连接到毛细管柱内壁, 制备了β-环糊精衍生化胰酶毛细管电色谱柱. 在加压毛细管电色谱模式下, 利用该柱分离了色氨酸、扑尔敏、布洛芬、异丙嗪和阿托品等对映异构体, 得到了理想的分离效果, 且在分离扑尔敏时, 随着电压的增加, 对映异构体分离的分离度和相对保留时间均增加.     

Molecular Recognition of Aliphatic Alcohols and Carboxylic Acid by Chromophoric Cyclodextrins

Abstract

Molecular recognition behavior of eight cyclodextrin derivatives, i.e. mono(6-pyridinio-6-deoxy)-α-cyclodextrin (1α), mono(6-pyridinio-6-deoxy)-β-cyclodetrin (1β), mono(6-pyridinio-6-deoxy)-γ-cyclodextrin (1γ), mono[6-(p-picolinio)-6-deoxy]-β-cyclodextrin (2β), mono(6-anilino-6-deoxy)-β-cyclodextrin (3β), mono[6-(m-toluidino)-6-deoxy]-β-cyclodextrin (4β), mono[6-O-(8-quinolyl)]-β-cyclodextrin (5β), and novel mono[6-(2-naphthylamino)-6-deoxy]-β-cyclodextrin (6β), with a series of aliphatic alcohols and carboxylic acid has been investigated spectroscopically. Using the appended aromatic group as a spectral probe, spectroflurometric or spectropolarimetric titrations have been performed at 25°C in aqueous phosphate buffer solution (pH 7.20, 0.1 M) to determine the complex stability constants (K_s ) and Gibbs free energy changes (-δG°) for the stoichiometric 1:1 inclusion complexation of cyclodextrin derivatives with the guests. The results obtained demonstrate that the modified cyclodextrins are highly sensitive to the size/shape and hydrophobicity of guest molecules, and particularly 5β gives an excellent molecular selectivity up to 215 for 1-adamantanol/cyclohexanol. The binding ability and selectivity of the modified cyclodextrins (1α, 1β, and 1β-6β) are discussed from the view points of size/shape-fit concept, induced-fit interaction, and the multiple recognition mechanisms.