Study on Inclusion Complexes of Cyclodextrin with Sodium Dodecyl Polyoxyethylenated Sulfonate Using Microcalorimetry and 1H NMR

The association of α‐, β‐ and γ‐cyclodextrin (α‐CD, β‐CD and γ‐CD) with sodium dodecyl polyoxyethylenated sulfonate (C₁₂E_nS n=1, 3) was studied by means of isothermal titration calorimetry and ¹H NMR measurements in aqueous solution at T=298.15 K. The results indicate that the binding processes of β‐CD with the surfactants are characterized by both enthalpy favorable and entropy favorable, while those of α‐CD or γ‐CD with the surfactants are mainly entropy driven. The stoichiometry of β‐CD binding with the surfactants is different with different numbers of oxyethyl groups in surfactant molecules, while that of α‐CD or γ‐CD binding with the surfactants makes no difference. The ¹H NMR spectra reveal that chemical shift data of all protons in α‐CD, β‐CD and γ‐CD molecules move to high field in the presence of C₁₂E_nS, which can be regarded as a microscopic evidence of the occurrence of inclusion interaction.     

Determination of Binding Constants for Cyclodextrin Complexes with Alkanols by the 1H NMR Measurements of Longitudinal Relaxation Time Using Tetramethylammonium Chloride as an Internal Reference

The longitudinal relaxation times (T₁)of ¹H NMR signals for a variety of alkanols in D₂Omarkedly decreased with increasing concentrations (c)of - and -cyclodextrins (CD). Tetramethylammoniumchloride (TMA) used as an internal reference wasavailable for evaluating an effect of solutionviscosity on relaxation rates R(=1/T₁), since TMAshowed no appreciable interaction with CD. Changes inthe ratio of R for alkanol protons to R for TMAprotons with c were analyzed by the curve-fittingmethod to give K_a. These K_a values agreedwell with those obtained by the analysis of changesin , indicating that T₁ measurement is available forthe determination of K_a for CD complexes. 2D ROESYspectra provided definite information on the molecularstructures of CD complexes with alkanols.     

环糊精包结物的制备与研究方法

环糊精是由6,7,8个葡萄糖基构成的环状化合物,分别叫做α,β,γ-CD。它们具有亲水的外围及疏水的内腔,可与多种物质形成包结物,而改变物质的特性,因而被广泛应用于各行各类,为了更好地研究环糊精包结物,在查阅大量文献的基础上,总结出环糊精包结物的多种制备方法及研究方法。     

Complexation study of midazolam hydrochloride with beta-cyclodextrin: NMR spectroscopic study in solution

(1)H NMR spectroscopic study of midazolam hydrochloride (MDL), beta-cyclodextrin (beta-CD) and their mixtures confirmed the formation of beta-CD-MDL inclusion complex in aqueous solution. The stoichiometry of the complexes was determined by Scott's method to be 1:1, and the association constant (K(a)) was calculated to be 108 M(-1). It was confirmed on the basis of 2D ROESY spectral data that only a fluorine-substituted aromatic ring acted as guest in complexation. Most of the aromatic signals of MDL exhibited induced shift changes as well as splitting, in the presence of beta-CD, indicating chiral differentiation of MDL by beta-CD.     

Formation of Inclusion Complexes between Cyclodextrins and Carbaryl and Characterization of the Complexes

The solubility of carbaryl increased with increasing concentrations of-CD, G₂--CD, and M--CD. The result suggests theformation of soluble inclusion complex. Solubility increase was highestin M--CD-carbaryl, being 18.4 fold higher than that of carbaryl when 100 mM M--CD was used. The apparent formation constant for the complex calculated from phase solubility diagram was 223.18 M^-1. The preparation of the complex in solid form for characterization was successful by kneading andfreeze-drying. The DSC curves for kneading and freeze-drying mixture didnot show the endothermic peak characteristic of carbaryl, but a small new endothermic peak was observed. FTIR analysis showed a shift of the major peak of carbonyl group in carbaryl molecule from 1717 to 1744 and 1734 cm^-1 in kneading and freeze-dried mixtures, respectively. M--CD-carbaryl complex demonstrated higher dissolution rate, higher thermal and UV stability but lower toxicity than its parent carbaryl compound.     

Experimental Analysis of Complex Formation of Niflumic Acid with β-Cyclodextrins

Complex formation of niflumic acid with β-, hydroxypropyl-β- and methyl-β-cyclodextrins in aqueous solution (pH 7.4) were studied by calorimetry of solution, ¹H NMR spectroscopy and solubility method. The enhancement of niflumic acid solubility in the presence of hydroxypropyl-β-cyclodextrin was detected. This effect is explained on the basis of ¹H NMR data confirming the inclusion of hydrophobic trifluoromethylphenyl residue of niflumic acid molecule into the macrocyclic cavity. The thermodynamic parameters of 1:1 binding were derived from the data of␣calorimetry and solubility measurements. It was obtained, that complex formation of niflumic acid with β-cyclodextrin and both its derivatives is enthalpy driven. Substitutes surrounding the macrocyclic cavity slightly influence the thermodynamics of complex formation resulting in decrease of stability of the complexes formed.     

Quantitative ROESY analysis of computational models: structural studies of citalopram and β‐cyclodextrin complexes by 1H‐NMR and computational methods

Complexation of racemic citalopram with β‐cyclodextrin (β‐CD) in aqueous medium was investigated to determine atom‐accurate structure of the inclusion complexes. ¹H‐NMR chemical shift change data of β‐CD cavity protons in the presence of citalopram confirmed the formation of 1 : 1 inclusion complexes. ROESY spectrum confirmed the presence of aromatic ring in the β‐CD cavity but whether one of the two or both rings was not clear. Molecular mechanics and molecular dynamic calculations showed the entry of fluoro‐ring from wider side of β‐CD cavity as the most favored mode of inclusion. Minimum energy computational models were analyzed for their accuracy in atomic coordinates by comparison of calculated and experimental intermolecular ROESY peak intensities, which were not found in agreement. Several least energy computational models were refined and analyzed till calculated and experimental intensities were compatible. The results demonstrate that computational models of CD complexes need to be analyzed for atom‐accuracy and quantitative ROESY analysis is a promising method. Moreover, the study also validates that the quantitative use of ROESY is feasible even with longer mixing times if peak intensity ratios instead of absolute intensities are used. Copyright © 2015 John Wiley & Sons, Ltd.     

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.     

Cyclodextrin inclusion of four phenylurea herbicides: determination of complex stoichiometries and stability constants using solution 1H NMR spectroscopy

An inclusion complex formation between α- and β-cyclodextrin and four phenylurea analogues, namely metobromuron, monolinuron, monuron and fenuron, is reported. Complex formation was established using solution ¹H NMR spectroscopy. Complex stoichiometries were determined by the method of continuous variation using the chemically induced shifts of both the host and guest protons. An analysis of the spectroscopic data revealed the stoichiometry as 1:1 in all cases while a further analysis of the same data yielded values for the association constant K ranging from 208 to 2749 M^? 1. From the observed chemical shifts it was deduced that in all cases, only the guest aromatic ring enters the host cavities, the substituted urea moiety protruding from the secondary rim in the case of α-cyclodextrin, but from the primary rim in the case of β-cyclodextrin.     

Spectral Studies on the Cyclodextrin Inclusion Complexes of Toluidine Blue O and Meldola's Blue in Aqueous Solution

The absorption and emission spectral properties of toluidine blue O (TBO) and Meldola's blue (MDB) in the presence of cyclodextrins (CDs) were studied. Formation of 1 : 1 and 1 : 2 (CD-Dye) inclusion complexes were observed with -CD and -CD, respectively. An increase in the emission intensity was noticed in the presence of -CD due to the formation of 1 : 1 (CD-Dye) inclusion complexes. However, a decrease in the emission intensity was observed in the presence of -CD due to the formation of 1 : 2 (CD-Dye) inclusion complexes. Dimerization of dye molecules in the presence of -CD lead to a decrease in the emission intensity. The formation constants for the 1 : 1 and 1 : 2 (CD-Dye) inclusion complexes were calculated.     

Structure determination of fexofenadine‐α‐cyclodextrin complex by quantitative 2D ROESY analysis and molecular mechanics studies

Complexation of fexofenadine with α‐cyclodextrin in aqueous medium was studied. The stoichiometry of the resulting inclusion complex was determined by ¹H NMR titration data. 2D ROESY data provided the evidence of formation of the complex by entry of the phenyl ring into the α‐cyclodextrin cavity probably from wider opening. Determination of relative peak intensities of intermolecular cross‐peaks for the most stable complexes obtained by molecular mechanics (MM2) studies and from 2D ROESY spectral data confirmed the presence of only one complex in solution that has been fully characterized. Copyright © 2012 John Wiley & Sons, Ltd.     

环糊精与乙烯和三十烷醇包结物的研究

本文报道在常压下制备了α-环糊精-乙烯包结物的微细晶体,和环糊精与三十烷醇的溶胶与粉末包结物,以增加长链烷基醇的溶解度。其溶胶在室温下放置半年不凝聚。还用X-射线粉未衍射法、1~H核磁共振及差热-热重分析等方法研究了包结物的形成。     

NMR spectroscopic investigation of inclusion complexes between cyclodextrins and the neurotoxin tetramethylenedisulfotetramine

The binding stoichiometry, strength and structure of inclusion complexes formed between the neurotoxin tetramethylenedisulfotetramine (TETS) and both native and modified cyclodextrins (CyDs) were investigated using nuclear magnetic resonance (NMR) spectroscopy. Of all six examined cases, native β‐cyclodextrin (β‐CyD) and its chemically modified counterpart heptakis‐(2,3,6‐tris‐(2‐hydroxypropyl))‐β‐cyclodextrin (2HP‐β‐CyD) were found to associate most strongly with TETS as reflected in the magnitude of their binding constants (K = 537 ± 26 M^?1 for β‐CyD and K = 514 ± 49 M^?1 for 2HP‐β‐CyD). Two‐dimensional rotating‐frame Overhauser effect spectroscopy NMR experiments confirm close proximity of the TETS molecule to both β‐CyD and 2HP‐β‐CyD as intermolecular, through‐space interactions between the H3 and H5 protons located in the interior of the CyD cavity and the methylene protons of TETS were identified. Copyright © 2012 John Wiley & Sons, Ltd.     

Solid State NMR Studies of the Bromocyclohexane/Thiourea Inclusion Compound

Solid state ¹³C-MAS and ²H-NMR investigationshave been performed on the bromo-cyclohexane/thiourea inclusion compound.The main objective of this study was the evaluation of the molecularfeatures of the guest molecules and their changes over a large temperaturerange (100 K < T < 350 K). Particular emphasis was placed on themolecular behaviour in the vicinity of a solid–solid phase transitionat T = 237 K and in the low temperature phase, which was hitherto unknown.The ²H-NMR lineshape and relaxation studies reveal that, inthe low temperature phase, restricted but fast overall motions (MHz to GHzregion) of the guest molecules are dominant and reflect the distortedsymmetry of the thiourea channels. On heating above the solid–solidphase transition almost unrestricted overall motions appear, together with alarge degree of orientational disorder at higher temperature. Furthermore,the ring interconversion process presents a major relaxation process in theMHz region. The conformational order is unusual in the sense that the axialconformational state of the guest molecules is stabilized in the thioureachannels. It turns out that this unique property is also preserved in thelow temperature phase.     

Spironolactone and its Complexes with β-cyclodextrin: Modern NMR Characterization and Structural DFTB-SCC Calculations

In the present work, inclusion complexes of spironolactone (SP) with β-cyclodextrin (β-CD) in solid phase and aqueous solution were studied by solubility methods, NMR spectroscopy and thermal analysis. The results showed different kinds of complexations when freeze-drying and kneading methods were used. The freeze-drying product (1:1, SP:β-CD) showed lower degree of complexation and stability than the (1:2, SP:β-CD) compound obtained by kneading method. The spironolactone molecule was also studied by NMR spectroscopy at 400 MHz. The chemical shifts of all spironolactone atoms and their inclusion compounds were assigned. Extensive use of 1D and 2D NMR techniques, including ROESY experiment, allowed verifying the position of the spironolactone molecule inside the cyclodextrin cavity in both situations. In addition, DFTB-SCC quantum mechanical calculations of the inclusion compounds were performed. The predicted structural properties are in good agreement with ROESY NMR results.     

The Respective Benefits of X-ray Crystallography and NMR for the Structural Determination of the Inclusion Complex Between Butyl-isothiocyanate and Alpha-cyclodextrin

Isothiocyanates are natural products extracted from plants. These molecules which exhibit very interesting antifungal properties, are insoluble in water. To increase their solubility, we have prepared inclusion complexes with different cyclodextrins. Among all the isothiocyanates studied, we have investigated in more detail the structure of one complex: butyl-isothiocyanate and alpha-cyclodextrin, using two different techniques. Firstly, ¹H NMR experiments were performed and revealed the inclusion phenomenon. In parallel, crystals of butyl-isothiocyanate–alpha-cyclodextrin were grown and their crystallographic structure determined. This confirmed the inclusion of the ITC molecules and allowed us to determine the exact position of the guest. Finally, we showed that even though the complex structure was determined separately in solution and in the solid state, the structural characterisations obtained with these two techniques are complementary, enhancing the respective benefits of X-ray crystallography and NMR.     

Analysis of lipoproteins using 2D diffusion-edited NMR spectroscopy and multi-way chemometrics

This study represents the first application of multi-way calibration by N-PLS and multi-way curve resolution by PARAFAC to 2D diffusion-edited ¹H NMR spectra. The aim of the analysis was to evaluate the potential for quantification of lipoprotein main- and subfractions in human plasma samples. Multi-way N-PLS calibrations relating the methyl and methylene peaks of lipoprotein lipids to concentrations of the four main lipoprotein fractions as well as 11 subfractions were developed with high correlations (R = 0.75-0.98). Furthermore, a PARAFAC model with four chemically meaningful components was calculated from the 2D diffusion-edited spectra of the methylene peak of lipids. Although the four extracted PARAFAC components represent molecules of sizes that correspond to the four main fractions of lipoproteins, the corresponding concentrations of the four PARAFAC components proved not to be correlated to the reference concentrations of these four fractions in the plasma samples as determined by ultracentrifugation. These results indicate that NMR provides complementary information on the classification of lipoprotein fractions compared to ultracentrifugation.     

NMR characterization of the host-guest inclusion complex between beta-cyclodextrin and doxepin

The interaction between doxepin, a member of the tricyclic antidepressant (TCA) class of drugs, with beta-cyclodextrin (beta-CD) was investigated using NMR. Several TCAs have been reported to form a complex with beta-CD having 1:1 stoichiometry. Previous results from UV-visible spectroscopy, fluorescence measurements, and molecular modeling indicated that for imipramine, desipramine, and amitriptyline, the TCA aliphatic tail is included in the cyclodextrin cavity with apparently no interaction of the tricyclic ring. An alternative view of the doxepin-beta-CD complex is presented in this work using analysis of complexation-induced chemical shifts (CICSs), the method of continuous variation (Job's analysis), and analysis of ROESY spectra. The Job's plot derived from the NMR spectral data confirms that the complex formed has 1:1 stoichiometry. The largest changes in the CICS data were observed for the aromatic protons of one of the doxepin rings, with much smaller chemical shift changes observed for the protons of the other aromatic ring and the doxepin tail. Perhaps the most significant evidence for inclusion of the doxepin tricyclic ring is the strong ROESY cross peaks between the doxepin aromatic resonances and the protons located inside the beta-CD cavity. Changes in the doxepin (1)H NMR spectrum and the behavior of ROESY exchange cross peaks suggest that inclusion complex formation decreases the rate of internal motions of doxepin.