Preparation and characterization of the inclusion complex of Ofloxacin with ��-CD and HP-��-CD

The formation of the inclusion complexes of Ofloxacin with cyclodextrins (CDs) including ??-cyclodextrin (??-CD), and hydroxypropyl-??-cyclodextrin (HP-??-CD) were studied by Fluorescence, UV?CVis absorption spectroscopy and nuclear magnetic resonance spectroscopy (NMR) in solution. Experimental conditions including the concentration of various CDs and media acidity were investigated in detail at room temperature. The results suggested that in different pH solutions, CDs have different inclusive capacity to different forms Ofloxacin. ??-CD was most suitable for inclusion of neutral form and HP-??-CD was suitable for acidic form. The binding constant (K) of the inclusion complex was determined by fluorescence measurement, and the complexation ratio was determined as 1:1 in the concentration range used in this study. A mechanism was proposed to explain the inclusion process based on the experimental NMR data.     

Inclusion complex of (−)-linalool and β-cyclodextrin

(?)-Linalool is a monoterpene alcohol which is present in the essential oils of several aromatic plants. Recent studies suggest that (?)-linalool has antimicrobial, anti-inflammatory, anticancer, antioxidant, and antinociceptive properties in different animal models. The aim of this study was to prepare and characterize inclusion complexes of (?)-linalool with β-cyclodextrin (β-CD). Equimolar binary (?)-linalool/β-CD systems were prepared by physical mixture, paste (PM), and slurry methods (SC) and characterized by differential scanning calorimetry, thermogravimetric analysis, FT-IR spectroscopy, X-ray diffractometry, Karl Fisher titration, and scanning electron microscopy. Thermal characterization indicates the occurrence of complexation, mainly in paste complexes, which is present in the interval from 140 to 280 °C a gradual mass loss (4.6 %), probably related to (?)-linalool loss. FT-IR spectra showed changes that may be related to the formation of intermolecular hydrogen bonds between (?)-linalool and β-CD. The new solid-phase formed using the PM and SC methods, had a crystal structure which was different from the original morphology of β-CD.     

Inclusion Complexation of β-CD with Phenothiazine and N-Alkylphenothiazine Derivatives

Phenothiazinederivatives(PTZ)havebeenstudiedfOrdecadesbecauseoftheirwideapplicationsintranquilizingdrugs,dyestuffsandsolarenergyconversionmaterialsI.Recently,westudiedtheelectrontransferreactionsofNsubstilutedphenothiazinewithelectronacceptorsinAcyclodextrin(ffCD)aqueous,olution2'3.TheelectrontransferprocesswassignificantlyinfluencedbythepresenceofffCD.IthasbeennotedthatthePTZwereincludedbyACDtoforminclusioncomplexes.Inthisletter,wereportthestudyofinclusioncomplexationofffCDwithphenoth…     

Study of inclusion complex of β-cyclodextrin and diphenylamine: photophysical and electrochemical behaviors

The photophysical, electrochemical and photoprototropic behaviors of diphenylamine (DPA) in aqueous β-cyclodextrin (β-CD) solution have been investigated using absorption spectroscopy and cyclic voltammetric techniques. Absorption of the neutral and cationic form of DPA is enhanced due to the formation of a 1:1 complex with β-CD. The formation of this complex has been confirmed by Benesi-Hildebrand plot and docking studies by RasMol tool methods. The solid complex of β-CD with DPA is investigated by FT-IR, XRD and AFM methods. The thermodynamic parameters (ΔG, ΔH and ΔS) of inclusion process are also determined. The pK(a) values of neutral-monocation equilibria have been determined with absorption (conjugate acid-base) titrations. A mechanism is proposed to explain the inclusion process.     

Spectroscopic studies of inclusion complex of β-cyclodextrin and benzidine diammonium dipicrate

Formation of inclusion complex between benzidine diammonium dipicrate and β-cyclodextrin with stoichiometry 1:2 (guest–host) has been established by UV, ¹H NMR, ¹³C NMR, IR spectra and powder X-ray diffractometry. ¹H NMR studies are used to confirm the inclusion and to provide information on the geometry of dipicrate inside the cavity of β-cyclodextrin.     

Study on complex formation equilibria of tervalent lanthanons with fluorinated β-ketoesters in aqueous dioxane medium

Summary The thermodynamic stepwise formation constants (log ^T K _n) of nine tervalent lanthanons (La³⁺, Pr³⁺, Nd³⁺, Sm³⁺, Eu³⁺, Gd³⁺, Dy³⁺, Er³⁺ and Lu³⁺) with three fluorinated -ketoesters (methyltrifluroacetoacetate, ethyltrifluoroacetoacetate, and ethylpentafluoropropionylacetate) have been evaluated potentiometrically in a 50% dioxane-water mixture at 25 and 35 ± 0.01 °C. The values of log ^T K _n do not follow a linearity when plotted againstZ/r and invariably obey the sequence: La³⁺ < Nd³⁺ < Pr³⁺ < Sm³⁺ < Gd³⁺ < Eu³⁺ < Dy³⁺ Er³⁺ Lu³⁺ in all instances. The standard thermodynamic parameters (G ₁ ⁰ , H ₁ ⁰ , S ₁ ⁰ ) associated with log ^T K _n have also been calculated. The validity of the chosen equilibrium model was examined by an error analysis usingS _min values (sum of the squared residuals), scatter plots, and slopes and intercepts of Abrahams-Kave type normal probability plots.

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Komplexbildungsgleichgewichte von dreiwertigen Lanthanoiden mit fluorierten -Ketoestern in wäßrigem Dioxanmedium

Zusammenfassung Es wurden die thermodynamischen stufenweisen Komplexbildungskonstanten (log ^T K _n) von 9 dreiwertigen Lanthanoiden (La³⁺, Pr³⁺, Nd³⁺, Sm³⁺, Eu³⁺, Gd³⁺, Dy³⁺, Er³⁺ und Lu³⁺) mit drei fluorierten -Ketoestern (Methyltrifluoracetoacetat, Ethyltrifluoracetoacetat und Ethylpentafluopropionylacetat) in 50% Dioxan-Wasser bei 25 und 35±0.01 °C potentiometrisch bestimmt. Die Werte für log ^T K _n ergeben keine lineare Abhängigkeit gegenüberZ/r, sie gehorchen stets der Reihenfolge: La³⁺ < Nd³⁺ < Pr³⁺ < Sm³⁺ < Gd³⁺ < Eu³⁺ < Dy³⁺ Er³⁺ Lu³⁺. Die thermodynamischen Standardparameter G ₁ ⁰ , H ₁ ⁰ und S ₁ ⁰ wurden ebenfalls berechnet. Die Gültigkeit des gewählten Gleichgewichtsmodells wurde unter Verwendung der Summe der Quadratreste (S _min), von Streukurven und Steigung/Ordinatenabschnitt der Normalwahrscheinlichkeitsdarstellung nach Abrahams-Kave untersucht.

     

Encapsulation of apple polyphenols in β-CD nanosponges

Rutin, phloridzin and chlorogenic acid are some of the most important and characteristic polyphenols found in apples and their by-products (cider, apple juice, apple pomace, etc.). Despite their antioxidant power, their low stability under light or heating conditions restricts the use of this kind of molecules as nutraceuticals. To deal with this issue, encapsulation seems to be an alternative solution. Based on the obtained results, it can be concluded that β-cyclodextrin nanosponges (β-CD NS) are promising agents for the encapsulation of polyphenols. Rutin, phloridzin and chlorogenic acid have been included for the first time in β-CD NS in this work. In particular, the highest encapsulation efficiency for rutin (83.7 %) was obtained using 1,1′-carbonyldiimidazole as cross-linker in a 1:3 ratio (nanosponge/cross-linker). However, for smaller molecules as phloridzin and chlorogenic acid, the nanosponge which showed the best results was the one with HMDI in a 1:8 ratio (87.2 and 77.5 %, respectively). In vitro dissolution studies of encapsulated polyphenols showed that rutin and phloridzin are better dissolved in ethanol, while chlorogenic acid is better dissolved in water. Besides, TGA, DSC, FTIR and XRPD were used as characterization techniques. Individual polyphenols and nanosponges, equimolar physical mixtures and synthesized complexes were characterized. Taking into account the obtained results, it can be confirmed that the solid products were not physical mixtures, but inclusion complexes. Thus, using these encapsulating agents, other polyphenols from apple and its by-products could be encapsulated in order to enhance their bioavailability.     

pH-dependent complex formation of amino acids with β-cyclodextrin and quaternary ammonium β-cyclodextrin

Stability constants for the complexes of anionic, neutral (zwitterionic) and protonated forms of l- and d-enantiomers of eight amino acids with β-cyclodextrin and the positively charged quaternary ammonium β-cyclodextrin (QA-β-CD, DS?=?3.6?±?0.3) have been determined by spectrophotometric and pH-potentiometric methods. The highest stability constants have been obtained for the aromatic amino acids phenylalanine, tyrosine and tryptophan. Except the dianion of tyrosine and QA-β-CD, values for the anions in the range of 80–120 have been found, the stability constants for the zwitterionic forms are much smaller and complex formation is negligible with the protonated species. In the case of the other amino acids the differences are less pronounced. The results are interpreted in terms of hydrogen bonding, steric effects and electrostatic interactions between the amino acid moiety and the rims of the cyclodextrins, in addition to the inclusion of the side chain, and are supported by ¹H and ¹³C NMR investigations on the systems containing l-phenylalanine and l-tyrosine. The differences between the complex formation constants of the l- and d-enantiomers do not exceed the limits of experimental error in most cases.     

Catalytic and stoichiometric reactivity of β-silylamido agostic complex of Mo: intermediacy of a silanimine complex and applications to multicomponent coupling

The reaction of complex (ArN═)(2)Mo(PMe(3))(3) (Ar = 2,6-diisopropylphenyl) with PhSiH(3) gives the β-agostic NSi-H···M silyamido complex (ArN═)Mo(SiH(2)Ph)(PMe(3))(η(3)-ArN-SiHPh-H) (3) as the first product. 3 decomposes in the mother liquor to a mixture of hydride compounds, including complex {η(3)-SiH(Ph)-N(Ar)-SiHPh-H···}MoH(3)(PMe(3))(3) characterized by NMR. Compound 3 was obtained on preparative scale by reacting (ArN═)(2)Mo(PMe(3))(3) with 2 equiv of PhSiH(3) under N(2) purging and characterized by multinuclear NMR, IR, and X-ray diffraction. Analogous reaction of (Ar'N═)(2)Mo(PMe(3))(3) (Ar' = 2,6-dimethylphenyl) with PhSiH(3) affords the nonagostic silylamido derivative (Ar'N═)Mo(SiH(2)Ph)(PMe(3))(2)(NAr'{SiH(2)Ph}) (5) as the first product. 5 decomposes in the mother liquor to a mixture of {η(3)-PhHSi-N(Ar')-SiHPh-H···}MoH(3)(PMe(3))(3), (Ar'N═)Mo(H)(2)(PMe(3))(2)(η(2)-Ar'N═SiHPh), and other hydride species. Catalytic and stoichiometric reactivity of 3 was studied. Complex 3 undergoes exchange with its minor diastereomer 3' by an agostic bond-opening/closing mechanism. It also exchanges the classical silyl group with free silane by an associative mechanism which most likely includes dissociation of the Si-H agostic bond followed by the rate-determining silane σ-bond metathesis. However, labeling experiments suggest the possibility of an alternative (minor) pathway in this exchange including a silanimine intermediate. 3 was found to catalyze dehydrogenative coupling of silane, hydrosilylation of carbonyls and nitriles, and dehydrogenative silylation of alcohols and amines. Stoichiometric reactions of 3 with nitriles proceed via intermediate formation of η(2)-adducts (ArN═)Mo(PMe(3))(η(2)-ArN═SiHPh)(η(2)-N≡CR), followed by an unusual Si-N coupling to give (ArN═)Mo(PMe(3))(κ(2)-NAr-SiHPh-C(R)═N-). Reactions of 3 with carbonyls lead to η(2)-carbonyl adducts (ArN═)(2)Mo(O═CRR')(PMe(3)) which were independently prepared by reactions of (ArN═)(2)Mo(PMe(3))(3) with the corresponding carbonyl O═CRR'. In the case of reaction with benzaldehyde, the silanimine adduct (ArN═)Mo(PMe(3))(η(2)-ArN═SiHPh)(η(2)-O═CHPh) was observed by NMR. Reactions of complex 3 with olefins lead to products of Si(ag)-C coupling, (ArN═)Mo(Et)(PMe(3))(η(3)-NAr-SiHPh-CH═CH(2)) (17) and (ArN═)Mo(H)(PMe(3))(η(3)-NAr-SiHPh-CH═CHPh), for ethylene and styrene, respectively. The hydride complex (ArN═)Mo(H)(PMe(3))(η(3)-NAr-SiHPh-CH═CH(2)) was obtained from 17 by hydrogenation and reaction with PhSiH(3). Mechanistic studies of the latter process revealed an unusual dependence of the rate constant on phosphine concentration, which was explained by competition of two reaction pathways. Reaction of 17 with PhSiH(3) in the presence of BPh(3) leads to agostic complex (ArN═)Mo(SiH(2)Ph)(η(3)-NAr-Si(Et)Ph-H)(η(2)-CH(2)═CH(2)) (24) having the Et substituent at the agostic silicon. Mechanistic studies show that the Et group stems from hydrogenation of the vinyl substituent by silane. Reaction of 24 with PMe(3) gives the agostic complex (ArN═)Mo(SiH(2)Ph)(PMe(3))(η(3)-NAr-Si(Et)Ph-H), which slowly reacts with PhSiH(3) to furnish silylamide 3 and the hydrosilylation product PhEtSiH(2). A mechanism involving silane attack on the imido ligand was proposed to explain this transformation.     

Synthesis and complex formation ability of monomeric and dimeric amphiphilic β-cyclodextrin derivatives

Applying 6-O-monotosyl derivative of β-cyclodextrin and hexane-1,6-diamine monomeric and dimeric (bridging) amphiphilic compounds were obtained, and the opportunity was demonstrated of the preparation on their basis of inclusion compounds at the interaction with 2-(4-isobutylphenyl)propionic acid (Ibuprofen).     

Preparation, Characterization, and Bacteriostasis of AgNP-Coated β-CD Grafting Cellulose Beads

A novel functional material of β-cyclodextrin (β-CD) grafting cellulose beads containing immobilized silver nanoparticles (AgNPs) is presented in this paper. The morphology was characterized by scanning electron microscopy, energy-dispersive X-ray, and X-ray photoelectron spectroscopy. Phenolphthalein probe molecule technique was used to detect the activity of the grafting β-CD, and the results demonstrated that the deposition of AgNPs had no influence on its encapsulation ability. Acid resistance of the AgNPs on the bead material was studied by atomic absorption spectrometry. The stability of the AgNPs was enhanced due to the grafting of β-CD. Tube dilution method was applied to study the bacteriostatic effect, and the minimal inhibitory doses of the novel material against Escherichia coli and Staphylococcus aureus were 12.5 and 25 mg, respectively. The minimal bactericidal doses for the two bacteria were 25 and 25 mg, respectively.     

Thermal Stability and Decomposition Kinetics of the β-CD Cinnamic Aldehyde Inclusion Complex

The stability of the -CD cinnamic aldehyde inclusion complex wasinvestigated by TG and DSC. The weight loss takes place in three stages:dehydration occurs at 50–120 °C; the dissociationof -CDC₉H₈O occurs at 200–260 °C;and the decomposition of -CD begins at 280 °C. Thekinetics of the dissociation of cinnamic aldehyde from the -CD cavitywere studied by means of thermogravimetry both at constant temperatureand linear increasing temperature. The results show that the dissociationof -CDC9H8O is dominated by a one-dimensional diffusionprocess. The activation energy, E, is 160 kJmol-1. Thepre-exponential factor A is 5.8 × 1014 min-1.     

Selection of Amino Acids and the Biomimetic Synthesis of Amido Bond in the Presence of β-CD

A new method was developed to construct a special amido bond in the presence of β-cyclodextrin. This process is similar to peptide synthesis in organisms. NMR experiments were performed to investigate the possible mechanism. This work has potential application in biomimetic peptide synthesis.

[Supplementary materials are available for this article. Go to the publisher's online edition of Synthetic Communications® for the following free supplemental resource(s): Full experimental and spectral details.]     

Synthesis and characterization of inclusion complex of the vasodilator drug minoxidil with β-cyclodextrin

The inclusion complex of β-cyclodextrin and minoxidil (2,4-diamino-6-piperidinopyrimidine 3-oxide) was synthesized using two methods—kneading and freeze-drying—and characterized by UV-Vis spectroscopy, infrared spectroscopy, powder X-ray diffractometry, differential scanning calorimetry, thermal gravimetric analysis, and nuclear magnetic resonance spectroscopy. These techniques have demonstrated the existence of inclusion compound formation between the host and guest with a molar ratio of 1:1. The studies of solubility and the data obtained by nuclear magnetic resonance spectroscopy showed a weak interaction between the guest and the cyclodextrin molecules in solution.     

Identification and releasing characteristics of β-cyclodextrin–phenylethanoid glycosides inclusion complex

β-Cyclodextrin–phenylethanoid glycosides inclusion complex was prepared and its releasing characteristic was investigated in this study. The results, obtained from Fourier-transform infrared spectroscopy, thermogravimetric analysis, and X-ray diffraction, indicated that phenylethanoid glycosides (PG) were able to form an inclusion complex with β-cyclodextrin (β-CD). This complex exhibited different spectroscopic features, thermal stability and crystalline structure from PG. Molecular simulation results showed the benzene rings of PG incorporating into the hydrophobic cavity of β-CD during the complex formation. Furthermore, the releasing rate of the included PG in the inclusion complex was positively correlated with temperature and it was slightly higher in 0.5 % HCl solution than in water. These results suggested that the complexation technique using β-CD was a promising strategy for increasing the applications of PG in food and healthcare industries.     

The physical properties and unusual pyrolysis behaviour of a supramolecular complex of β-cyclodextrin and potassium ferrioxalate

The thermal pyrolysis behaviour of a complex of β-cyclodextrin (CD) and potassium ferrioxalate (PF) was analyzed using gas chromatography coupled to time-of-flight mass spectrometry. Two rare inorganic ions: CO(2)(2+) and O(4)(+), neither of which was found in the cases of free β-CD and PF, were synchronously observed during the decomposition of the complex. Our observations led to proposed formation mechanisms of the ions, in which the structural transformation of a metastable intermediate ion (C(2)H(4)O(3)(+)) was employed to qualitatively explain our data. Besides this, the formation, structure and magnetic properties of the complex were evaluated carefully. First, XPS analysis indicates a decrease of electron densities of Fe(III) ions in the presence of β-CD. We think that this is due to an effect of the noncovalent complexation between PF and β-CD. This gives an indication on the effect of second sphere coordination of β-CD on the electronic structure of the Fe(III) in the first coordination sphere. Second, structural changes in stacking modes and morphologies provide further support for the noncovalent complexation. For example, the surface feature of the complex gives us an impression that both β-CD and PF are evenly dispersed with each other. Also, the complex presents a uniform sponge-like porous nanostructure with diameters of less than 50 nm. This seems to be an important reason for those changes that occurred in the thermal analysis. Finally, the result of magnetic experiments implies that the coordination compound PF upon complexation with β-CD will experience a gradual decrease in magnetization with the increase of magnetic fields. These observations have significant implications for a better understanding of the importance of the construction and deconstruction of a second sphere coordination in modifying the physical properties of an σ-coordination compound.     

Synthesis and MALDI-TOF Characterization of β-CD Core ATRP Initiators and RAFT Chain Transfers with Different Degrees of Substitution

In this paper, three different kinds of β-CD derivatives were synthesized as atom transfer radical polymerization(ATRP) initiator or reversible addition-fragmentation chain transfer polymerization(RAFT) chain transfers. The degree of substitution for each derivative was carefully characterized through 1H-NMR, 13C-NMR spectroscopy and matrix-assisted laser desorption/ionization time of flight mass spectrometry(MALDI-TOF-MS). The factors influencing the degree of substitution were discussed. Moreover, the comparison between ATRP and RAFT was shown in the polymerization of Nisopropyl acrylamide(NIPAM).     

Pharmacology and structures of the free base of the anaesthetic kazcaine and its complex with β-cyclodextrin

The base form of the local anaesthetic kazcaine (BFK, [1-(2-ethoxyethyl)-4-ethynyl-4-benzoyloxypiperidine, C₁₈H₂₃NO₃]) and β-cyclodextrin (β-CD) co-crystallized as BFK:β-CD inclusion complex in 1:2 M ratio from a mixture of water and ethanol while the filtered mother liquor yielded crystals of free BFK. X-ray diffraction showed that the crystals of BFK and its inclusion complex with β-CD belong to monoclinic (P2₁/c) and triclinic (P1) space groups, respectively. The crystals of free BFK are stabilized by pairs of C–H?O, C–H?π and ≡C–H?O type interactions and van der Waals contacts. In the 1:2 BFK:β-CD complex the two β-CD molecules are in hydrogen-bonding contact with their primary hydroxyl groups, the 1-(2-ethoxyethyl)-4-ethynyl-piperidine moiety being located in one and the benzoyloxy group of BFK in the other β-CD. This crystal structure is of the channel-type, the β-CD molecules of the 1:2 BFK:β-CD complex interacting with their secondary hydroxyl groups. The pharmacological activities of the 1:2 BFK/β-CD inclusion complex have been determined in mice, rats, porpoises and rabbits and compare favourably with those of kazcaine, procaine, dicaine, lidocaine and trimecaine. The methods used include terminal (superficial), infiltration, conduction anaesthesia, and acute toxicity.     

Molecular Recognition of Immobilized Supramolecular Complex of Ironporphyrin and β-CD Polymer as an Analogue for Peroxidase

The immobilized supramolecular inclusion complex of FeTPPS4 and -CD polymer was applied as a mimesis of peroxidase, and its molecular recognition for twenty substrates was studied. As the space structure;CD interior cavities, high selectivity was obtained by immobilized mimetic enzyme. p-Chlorophenic acid was identified as an optimal substrate in the system tested.