Reduction of phytotoxicity of nonionic tensides by cyclodextrins

The effect of nonionic tenside nonylphenylnonylglycolate and its -, -, -cyclodextrin, 2,6-di-O-methyl--cyclodextrin (DIMEB) and 2,3,6-tri-O-methyl--cyclodextrin (TRIMEB) complexes was tested on the potassium influx of wheat seedling roots. Tenside alone inhibited strongly the potassium influx. This noxious effect was alleviated by cyclodextrins. The alleviating effect increased with increasing cyclodextrin: tenside molar ratio, in the order: DIMEB>CD>CD>CDTRIMEB.Presented at the Fourth Internatinal Symposium on Inclusion Phenomena and the Third International Symposium on Cyclodextrins, Lancaster, U.K., 20–25 July 1986.     

Supramolecular Polymers Formed by Modified Cyclodextrins

6-Hydrocinnamoyl -cyclodextrin(6-HyCiO--CD), 6-hydrocinnamoyl -cyclodextrin(6-HyCiO--CD), 6-cinnamoyl -cyclodextrin(6-CiO--CD), and 6-cinnamoyl -cyclodextrin (6-HyCiO--CD) have been prepared.6-HyCiO--CD formed an intramolecular complex in an aqueous solution. 6-HyCiO--CD formed weak intermolecular complexes.6-CiO--CD formed intermolecular complexes to give supramolecular oligomers. 6-CiO--CD formed insoluble supramolecular complexes in the solid state. The structures of these complexes are discussed.     

Influence of Cyclodextrins on the Kinetics of Oxidation of Amino Acids and BSA by Hydrazyl Radicals

The kinetics of oxidation of amino acids (Arg, His, Lys, Phe, Thr and Tyr), a dipeptide (Gly-His), and BSA (bovine serum albumin) by two persistent water soluble free radicals of the hydrazyl type has been studied.The rate decreases in the order Arg>Lys>Tyr>Thr>HisBSAPheGly-His with bothfree radicals. Addition to the reaction mixture of - and -cyclodextrin decreases the oxidation rate, probably due to amino acidencapsulation in the cyclodextrin cavity. -Cyclodextrin protects more efficiently against oxidation than -cyclodextrin.     

In vitro nitrosation of ephedrine in the presence of cyclodextrins

-, and -cyclodextrin and heptakis-2,6-di-O-methyl--cyclodextrin enhance the nitrosation rate of l-ephedrine if the nitrosation assay procedure (NAP test) is applied. During this reaction with -cyclodextrin a solid inclusion compound of -cyclodextrin andN-nitrosoephedrine precipitates. Solubilities and stabilities of inclusion compounds of the cyclodextrins with ephedrine and nitrosoephedrine, respectively, explain especially the catalytic effects of some cyclodextrins on ephedrine.Part of the PhD thesis of V. Wedelich, Freie Universität Berlin, 1985.     

Inclusion complexing by water-soluble β-cyclodextrin polymers

Cross-linked -cyclodextrin with a molecular weight of less than 10000 has good solubility in water, and it is a better inclusion complexing agent than the parent -cyclodextrin. By including lipophilic guest molecules into the apolar cyclodextrin cavity, their apparent lipophilicity is reduced because the outer surface of the molecular wrapping (the crosslinked -CD) is highly hydrophilic. The relative stability of the inclusion complexes can be rapidly determined by reversed-phase thin-layer chromatography. The reversed-phase TLC behaviour of 25 triphenylmethane derivatives and analogues were studied in the presence of -cyclodextrin polymers containing neutral and carboxyl groups. Increasing the molecular weight results in an increased complex-forming capacity. The carboxyl group modifies the accessibility of the CD cavity which in turn results in increased or decreased complex stability, depending on the guest molecule. The presence of organic solvents diminishes the stability of the CD complexes.     

The Effects of Cyclodextrins on Hydrocortisone Permeability Through Semi-Permeable Membranes

Determinations of drug fluxes through semi-permeable cellophanemembranes are used to evaluate cyclodextrin complexes and cyclodextrin containingdrug formulations. In the present study we investigated how the cyclodextrin concentration,the membrane thickness and the molecular weight cut off (MWCO) of the membraneinfluence drug fluxes. The cyclodextrin used was 2-hydroxypropyl--cyclodextrin(HP--CD) and the sample drug was hydrocortisone. The MWCO ofthe membranes ranged from 500 to 14,000 and the HP--CD concentrationranged from 0 to 25% (w/v). The hydrocortisone flux from saturated solutions through the MWCO 500 membrane was unaffected by the cyclodextrin concentration. When MWCO of the membrane was greater than the molecular weight of the complex the flux fromsolutions saturated with hydrocortisone increased with increasing HP--CD concentration.This increase showed negative deviation from linearity. When the flux was correctedfor the viscosity increase with increasing HP--CD concentration then the fluxpattern could be described on the basis of Fick's first law and Stokes–Einsteinequation. However the flux did not correlate with the viscosity when it was increasedby adding polymer to the saturated drug solutions. It was shown that the observed fluxpattern was consistent with self-association of cyclodextrin complexes in the aqueousdonor phase.     

Complexation of the Non-steroidal Anti-inflammatory Drug Nabumetone with Modified and Unmodified Cyclodextrins

The inclusion of the anti-inflammatory drug, Nabumetone, in -, - and hydroxypropyl--cyclodextrin (CDs) is studied using UV-VIS absorption and steady-state fluorescence emission. Binding constants and thermodynamic parameters of complex formation are determined by spectrofluorimetry. The inclusion phenomena of Nabumetone with the three cyclodextrins is compared with that of the well known similar anti-inflammatory drug Naproxen. In the case of Nabumetone pronounced differences are observed in the complexation process with each cyclodextrin whereas the respective Naproxen complexes are nearly identical. ¹H-NMR experiments show that the inclusion process in Nabumetone can occur either through the substituents in the -2 (butanone) or -6 (methoxy) positions in the naphthalene ring.     

Some Pharmaceutical Properties of a New Branched Cyclodextrin, 6-O-α-(4-O- α-D-Glucuronyl)-D-glucosylβ-cyclodextrin

Some physicochemical and biological properties of a new branched cyclodextrin, 6-O--(4-O--d-glucuronyl)-d-glucosyl--cyclodextrin GUG--CyD) were investigated. Further, theinteraction of GUG--CyD with several drugs was studied by the solubility and spectroscopic methods, and compared with those of parent -CyD and 6-O--maltosyl--CyD(₂--CyD).The hemolytic activity of GUG--CyD on rabbit erythrocytes was lower than those of -CyD and ₂--CyD. GUG--CyD and ₂--CyD showed negligible cytotoxicity on Caco-2 cells up to at least 0.1 M. The inclusion ability of GUG--CyD to neutral and acidic drugs was comparable to or slightly smaller than those of -CyD and ₂--CyD, probably because of a steric hindrance of the branched sugar. On the other hand, GUG--CyD showed greater affinity for the basic drugs, compared with -CyD and ₂--CyD, owing to the electrostatic interaction of its carboxylate anion with positive charge of basic drugs. Thus GUG--CyD may be useful as a safe solubilizing agent particularly for basic drugs.     

Thermal Behaviour of Anhydrous α-, β- and γ-Cyclodextrin at Low Temperature

Heat capacities of anhydrous -and -cyclodextrin were measured by adiabaticcalorimetry between 10 K and 300 K. The thermalbehaviour of the two compounds exhibits significantdifferences. -Cyclodextrin shows an anomalousexcess heat capacity in the entire region between 70 Kand 210 K. In the case of -cyclodextrin, anendothermic effect is observed at 240K. This effect isanalysed through the study of the correspondingentropy change and discussed in terms ofintramolecular organization.Using the known heat capacity values of anhydrous-CD, a comparative analysis has been developed.For each cyclodextrin, the average behaviour of abound -D-glucopyranose has been calculated andcompared. From a thermodynamic point of view, thedegree of organization of the dehydrated macrocycliccompounds could be expressed as-CD -CD -CD.     

Solubility Study of Nimodipine Inclusion Complexation with α- and β-Cyclodextrin and some Substituted Cyclodextrins

The solubility of nimodipine was measured in aqueous solutions of the following cyclodextrins: -cyclodextrin (-CD), hydroxypropyl--CD (HP--CD), -cyclodextrin (-CD), random substituted methyl--CD (M--CD), three hydroxypropyl--CDs (HP--CD) with mutually different average degree of substitution, and hydroxypropyl--cyclodextrin (HP--CD). From the determined linear solubility diagrams the values of the binding constant K₁₁ of the inclusion complexes of nimodipine with the respective CDs were evaluated. The -CDs efficiently solubilized sparingly soluble nimodipine, the highest value of K₁₁ was found for M--CD (1680 M^-1), followed by -CD (550 M^-1) and HP--CDs, where the higher degree of substitution lowered K₁₁. Only slight solubilization of nimodipine was observed in the solutions of the -CDs and HP--CD.     

Interactions of amphiphilic drugs withα-,β-, andγ-cyclodextrins

The association of several amphiphilic drugs with -, -, and -cyclodextrins has been measured by use of drug-sensitive electrodes. Drugs investigated are hydrochlorides of chlorpromazine, dibucaine, tetracaine, and procaine, and valethamate bromide. Each drug forms the drug:cyclodextrin=11 complex with - and -cyclodextrin, and both the 11 and 21 complex with -cyclodextrin, except valethamate which only forms the 11 complex. The strength of the 11 complex formations is in the order of CyD>-CyD>-CyD. The association constant of the 21 complex in drug--CyD is larger than that of 11 complex. The free energy change of the conplex formation has a positive correlation with that of the micelle formation of drugs. The deviation from this relation is explained in terms of fittability of the bulky hydrophobic group of drugs into the cyclodextrin's cavity. The free energy change for the complex formation between chlopromazine or valethamate and -CyD is governed by the enthalpy term and not by the entropy term which controls the surfactant--CyD interactions.     

Investigation on the Interaction of Bendazac with β-, Hydroxypropyl-β-, and γ-, yclodextrins

The interactions of Bendazac, a topical non-steroidal anti-inflammatory drug, with-cyclodextrin, hydroxypropyl--cyclodextrin and -cyclodextrinwere investigated to evaluate possibilities to improve the drug's poor water solubilityand eventually to enhance the topical delivery of Bendazac. Phase solubility studiesdemonstrated the ability of the selected cyclodextrins to complex with Bendazac andincrease drug solubility. The amount of solubilized Bendazac increased linearly withthe addition of each cyclodextrin according toA_L type plots. ¹³C-NMR studiesshowed that the Bendazac A-ring was included in the cavity of the three cyclodextrins.The -cyclodextrin was also able to include the B-ring of Bendazac, forminga complex where one drug molecule fitted into two cyclodextrin molecules. Equimolarsolid systems of the drug with each cyclodextrin carrier were prepared using varioustechniques (physical mixing, spray-drying and freeze-drying). The results of differential scanning calorimetry and Fourier transform infrared analysis, performed on the solid systems, demonstrated that freeze-dried and spray-dried products had a high degree of amorphization and agreed with the hypothesis of the existence of drug–cyclodextrin interaction in the solid state. The cyclodextrins tested were able to improve the dissolution of Bendazac. The dissolution profile of the drug was also affected by the physico-chemical properties of each solid system, the freeze-dried products being the most rapidly dissolving forms.     

Crystal packing patterns of cyclodextrin inclusion complexes

Cyclodextrin inclusion complexes crystallize in two basically different patterns, the cage and the channel type. The cage type occurs when cyclodextrins are packed crosswise (fishbone) or, if they are packed side-by-side, in layers and adjacent layers are displaced by about one half molecule. In each case, the internal cavity of one cyclodextrin is closed on both sides by neighbouring cyclodextrins. On the other hand, channel complexes are formed if cyclodextrins are stacked like coins in a roll so that cavities line up to produce long channels. In these crystal structures, cyclodextrins can be arranged in head-to-head or head-to-tail mode. In the smaller -cyclodextrin, cage type structures are formed with small, molecular guests whereas long molecular guests and ionic guest molecules induce channel type structures. The latter are generally preferred with the - and -cyclodextrin series which is probably due to the higher tendency for self aggregation in these two members of the cyclodextrin family.Part XXII of the series Topography of Cyclodextrin Inclusion Complexes. For part XXI, see ref. 6.     

Asymmetric Solid–Gas Hydrohalogenation of Unfunctionalized Olefins via Formation of Crystalline Cyclodextrin Complexes

Asymmetric solid–gas hydrohalogenation of styrene, -methylstyrene,allylbenzene, and 2-norbornene as unfunctionalized olefins was carried out by using theirchiral crystalline - and -cyclodextrin complexes by exposing them to gaseous HCl and HBrin the dark at room temperature. The optical purities of the Markovnikov products obtainedfrom the ionic addition of HCl to the included olefins appear considerably higher than thosefrom the reaction with HBr. The highest enantioselectivities of 58% and 62% enantiomericexcess (ee) were obtained for the hydrochlorination of 3-phenyl-1-propene (allylbenzene) inthe crystalline - and -cyclodextrin complexes, respectively, and both reactions, which hadlittle danger of racemization, gave (S)-(+)-2-chloro-1-phenylpropane as the same predominantproduct in moderate chemical yields. A much lower enantioselectivity (<10% ee) wasobserved in the hydrobromination of the same olefin in the solid - and -cyclodextrincomplexes involving a racemization reaction. The enantiofacial selection provided the (S)-enantiomer similarly during hydrochlorination.     

Prolonged release of drug from triacetyl-β-CyD complex for oral and rectal administration

Triacetyl--cyclodextrin (TA--CyD), a hydrophobic cyclodextrin derivative, that is insoluble in water, was used to form a complex with flufenamic acid (FA). FA-TA--CyD complex formation was demonstrated by differential scanning calorimetry and powder X-ray diffractometry. The release rate of FA from the FA-TA--CyD complexes in phosphate buffer pH 6.8 was significantly retarded compared to that of FA from the FA and glucose mixture. When the FA-TA--CyD complexes were administered directly into the intraduodenal lumen, the plasma concentration of FA remained at a plateau level (10-18 g/ml) for 6–8 h. An increased mean residence time of FA following FA-TA--CyD complexes administration was observed. These results indicate that TA--CyD may serve as a hydrophobic carrier in prolonged-release preparations of FA.     

Studies on Water-soluble α-, β- or γ-Cyclodextrin Prepolymer Inclusion Complexes with C60

Treatment of water-soluble -,- and -cyclodextrin-epichlorohydrin prepolymer (CDP) with C60 by kneading leads to the formation of six distinct water-soluble inclusion complexes: -CDP/C60 (1 : 1), -CDP/C60 (1 : 1), -CDP/C60 (1 : 1), -CDP(2 : 1), -CDP(2 : 1) and -CDP(2 : 1). Their formation and structures have been examined by X-ray powder diffraction (XRD), differential scanning calorimeter (DSC) and UV-vis spectrosocopy. The effect of side chains of the CDPs has also been studied.     

Influence of cyclodextrins on nitrosation of drugs

The World Health Organization issued a nitrosation procedure (NAP Test) which allows to carry out nitrosation under standard conditions. It has proved that the in vitro reaction rates of the fast nitrosatable drugs piperazine, cimetidine and ethambutol are not influenced by -, - and -cyclodextrin. On the contrary, -, -cyclodextrin and heptakis-2,6-di-O-methyl--cyclodextrin enhance the nitrosation of the slower nitrosatable 1-ephedrine and fencamfamine significantly. This possible reaction must be considered if nitrosatable drugs are formulated with cyclodextrins to be administered to human beings.     

Monomolecular films of pluronic-cyclodextrin inclusion complexes at the water-gas interface

This paper reports the synthesis and characteristics of inclusion type complexes between amphiphilic block copolymer of ethylene and propylene oxides (pluronic) and -, -, and heptakis-(2,6-di-O-methyl)--cyclodextrins. The process was investigated in monolayers at the water-gas interface according to Langmuir-Blodgett technique. Pluronic forms a monolayer, stable at the surface pressure 5 mN/m, which reacts with heptakis-(2,6-di-O-methyl)--cyclodextrin and does not react with - and -cyclodextrins. The absence of the reaction in the case of -cyclodextrin is explained by the fact that the polymer guest does not fit into a small cavity of the macrocyclic host, but for -cyclodextrin it may be explained by its low surface activity and, hence, its low local concentration in the vicinity of the pluronic monolayer. After introducing heptakis-(2,6-di-O-methyl)--cyclodextrin into the aqueous subphase under the pluronic monolayer an instant increase in the area is observed. An increase in the amount of heptakis-(2,6-di-O-methyl)--cyclodextrin in the aqueous phase causes first steep linear increase in the monolayer area, then its leveling off at the polymer-heptakis-(2,6-di-O-methyl)--cyclodextrin ratio equal to about 1:15. This value correlates well with a stoichiometric composition of the similar complex in solution.     

Molecular Recognition Studies on Supramolecular Systems. Part 38. Inclusion Complexation of Organic Dyes by Organoselenium Bridged Bis(β-cyclodextrin)s with a Short Linker

In order to further explore the inclusion complexation behavior with -cyclodextrin dimers, the binding constants (K_S) of three organoselenium bridged bis(-cyclodextrin)s (2ndash;4) tethered with a short linker were determined with some representative dye molecules in aqueous phosphate buffer solution (pH 7.20) at 25 °C by fluorescence and UV-vis spectrometry. As compared with the parent -cyclodextrin (1), the bridged bis(-cyclodextrin)s (2ndash;4) can not only significantly enhance the original binding affinity of the parent -cyclodextrin by the cooperative binding of one guest molecule in the closely located two -cyclodextrin cavities but also remarkably extend its molecular recognition abilities towards the different size/shape or substituent of model substrates. The higher binding ability and selectivity of dye molecules by bridged bis(-cyclodextrin)s (2ndash;4) are discussed from the viewpointof the size/shape-fit concept and multiple recognition mechanism.     

Formation of Supramolecular Polymers Constructed by Cyclodextrins with Cinnamamide

-Cyclodextrin having cinnamamide at 6- or 3-positions (6-CiNH--CD, 3-CiNH--CD) and -cyclodextrin with cinnamamide on 6-position (6-CiNH--CD) have been prepared. Supramolecular structures were formed in the solid state or aqueous solutions and characterized by measurements of NMR and vapor pressure osmometry (VPO). The results indicate that 6-CiNH--CD formed insoluble supramolecular polymers in the solid state, while 6-CiNH--CD and 3-CiNH--CD formed supramolecular complexes in aqueous solutions. 6-CiNH--CD was found to form a dimer in an aqueous solution. 3-CiNH--CD formed intermolecular complexes to give supramolecular polymers. The differences of the position of guest part on cyclodextrins caused to give a variety of supramolecular structures in aqueous solutions.