Improvement in biopharmaceutics of prednisolone by β- and γ-cyclodextrins

Inclusion complexes of prednisolone with - and -cyclodextrins in the molar ratio of 1:2 and 2:3, respectively, were prepared, and their dissolutions, permeations through a cellophane membrane, releases from a suppository base, andin vivo absorption behaviors were examined. The apparent rates of dissolution and permeation of prednisolone were significantly increased by the formations of inclusion complexes with - and -cyclodextrins. The release of the drug from Witepsol H₁₅ suppositories was also increased by complexation. The serum levels of prednisolone following oral and rectal administrations of the cyclodextrin complexes to rabbits were higher than those of the drug alone. The enhanced initial absorption of prednisolone by cyclodextrin complexation suggested the possibility of smaller doses in prednisolone therapy.     

Behavior of rifampicin in association with<Emphasis Type="Italic"> β</Emphasis>-cyclodextrin in aqueous media: a spectroscopic and conductometric study

The behavior of rifampicin (D) with -cyclodextrin (-CyD) in aqueous media (W) has been examined by means of UV-vis spectroscopy and conductivity measurements over the temperature range 15–30 °C. The UV-vis study has been used to characterize the systems. The estimated molar absorption coefficient for D/CyD/W system was 10757±280 M^–1 cm^–1 in comparison to the value of 6133±99 M^–1 cm^–1 for D/W system. The conductivity was measured (i) as a function of [D] for binary D/W systems, (ii) as a function of [CyD], keeping the concentration of drug constant, for D/CyD/W system, and (iii) as a function of [D] in the presence of a constant cyclodextrin concentration. Two transition points were observed for D/CyD/W system at constant [CyD], which were assigned as cac-1 and cac-2. The stoichiometry of the association was estimated from the conductivity data. This was obtained from [drug] value at which the change in slope of occurs. The standard free energy change, of aggregation was also calculated from the critical concentration data. An attempt has also been made to estimate the stoichiometry of -cyclodextrin:rifampicin association.     

Trans-cis Photoisomerization of 1-Methyl-4-(4′-hydroxystyryl)pyridinium in inclusion complexes ofβ-cyclodextrin and its derivatives

The effects of -cyclodextrin (-CyD), heptakis(2,6-di-O-methyl)--cyclodextrin (DMCyD) and heptakis(2,3,6-tri-O-methyl)--cyclodextrin (TMCyD) ontrans-cis photoisomerization of 1-ethyl-4-(4-hydroxystyryl)pyridinium (POH) have been studied in aqueous solutions. The ratio of [cis]/[trans] for POH in the photostationary state at pH 8.54 was remarkably reduced by the presence of CyD or DMCyD. The reduction of the [cis]/[trans] ratio in the photostationary state was explained in terms of the shift of the equilibrium of POH ₊ ^trans PO _trans + H^– toward PO _trans formation. The binding constants of CyD and DMCyD for PO _trans were 2.00- and 1.36-fold larger than those for POH ₊ ^trans , respectively. The binding constants of TMCyD for both species are much smaller than those of CyD and DMCyD. This result indicates that PO _trans , which has a betain structure, forms stable complexes with CyD and DMCyD with its hydrophobic parts inside and the charged parts outside the CyD cavities.     

Diastereomeric Difference of the Self-Inclusion Complex of N(N′-Formyl-Phenylalanyl)-Deoxyamino-β-Cyclodextrin Caused by the Interaction between the Arm and the Rim of the Cavity

A complete assignment of proton resonances for N(N-formyl d-phenylalanyl)-deoxyamino--cyclodextrin (1d) was performed by means of 1D and 2D NMR,¹H–^1H-COSY, ¹H–^13C-COSY, TOCSYand NOESY spectroscopy. Based on 2D-NMR ROESY and circular dichroism spectroscopy, the conformation of 1d was determined; the phenyl group stays inside the distorted cyclodextrin (CyD) cavity forming a self-inclusion complex, which is almost the same as N(N-formyl l-phenylalanyl)-deoxyamino--CyD (1l). The remarkable diastereomeric difference was observed in the chemical shifts of H(5) and H(6) protons at the narrow rim of the CyD cavity and induced circular dichroism spectra. These results suggest the existence of hydrogen bonds between the hydroxyl group on CyD and the amide groups on the arms, which provides the difference in the molecular recognition properties.     

Membrane-introduction mass spectrometry (MIMS)

Membrane-introduction mass spectrometry (MIMS) for chemical analysis involves directly sampling analytes in gaseous, liquid and solid samples through a semi-permeable membrane coupled to a mass spectrometer, yielding selective and sensitive quantitation. Because MIMS is an on-line technique, in which samples can be continuously flowed over a membrane interface, it can yield analytical results in real time without the need for sample clean-up and chromatographic separation. This review highlights trends and developments in MIMS over the past decade and describes recent studies that pertain to its use for on-site, in-situ and in-vivo chemical analysis. We report on advancements in instrumentation, including membrane materials, interface configurations and ionization techniques that have extended the range of analytes amenable to MIMS.We summarize the progress made in the miniaturization of mass spectrometers that have resulted in field-portable systems and review recent applications of continuous mobile monitoring and on-site environmental monitoring to yield both temporally and spatially resolved quantitative and semi-quantitative data. Finally, we describe recent work involving the use of MIMS for in-vivo chemical analysis.     

Inclusion Complexation of a Seleno-Organic Antioxidant, Ebselen, with Cyclodextrins in Aqueous Solution

The interaction of ebselen, 2-phenyl-1,2-benzisoselenazol-3(2H)-one, a novel neuroprotective agent, with cyclodextrins (CyDs) in aqueous solution was studied by the solubility method and spectroscopic methods. The ability of sulfobutyl ether -CyD (SBE7--CyD, average degree of substitution= 6.2) to solubilize ebselen was greater, and its stability constant (> 2000 M^-1) was significantly higher than those (< 1000 M^-1) of other CyD complexes employed. The stability constant of the complexes rose as hydrophobicity of the substituents of CyDs increased, whereas it was negligibly affected by change in ionic strength of the medium, indicating a significant contribution of hydrophobic interaction in the complexation. SBE7--CyD gave positive and negative CD bands at around 320 and 350 nm, respectively, indicating that the guest is embedded in the asymmetric locus of the CyD cavity. ¹H-NMR spectroscopic studies suggested that the mono-substituted benzene ring of ebselen is preferably included in the cavity of SBE7--CyD. The results indicate that SBE7--CyD is useful as a solubilizing agent for ebselen.     

Direct potentiometry and potentiotitrimetry of warfarin and ibuprofen in pharmaceutical preparations using PVC ferroin-based membrane sensors

Sensitive and fast-responding potentiometric sensors are described for the determination of warfarin and ibuprofen. They consist of PVC matrix membranes containing the drag-ferroin ion-association complexes as electroactive materials and dioctylphthalate as a solvent mediator. Linear dynamic response range between 1 × 10^–2 and 2 × 10^–5 M with Nernstian slopes of 59–60 mV/decade concentration and a detection limit of 0.8–1.3 g/ml are obtained. A wide range of organic anions and drag excipients do not interfere. Titration of the drugs with a standard ferroin solution using either a drag-ferroin or ferroin-TPB PVC sensor in conjunction with an Ag-AgCl reference electrode displaysS-shaped titration curves with sharp potential breaks at stoichiometric 12 (ferroin:drug) reaction. Differential titration curves with well-defined peaks at the equivalence points are obtained using drug-ferroin/ferroin-TPB PVC membrane sensors. Direct potentiometry and potentiotitrimetry of warfarin and ibuprofen in various pharmaceutical preparations are presented and compared. Several advantages over the pharmacopoeial methods and other techniques in current use are offered by the proposed technique.     

Inclusion Complexation of the Sunscreen 2-Hydroxy-4-Methoxy Benzophenone (Oxybenzone) with Hydroxypropyl-β-Cyclodextrin: Effect on Membrane Diffusion

It is desirable to minimize skin penetration of some drugs, such as sunscreens and insect repellents. Available in vivo and in vitro data suggest appreciable absorption of some sunscreen agents. The purpose of this study was to investigate the effect of hydroxypropyl--cyclodextrin (HPCD) on the release and permeation of the sunscreen agent 2-hydroxy-4-methoxy benzophenone (oxybenzone). The interaction between oxybenzone and HPCD was studied in water by phase solubility analysis. The inclusion complex was characterized by thermal analysis and nuclear magnetic resonance spectroscopy. UV transmittance and percent UVA transmittance, as a preliminary measure of sun protection factor (SPF), were determined. In vitro permeation experiments were conducted in Franz-type diffusion cells at 37 °C, using the model membrane poly(dimethyl siloxane) (PDMS) and 4% bovine serum albumin in phosphate buffer solution (pH 7.4) as the receptor phase. HPCD caused a marked increase in the aqueous solubility of oxybenzone. Data from the phase solubility experiment indicated the formation of 1:1 oxybenzone-cyclodextrin complex. UV transmittance studies indicated that the presence of HPCD did not suppress the UV absorbing properties of oxybenzone. The release and membrane permeation of oxybenzone was significantly reduced in the presence of equimolar, 2 times molar and 1, 2 and 4% of HPCD. It is concluded that HPCD can reduce the release/membrane diffusion of oxybenzone whilst retaining its efficacy as a sunscreen agent. This formulation strategy may be useful in controlling skin penetration of topically applied sunscreens and other chemicals.     

In-vivo and in-vitro testing to assess the bioaccessibility and the bioavailability of arsenic, selenium and mercury species in food samples

In-vivo and in-vitro gastrointestinal (GI) extractions, also known as oral bioaccessibility and bioavailability, are important approaches to assess chemical risk to humans. We give an overview of in-vivo and in-vitro bioaccessibility and bioavailability assays for testing arsenic, selenium and mercury (As, Se and Hg) species from food samples. We critically evaluate the parameters affecting in-vivo and in-vitro processes. In addition, we consider the effect of cooking food on bioaccessibility and bioavailability, and stability and transformation, of species during in-vivo or in-vitro processes. The bioaccessibility and bioavailability of As, Se and Hg species are affected by the sample matrix, cooking food and the experimental conditions applied (gastric and intestinal pH, incubation temperature and residence time). Regarding species degradation and transformation during in-vitro procedures, good stability has been observed for most As species, except for certain arsenosugars. Important transformations during in-vitro processes have been reported for Se species [e.g., conversion of γ-glu-Se-MeSeCys to Se-MeSeCys, and organic Se species (MeSeCys, SeCys2 and SeMet) degradation to inorganic Se]. Finally, we summarize speciation and detection conditions for As, Se and Hg speciation, and quality control to assure reliable measurements.     

Plastic membrane electrodes for the potentiometric determination of codeine in pharmaceutical preparations

Four PVC membrane electrode systems responsive to codeinium cation are described. These electrodes are based on the use of the ion-association complexes of the codeinium cation with tetraphenylborate and reineckate counter-anions as ion-exchange sites in a PVC matrix plasticized with dioctylphthalate and dibutylsebacate. The performance characteristics of these electrodes reveal fast, stable and near-Nernstian responses for codeine down to concentrations of 3.5–7.0 × 10^–5 M. Over the pH range 2.5–7, the electrodes are satisfactory for manual and flow injection determination of codeine in various pharmaceutical preparations. There is negligible interference from a number of inorganic and organic cations and some common drug excipients. In the direct determination of 30 g/ml -1.0 mg/ml codeine, the average recovery is 100.6% and the mean standard deviation is ± 0.8%. The results compare favorably with those obtained by the British Pharmacopoeia method.     

Fish Skin as a Model Membrane to Study Transmembrane Drug Delivery with Cyclodextrins

The possibility of using fish skin as model membrane tostudy drug permeation and penetration enhancement by cyclodextrins was investigated.The permeability of the skin from four species of fish, Anarhichas lupus (catfish),Pleuronectes platessa (Plaice), Hippoglossus hippoglossus (Halibut)and Anarhichas minor (Spotted catfish), was compared in a Franz diffusion cell set-up using 1% hydrocortisone aqueous solution as a donor phase. The drug fluxthrough fish skin was more than 100 times faster than the flux through hairless mouse skin and more than 10 000 times faster than through snake skin. Catfishskin was most easily accessible and was therefore used for further study. The octanol-water partition coefficient did not affect the transmembrane flux of small molecules whereas the aqueous diffusion coefficient could be correlated with the flux.The hydrocortisone flux of from aqueous hydroxypropyl--cyclodextrin solutions, which were saturated with the drug, increased with increasing cyclodextrinconcentration. From these and other observations it was concluded that small moleculesare transported through fish skin in aqueous channels. The properties of thesechannels resemble the properties of the aqueous diffusion layer present in human andanimal skin and other types of biological membranes. Previous studies have shown thatcyclodextrins will enhance drug delivery by increasing aqueous diffusion rate. Catfish skin can therefore be a good model membrane to study penetration enhancementby cyclodextrins.     

Electrochemical studies of cationic drug inclusion complexes with α- andβ-cyclodextrins

Drug membrane selective electrodes have been constructed for the cationic drug propranolol hydrochloride, diphenhydramine hydrochloride, diphenylpyraline hydrochloride and also chlorcyclizine hydrochloride. The characteristics of these drug selective electrodes have been evaluated and the electrodes used to measure equilibrium constants of the inclusion compounds involving the drugs with both - and-cyclodextrins. The enthalpies and entropies associated with the formation of the inclusion complexes have also been estimated from the temperature dependence of the equilibrium constants.     

Rapid analysis of NSAIDs binding to β-cyclodextrin using the simultaneous measurement of absorption and circular dichroism with a novel multi-cell low-volume device

One of the relatively recent and most widely used approaches to reduce side effects associated with the use of nonsteroidal anti-inflammatory drugs (NSAIDs) is the complexation of NSAIDs with Cyclodextrins (CyD). So far, CyD interaction with drugs is not well understood. There have been many reports along these lines; however, rarely do these studies exploit the full potential of optical techniques. The purpose of this work is to produce a versatile, compact, low-volume, routine apparatus for the simultaneous measurements of absorbance and circular dichroism (CD) which allows for the concurrent use of three different pathlengths for binding studies of NSAIDs/CyD as a function of pH. A new rotating multi-cell holder which holds four cells was designed and manufactured. The work was achieved using an effective novel method for binding titration employing four separate flow cells connected in series in a flow system involving a titration flask and a pump. The pK _a, binding constants, stoichiometry and structural co-conformations of NSAIDs/β-CyD complexes were elucidated and determined with accuracy. The system proved to be efficient and the analysis time was reduced to less than or equal to one fourth of total analysis time used in one-cell systems, with possible automation for high-throughput analysis.

ESR spectroscopy of copper(ii) complexes with aza- and thia-containing crown ethers

Six copper(ii) chloride complexes with crown ethers containing besides oxygen also nitrogen or sulfur atoms in 15- or 18-membered cycle were studied by ESR and electron absorption spectroscopies. Theg and HFI tensor components determined by spectral simulation indicate rhombic symmetry and localization of an unpaired electron on the d _xy orbital for all the complexes. The unpaired electron fractions on - and -type metal ion and ligand AO were estimated from ESR and absorption spectra using LCAO MO method. Both - and -type bond covalences were shown to be greater in these complexes compared to only oxygen-containing crown ether complexes. The temperature dependence of g and A components in some complexes may be due to conformational changes.Translated fromIzvestiya Akademii Nauk. Seriya Khimicheskaya, No. 11, pp. 1938–1944, November, 1994.The present work was carried out with financial support from the Russian Foundation for Basic Research (Project 93-03 04089).     

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.     

Circular dichroic investigation of factors that affect inclusion complexes of cyclodextrins as a drug carrier

Drug/cyclodextrin (CyD) inclusion complexes have become one of the most widely used approaches to increase aqueous solubility of poorly soluble drugs, to increase their bioavailability and stability, to reduce undesirable side effects and prevent drug–drug and drug–excipient interactions. Although drug molecules as well as CyDs exhibit detectable changes in their physicochemical properties upon complexation, to date, the interaction of CyDs with drugs is not well understood. So far, only few methods can be applied to obtain structural information on drug/CyD complexes. Circular dichroism spectroscopy (CD) has often been used to study molecular binding, nevertheless, rarely do these studies exploit the full potential of optical techniques. The objective of this article is to highlight important factors that affect drug/CyD binding interaction in particular β-CyD. On the basis of chirality, (S)-(+)-ibuprofen, meta-chlorobenzoic acid and aspirin were used to study binding interaction with β-CyD using CD. Based on CD equations for a simple 1:1 binding complex, the Levenberg–Marquadt non-linear equation was used for binding analysis and the production of simulated graphical presentations to explain the effect of various factors that influence the binding reaction and the binding curve. The results show reliability indicated by the binding constant which is in agreement with literature values. In addition, the effect of guest/host concentrations and the extent of binding on the inclusion complexes are elucidated with accuracy. This work provides useful information that can prove valuable in drug binding studies.     

Effect of 2-Hydroxypropyl-β-cyclodextrin on Release Rate of Metoprolol from Ternary Metoprolol/2-hydroxypropyl-β-cyclodextrin/Ethylcellulose Tablets

The effect of 2-hydroxypropyl--cyclodextrin (HP--CyD) on the release of a water-soluble ₁-selective adrenoreceptor antagonist, metoprolol (Met), from ternary Met/HP--CyD/ethylcellulose (EC) tablets was investigated. The release rate of Met from the ternary tablets was dependent on amounts of HP--CyD in the tablets, i.e., the rate decreased when small amounts of HP--CyD were added, while large amounts of HP--CyD accelerated the rate. The slowest rate was observed for the tablet consisted of a 30/10/60 weight ratio of Met/HP--CyD/EC. The analyses of the release rates by the Korsmeyer equation and their temperature dependence suggested that Met is released from the EC matrix containing HP--CyD according to the diffusion-controlled mechanism. The water penetration studies and the micro- and macroscopic observations suggested that the retarding effect of HP--CyD is attributable to a viscous gel formation in small pores on the surface of the tablets, where HP--CyD gels may work as a barrier for the water penetration into the tablets and the release of the drug from the tablets. The in-vitro release property of the ternary tablets was reflected in the in-vivo absorption profile in dogs. The results indicated that a combination of HP--CyD and EC is useful for the release control of water-soluble drugs such as Met.     

The in vitro Pulmonary Deposition of a Budesonide γ-Cyclodextrin Inclusion Complex

The interest in dry powder inhalers (DPIs) has recently increasedbecause the problems associated with the propellants used in pressurized metered-dose inhalers (PMDIs) will be avoided. Cyclodextrins (CDs) may be used as excipients in inhalation powders;e.g., in order to increase the solubility, stability and absorption of an inhaled drug. In thepresent study, the effect of complexation of budesonide with -CD on its pulmonary deposition wasstudied in vitro. In the presence of -CD, the aqueous solubility of budesonidefollowed B_S-type phase-solubility behaviour. A precipitationcomplexation method was used to prepare the solid budenoside/-CD complexes. The pulmonary in vitrodeposition of budenoside was evaluated after inhalation of plain budesonide and budenoside/-CDcomplexes (lactose carrier used in both formulations) by using the ``Andersen' cascadeimpactor. The novel Taifun® was used as the DPI. The respirable fractionsof the emitted budesonide dose (initially and after the storage in 40 °C, RH 75%) werecomparable for both plain budesonide and budesonide/-CD complexes. The present studyindicates that a drug/CD-complex can be used in inhalation powderswithout lowering the pulmonary deposition of the drug.     

Model calculations on LIS,III. A simple force field model for Ln(III)-shift-reagent—Substrate complexes, 1. Carbinols

A force field type of calculation (FFLIS model, force field aided LIS calculation) is presented allowing to predict the lanthanide(III) positionand the relative LIS values for carbinol—Ln(III) complexes.II.:O. Hofer, Mh. Chem.110, 745 (1979).     

Analysis of the phase solubility diagram of a phenacetin/competitor/beta-cyclodextrin ternary system, involving competitive inclusion complexation

The competitive inclusion complexations in the ternary phenacetin/competitors/beta-cyclodextrin (beta-CyD) systems were investigated by the solubility method, where m-bromobenzoic acid (m-BBA) and o-toluic acid (o-TA) were used as competitors. The solubility changes of the drug and competitors as a function of beta-CyD concentration in the ternary systems were formulated using their stability constants and intrinsic solubilities. The decrease in solubility of phenacetin by the addition of competitors could be quantitatively simulated by the formulation, when both drug and competitor give A(L) type solubility diagrams. On the other hand, when one of the guests gives a B(S) type solubility diagram, its solubility change was clearly reflected in that of the another guest, i.e., phenacetin gave an A(L) type solubility diagram in the binary phenacetin/beta-CyD system and o-TA gave a B(S) type diagram in the binary o-TA/beta-CyD system, but in the ternary phenacetin/o-TA/beta-CyD system, a new plateau region appeared in the original A(L) type diagram of phenacetin. This was explained by the solubilization theory of Higuchi and Connors. The solubility analysis of the ternary drug/competitor/CyD systems may be particularly useful for determination of the stability constant of a drug whose physicochemical and spectroscopic analyses are difficult, because they can be calculated by monitoring the solubility change of a competitor, without monitoring that of a drug. Furthermore, the present results suggest that attention should be paid to the type of the phase solubility diagram, as well as the magnitude of the stability constant and the solubility of the complex, for a rational formulation design of CyD complexes.