Preparation and properties of insoluble films of cyclodextrin condensation polymers

The preparation and properties of smooth and stable films of cyclodextrin polymers are described. The commercially available water soluble prepolymers of-, -, and-cyclodextrin of low molecular masses were crosslinked with glutaric dialdehyde. Side-chain unreacted aldehyde groups were reduced with sodium borohydride. For the-cyclodextrin polymer, optimum film performance was found for a 1:10 mass ratio of glutaric dialdehyde to prepolymer, which corresponds to a molar ratio of glutaric dialdehyde to cyclodextrin units of about 1.75: 1. Such films, of thickness 2.4 µm, were prepared on metallic or glassy-carbon substrates for characterization by scanning-electron microscopy, and for studies with the electrochemical quartz-crystal microbalance.     

相溶解度法研究环糊精对蒽醌药物的增溶作用

通过相溶解度法,测定1,2-二氨基蒽醌、1,4-二氨基蒽醌和1,8-二羟基蒽醌在不同温度、不同浓度的β-环糊精(β-CD)、羟丙基-β-环糊精(HP-β-CD)以及羟乙基-β-环糊精(HE-β-CD)中的溶解度,绘制相溶解度曲线,并进行回收率及稳定性实验.实验结果表明:1,2-二氨基蒽醌、1,4-二氨基蒽醌和1,8-二羟基蒽醌的溶解度均随3种环糊精浓度的增加而呈线性增加,相溶解度曲线为AL型,蒽醌与环糊精形成的包合物类型为1∶1型,3种环糊精对蒽醌均有增溶作用,增溶效应顺序为HP-β-CDHE-β-CDβ-CD,与HP-β-CD作用顺序为1,2-二氨基蒽醌1,4-二氨基蒽醌1,8-二羟基蒽醌.     

Water soluble progesterone–hydroxypropyl-β-cyclodextrin complex for injectable formulations

The use of cyclodextrin to increase the water solubility of progesterone (P) was described by Pitha as a complex with β-cyclodextrin and derivates to obtain a water soluble formulation (Pitha, J.: US patent n. 4,727,064). Hydroxypropyl-β-cyclodextrin (HPBCD) has a high water solubility which allows the solubilization of high quantity of P. Considering a 1:2 guess/host complex stoichiometry it is possible to obtain up to 50 mg/ml of P concentration, which is a considerable dosage for drug development in the progesterone therapy. In our drug development the P/HPBCD complex in water showed the formation of a light precipitate during stability ICH conditions. A precipitate formation was described already by Choi (J. Korean Pharm. Sci. 31(3), 151, 2001) and also by Pitha (US patent n. 4,727,064) but the chemical structure was not elucidated. In our case the precipitate was purified and it turned out to contain progesterone and residual unmodified β-cyclodextrin. We have developed a production process in which the residual unreacted β-cyclodextrin is separated from the HPBCD by the formation of the insoluble inclusion complex (Zoppetti et al.: European Patent deposit n. 05108494.5). The resulting P/HPBCD contains up to 0.1% of residual β-cyclodextrin and does not produce precipitate during the stability study. The complex stoichiometry and the complex constant were calculated by the phase solubility study according to Higuchi and Connors (Adv. Anal. Chem. Instrum. 4, 117, 1965) and the presence of the inclusion complex was demonstrated by DSC, NMR, X-ray, FTIR. The formulation prepared at pilot scale as injectable form compared with the commercial oil formulation demonstrated a favourable kinetic in humans.     

Solid dispersion systems engineered from hydroxypropyl‐β‐cyclodextrin and water‐soluble polymers for enhanced oral bioavailability of nimodipine

Nimodipine (NMD) is a calcium channel blocker that is used in the treatment of cerebrovascular disorders, such as stroke indicated for biological rhythm and neurological disorders. According to biopharmaceutical classification, NMD is categorized as a class ΙΙ drug, meaning it has a poor solubility profile. The objective of this experiment is to prepare multicomponent systems to enhance the solubility, dissolution, and bioavailability of NMD. Inclusion complex and solvent evaporation techniques have been exploited to overcome this challenge. in vitro dissolution studies and solubility, the profile was performed in three pH media (pH 7.5, 1.2, and 6.8). The drug release at (Q_60min) for SD‐PVP3 was 33‐fold higher than pure NMD in double‐distilled water. The solubility of SD PVP3 was about 30 times higher than plain NMD in double‐distilled water. A pharmacokinetic study in rats indicated that the AUC_0‐720 value of the inclusion complex (NMD‐KD) was 1.63‐fold higher than pure NMD. At the same time, the solid dispersion (NMD‐SD PVP3) was 3.94‐fold higher than that of plain NMD, indicating a significant increase in the bioavailability of NMD. The combination of the inclusion complex and solvent evaporation method led to the formation of new solid dispersions (SD PLX and SD PVP), which significantly increased the solubility, dissolution, and the oral bioavailability of NMD.     

The use of naphthalene fluorescence probes to study the binding sites on cyclodextrin polymers formed from reaction of cyclodextrin monomers with epichlorohydrin

Three naphthalene-based fluorescence probes were used as guest molecules to study host/guest binding with cyclodextrin (CD) polymer hosts prepared by treating -,-, or -cyclodextrin monomers with epichlorohydrin. The fluorescence data indicate that the binding interaction is much stronger for the probes with the CD polymers than with the CD monomers. Moreover, the fluorophore binding site on the CD polymers is also more hydrophobic than that on the CD monomers. Fluorescence lifetime data from one of the bound probes (2-(N-methylanilino) naphthalene-6-sulfonic acid) suggest that more than one type of binding site may exist on the CD polymers with this probe. A comparison of fluorescence data using different molecular weight ranges of the CD polymers appear to rule out the possibility of a 12 host/guest complex, where the two CD units come from the same polymer chain.     

Structure and molecular dynamics of solid-state inclusion complexes of cyclodextrin and permethylated cyclodextrin with benzaldehyde studied by high-resolution CP/MAS13C NMR

The structure and molecular dynamics of the benzaldehyde inclusion-complexes with -and-cyclodextrins and permethylated -cyclodextrin in the solid state have been studied by high-resolution cross-polarization/magic angle sample-spinning¹³C NMR spectroscopy. It is shown that the guest benzaldehyde molecule undergoes motion in the host cyclodextrin cavity and the rate of motion depend on the cavity size. In the -cyclodextrin complex, compared to -and permethylated -cyclodextrin complexes, the benzaldehyde motion is severely restricted, but under high-vacuum benzaldehyde is released more easily from the cavity.     

Synthesis of water‐soluble cationic polymers with star‐like structure based on cyclodextrin core via ATRP

A range of novel cationic star‐like polymers (Star‐P(MeDMA)s) were synthesized through atom transfer radical polymerization (ATRP) by core‐first method, using a β‐cyclodextrin initiator with 21 initiation sites (21Br‐β‐CD). Methyl chloride‐quaternized 2‐(dimethylamino)ethyl methacrylate (MeDMA) was polymerized in an aqueous medium using 21Br‐β‐CD, Cu(I)Br, and 2,2′‐dipyridyl as an initiator, catalyst, and ligand, respectively. The effects of polymerization temperature and monomer/initiator ratios on the degree and kinetics of polymerization were investigated. The molecular weights, hydrodynamic sizes, and charge densities of the quaternized polymers were characterized using gel permeation chromatography (GPC), dynamic light scattering (DLS), and colloidal titration, respectively. The results demonstrated that the moderate aqueous solubility of the 21Br‐β‐CD initiator had significant impact on the physicochemical properties of the obtained star polymers. The polymerization of 500/1/2/5 ([M]₀/[I]₀/[Cu(I)₀/[L]₀]) at 90 °C for 6 h was found to be the best condition to synthesize the proposed cationic star polymer with well‐defined structures in aqueous medium. The nonlinear relationship between the apparent charge density and the particle size of the cationic star polymers was further revealed by GPC and DLS measurements. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 6345–6354, 2005     

几种氰类, 酯类取代基季铵盐吡啶卟啉及其金属配合物的合成

水溶性卟啉及其金属络合物可用作催化剂、络合剂、光敏剂以及抗癌药物等,用途较广。近年来,利用水溶性卟啉的光敏化作用对     

Complexation of nitrostyrenes with soluble β-cyclodextrin polymer studied by reversed-phase thin-layer chromatography

Cyclodextrin complexation decreases the apparent lipophilicity of hydrophobic guest molecules. A higher complex stability results in a larger decrease of lipophilicity as determined by reversed-phase thin-layer chromatography. The method was applied to study the complex formation of 33 nitrostyrene derivatives with a water soluble cross linked -cyclodextrin polymer (weight average molecular weight: 4300). The substituents in thepara position of the benzene ring had a higher impact on the complex stability than those in themeta andortho positions. The substituents on the alkyl side chain influenced the complex stability to the same extent as those on the benzen ring.     

Biophysical aspects of cyclodextrin interaction with paraoxon

Cyclodextrins are torus‐shaped polymers of glucose that can bind organophosphorous compounds such as nerve agents and pesticides. We demonstrate here that cyclodextrin can bind up to two paraoxon molecules with a K_av of 6775 M^‐1. Molecular modeling shows that the paraoxon appears to bind in polar opposite orientation and have an average binding energy of ?89 Kcals/mol. Published 2013. This article is a U.S. Government work and is in the public domain in the USA.     

Crown ethers derived from cyclodextrin: Interaction with triphenylmethane derivatives

Periodate oxidation followed by borohydride reduction of beta cyclodextrin results in crown ether type derivatives. The polyaldehyde obtained by periodate oxidation has been reduced to polyalcohol and converted to a permethylated derivative. These macrorings are much more flexible than beta cyclodextrin itself.The interaction of beta cyclodextrin (-CD), methylated beta cyclodextrin (DIMEB), polyalcohol and permethylated crown ethers derived from beta cyclodextrin with two triphenylmethane, derivatives and their triphenyltin analogues has been studied. On the basis of the changes in the UV spectra and the solubility enhancement it can be concluded that cyclodextrins (-CD and DIMEB) form complexes only with the triphenylmethane, derivatives. On the other hand the crown ethers prepared from -CD give complexes only with the triphenyltin derivatives.     

Novel species of soluble thermally stable poly(keto ether ether amide)s: preparation,characterization, and properties

A new diamine containing one keto and four ether groups was prepared through a three‐step reaction: first, hydroquinone was reacted with 1‐fluoro‐4‐nitrobenzene and 4‐(4‐nitrophenoxy) phenol was obtained. The next step was reduction of nitro group to amino group in which 4‐(4‐aminophenoxy) phenol was prepared. In the final step, the new diamine named as bis(4‐(4‐(4‐aminophenoxy)phenoxy)phenyl) methanone was synthesized through reaction of the later compound with 4,4′‐difluoro benzophenone. All prepared materials were fully characterized by spectroscopic methods and elemental analysis. Novel species of poly(keto ether ether amide)s were synthesized via polymerization reaction of the diamine with different diacid chlorides including terephthaloyl chloride, isophthaloyl chloride, and adipoyl chloride. All polyamides were characterized, and their properties such as thermal behavior, thermal stability, solubility, viscosity, water uptake, and crystallinity were investigated and compared together. The glass transition temperatures of the polymers were about 204–232°C, and their 10% weight losses were in the range of 396–448°C. Polymers showed high thermal stability and enhanced solubility that mainly resulted from incorporation of the diamine structure containing keto, ether, and aromatic units into polyamide backbones. Copyright © 2014 John Wiley & Sons, Ltd.     

Study on inclusion interaction of piroxicam with beta-cyclodextrin derivatives

The inclusion behavior of piroxicam (PX) with beta-cyclodextrin (beta-CD), hydroxypropyl-beta-cyclodextrin (HP-beta-CD), and carboxymethyl-beta-cyclodextrin (CM-beta-CD) was investigated by using steady-state fluorescence and nuclear magnetic resonance (NMR) technique. The various factors affecting the inclusion process were examined in detail. The remarkable fluorescence emission enhancement upon addition of CDs suggested that cyclodextrins (CDs) were most suitable for inclusion of the uncharged species of PX. The stoichiometry of the PX-CDs inclusion complexes was 1:1, except for beta-CD where a 1:2 inclusion complex was formed. The formation constants showed the strongest inclusion capacity of beta-CD. NMR showed the inclusion mode of PX with CDs.     

Kinetic resolution of primary amines via enantioselective N-acylation with acyl chlorides in the presence of supramolecular cyclodextrin nanocapsules

The non-enzymatic kinetic resolution of primary amines via enantioselective N-acylation with acyl chlorides was accomplished for the first time by using the selective sequestration of one enantiomer within a supramolecular cyclodextrin (CD) nanocapsule in nonpolar solvents. In addition, the first example of a crystalline structure for an inclusion complex between an acyl chloride and a CD derivative is reported.     

稀土离子配合物与磷脂双分子膜的作用研究

利用一维和二维Ｈ核磁共振方法研究了柠檬酸稀土、稀土－ＤＴＰＡ配合物与磷脂双分子膜的作用，结果表明Ｌ在近生理条件下（ＰＨ＝７．４）及 柠檬酸配体的磷脂双分子膜体系中，稀土离子首先与柠檬酸体作用，形成的配合物对磷脂双分子膜的结构影响较小，稀土－ＤＴＰＡ配合物对磷脂双分子膜的结构没有影响这些结果为科学地评价稀土离子进行体内的毒性提供了实验依据。     

Mechanistic studies on cationic ring-opening polymerisation of cyclodextrin derivatives using various Lewis acids

In order to investigate the potential of cyclodextrins for the preparation of block-like substituted polysaccharides, we submitted mixtures of heptakis[2,3,6-tri-O-methyl]-β-cyclodextrin (Me₂₁-β-CD, 1) and heptakis[2,3,6-tri-O-methyl-d ₃]-β-cyclodextrin ((Me-d ₃)₂₁-β-CD, 2) to cationic ring-opening polymerisation (CROP). Reactions were performed with BF₃·OEt₂, methyl triflate (MeOTf), and Et₃OSbCl₆. Products were compared with respect to their degree of polymerisation (DP) and the average block length (BL). Highest DP was observed with BF₃·OEt₂, while Et₃OSbCl₆ was the most active initiator. Average block length decreased from 14 in the early stage of product formation to about 2 due to competing chain transfer reaction. ¹H NMR spectroscopy, GLC, GLC–MS, ESI-MS and MALDI-TOF-MS were applied for detailed investigations of side reactions. During incubation with BF₃·OEt₂, a stereroisomeric β-CD with one β-glucosidic linkage (Me₂₁-β-CD_6α1β, 3a (Me-d ₃)₂₁-β-CD_{6α 1β}, 3b) is formed as an intermediate, while linear Me₂₁- and (Me-d ₃)₂₁-maltoheptaose (4a/b) was detected in the early stage of the reaction promoted by MeOTf. In the case of Et₃OSbCl₆, both intermediates (3a/b, 4a/b) can be observed during the lag phase of polymerisation, but to a very low degree. End group analysis by GLC reveals that some alkyl exchange occurs at position 3 and 6 in the presence of Et₃OSbCl₆, and that polymerisation is also initiated by protons. Copolymerisation of heptakis[2,3,6-tri-O-benzyl]-β-cyclodextrin (Bn₂₁-β-CD, 5) and Me₂₁-β-CD (1) and subsequent debenzylation yielded a polymer of only 1,4-glcp-Me₃- and 1,4-glcp-residues. Reactivity of Bn₂₁-β-CD was significantly lower than of Me₂₁-β-CD, resulting in higher average block length of 1,4-glcp-Me₃-units.     

Low-field 1H NMR spectroscopy: Factors impacting signal-to-noise ratio and experimental time in the context of mixed microstructure polyisoprenes

Low-cost, high-accuracy characterization of polymeric materials is critical for satisfying societal demand for high-quality materials with ultra-specific requirements. Low-field nuclear magnetic resonance (NMR) spectroscopy presents an opportunity to replace costlier or destructive methods while utilizing nondeuterated solvents. Many factors play key roles in the ability of low-field NMR spectroscopy to accurately analyze polymer systems. Sample characteristics such as polymer concentration, composition, and molecular weight all directly affect the capability of low-field spectrometers to accurately determine polymer microstructure compositions. In addition to inherent sample properties affecting instrumental accuracy, many choices concerning instrumental parameters (including number of scans, relaxation delay, spectral width, and points per scan) must be made that impact the quality of the resulting NMR spectra. In this work, we benchmark the capability of a 60-MHz low-field NMR spectrometer for analyzing polymer materials using mixed microstructure polyisoprenes as a model polymer system of interest. The aforementioned critical sample and instrumental variables are varied, and we report on the ability to quantitatively characterize polyisoprene microstructure to within 1–2% of a higher field NMR spectrometer (400 MHz). We anticipate our findings to be generally applicable to other low-field spectrometers of similar field strength and other polymer systems.     

Reaction of water soluble polymers with oxidising agents: reaction of dextran with tetravalent cerium

Dextran, an extracellular bacterial polysaccharide, was subjected to reaction with ceric ammonium nitrate in aqueous nitric acid at varying temperatures. The polymer has been found to be degraded due to the selective oxidative cleavage of vicinal glycol units present in the monosaccharide unit of each chain. The aldehyde groups produced upon cleavage at low temperature were found to undergo further oxidation to acids and formic acid with rise in temperature of the reaction. The course of the reaction has been followed by cerimetry and by spectrophotometrical measurements. The effect of the concentration of reacting components on the reaction has been studied and various kinetic aspects have been evaluated. Depending on the kinetic results, a plausible reaction mechanism for the oxidative degradation and the subsequent reactions have been suggested by the study of the changes of solution viscosity and initiation of graft copolymerization of vinyl monomers by Ce(IV)/dextran mixture. Various thermodynamic parameters have been evaluated.     

Interaction of cyclodextrins with drugs. Chromatographic investigation using a cyclodextrin bonded-phase and its application to chiral separations

Summary The interaction between cyclodextrin and the drug (1R,2S,3S,4S)-(5Z)-7-(3-((phenylsulfonyl)amino)bicyclo[2.2.1]hept-2-yl)hept-5-enoic acid ((+)-S-145), was studied using -, -, and -cyclodextrin bonded-phase columns. Retention behavior of (+)-S-145 on these columns revealed that the strength of inclusion was -cyclodextrin. Interaction between -cyclodextrin and (+)-S-145 was found to increase as the proportion of carboxylic ion in the (+)-S-145 molecule increased. Comparison of binding capacities of these bondedsilica gels obtained by frontal analysis and surface coverage indicated that availability of the immobilized - and -cyclodextrin was 20–25%. The synthesized -cyclodextrin bonded-phase column was superior to that of commercial columns in terms of chiral separation of (±)-S-145. A typical usage of the -cyclodextrin column is discussed for separation of (±)-S-145 in plasma samples.