Thermosensitive mucoadhesive gel formulation loaded with 5-Fu: cyclodextrin complex for HPV-induced cervical cancer

Human Papilloma Virus (HPV) infections are the major cause of cervical cancers. To achieve a better therapeutic efficacy and patient compliance in the treatment for HPV-induced cervical cancers, anticancer agent 5-fluorouracil has been formulated in a vaginal gel using the thermosensitive polymer Pluronic^® F127 together with alternative mucoadhesive polymers e.g., hyaluronic acid, Carbopol 934 and hydroxypropylmethylcellulose. To increase its aqueous solubility and to achieve the complete release of 5-FU from the gel, the drug was incorporated as its inclusion complex with 1:1 molar ratio with either β-cyclodextrin or hydroxypropyl-β-cyclodextrin. Following the characterization of drug:CD complexes, thermosensitive gel formulations containing different mucoadhesive polymers and the drug in free or complexed form were characterized in vitro by determining the gelation temperature and the rheological behavior of different formulations along with the in vitro release profiles of these formulations in pH 5.5 citrate buffer. It was observed that complexation with cyclodextrin accelerated the release of 5-FU with the exception of formulation containing Carbopol 934 as mucoadhesive polymer. As far as rheological properties are concerned, favorable thermosensitive in situ gelling properties were obtained with formulations containing HPMC as mucoadhesive polymer. Complete release of 5-FU from gels were obtained with both complexes of β-CD and HP-β-CD and cytotoxicity studies against HeLa human cervical carcinoma cells demonstrated that 1% 5-FU:CD complexes were equally effective as 1% free 5-FU indicating better therapeutic efficacy with lower dose.     

One Convenient Preparation and Characterization of a New Amphiphilic Cationic Cyclodextrin Derivative 2-O-(Hydroxypropyl-N,N-Dimethyl-N-Dodecylammonio)-β-Cyclodextrin

A new amphiphilic cyclodextrin derivative 2-O-(hydroxypropyl-N,N-dimethyl-N-dodecylammonio)-β-cyclodextrin (2-HPDMDA-β-CD) was prepared and characterized by surface tension, electrical conductivity, dynamic light scattering, transmission electron microscopy (TEM) and steady-state fluorescence. 2-HPDMDA-β-CD was found to be a fine surfactant with a smaller critical micelle concentration (1.21 mM) value than that of dodecyltrimethylammonium chloride. TEM showed that 2-HPDMDA-β-CD could form two kinds of spherical aggregates in solution. The smaller one showed little concentration dependence while the larger one showed relatively strong concentration dependence. 2-HPDMDA-β-CD could be a fine host compound in molecular recognition with two functional spaces of the cyclodextrin cavity and micelles.     

Synthesis and characterization of poly(ethylene glycol) based β-cyclodextrin polymers

A series of novel water soluble β-cyclodextrin (βCD) polymers has been synthesized from functionalized poly(ethylene glycol) (PEG). The chemical composition of the polymers has been characterized by ¹H NMR and the βCD content is found to be between 48 and 33% (w/w). The molecular weight has been determined by Size Exclusion Chromatography (SEC) and depends on the ratio between βCD and PEG, varying from 2.1 × 10⁴ to 8.6 × 10⁴ g mol^?1. The physico chemical properties have been characterized by differential scanning calorimetry (DSC), viscometry and isothermal titration calorimetry (ITC). ITC shows that the polymers have association constants comparable to βCD with different guest molecules, indicating a good accessibility of the CDs.     

Comparison between 2-hydroxypropyl-��-cyclodextrin and 2-hydroxypropyl-��-cyclodextrin for inclusion complex formation with danazol

Complexation in solution between danazol and two different cyclodextrins [2-hydroxypropyl-??-cyclodextrin (HP-??-CD) and 2-hydroxypropyl-??-cyclodextrin (HP-??-CD)] was studied using phase solubility analysis, and one- and two-dimensional ¹H-NMR. The increase of danazol solubility in the aqueous cyclodextrin solutions showed a linear relationship (A_L profile). The apparent stability constant, K _1:1, of each complex was calculated and found to be 51.7 × 10³ and 7.3 × 10³ M^?1 for danazol?CHP-??-CD and danazol?CHP-??-CD, respectively. ¹H-NMR spectroscopic analysis of varying ratios of danazol and the different cyclodextrins in a mixture of EtOD?CD₂O confirmed the 1:1 stoichiometry. Cross-peaks, from 2D ROESY ¹H-NMR spectra, between protons of danazol and H3?? and H5??of cyclodextrins, which stay inside the cyclodextrin cavity, proved the formation of an inclusion complex between danazol and the cyclodextrins. For HP-??-CD, the inclusion complex is formed by entrance of the isooxazole and the A rings of danazol in the cyclodextrin cavity. For HP-??-CD, two different inclusion structures may exist simultaneously in solution: one with the isooxazole and A ring in the cavity and the other with the C and D ring inside the cavity. DLS showed that self-aggregation of the CD??s was absent in the danazol HP-??-CD system up to a CD concentration of 10% and in the danazol HP-??-CD system up to a CD concentration of 5%.     

Comparison and correlation of in vitro, in vivo and in silico evaluations of alpha, beta and gamma cyclodextrin complexes of curcumin

In the present study investigated the effect of curcumin (CUR) alpha (α), beta (β) and gamma (γ) cyclodextrin (CD) complexes on its solubility and bioavailability. CUR the active principle of turmeric is a natural antioxidant agent with potent anti-inflammatory activity along with chemotherapeutic and chemopreventive properties. Poor solubility and poor oral bioavailability are the main reasons which preclude CUR use in therapy. Extent of complexation was β-CD complex (82 %) > γ-CD (71 %) > α-CD (65 %). Pulverization method resulted in significant enhancement of CUR (0.002 mg/ml) solubility with CUR α-CD complex (0.364 mg/ml) > CUR β-CD complex (0.186 mg/ml) > CUR γ-CD complex (0.068 mg/ml). Gibbs-free energy and in silico molecular docking studies favour formation of α-CD complex > β-CD complex > γ-CD complex. With reference to CUR, relative bioavailability of CUR α-CD, CUR β-CD and CUR γ-CD complexes were 460, 365 and 99 % respectively. CUR–CD complexes exhibited increased bioavailability with an increase in t_½, tmax, Cmax, AUC, Ka, and MRT; and a decrease in Ke, clearance and Vd values. AUC increase was CUR α-CD complex > CUR β-CD complex > CUR γ-CD complex. Significant difference (p < 0.05) was observed between CUR α-CD complex and CUR γ-CD complex by one-way ANOVA and Dunnett’s post hoc test for multiple comparison analysis. Correlation observed between in vitro, in vivo and in silico methods indicates potential of in silico and in vitro methods in CD selection.     

β-Cyclodextrin as a photostabilizer of the plant growth regulator 2-(1-naphthyl) acetamide in aqueous solution

The plant growth regulator 2-(1-naphthyl) acetamide (NAAm) is susceptible to degradation by sunlight and UV light in aqueous solution. Its inclusion complex with β-cyclodextrin (β-CD) was characterized by absorption and fluorescence spectroscopy and its photodegradation was compared with that of aqueous solutions of NAAm. The complex was formed with a stoichiometric ratio of 1:1 with a binding constant of 651 M^?1. The photodegradation behavior of NAAm in the inclusion complex NAAm:β-CD was investigated using both UV (λ = 254 nm) and simulated solar light (Suntest) irradiation. It was found that the NAAm:β-CD complex increases NAAm photostability towards photochemical degradation markedly. In addition, an influence of β-CD concentration was also observed on NAAm degradation rate: higher β-CD concentrations lead to a slower photoinduced transformation. Moreover, some differences were found in the photoproducts in the presence and absence of the cyclodextrin, indicating inhibition of some of the mechanistic pathways. β-CD stabilizes NAAm photodegradation towards sunlight and UV irradiation, enhancing its efficient application on formulations for the treatment of fruits and vegetables.     

Sustained release drug delivery using supramolecular hydrogels of the triblock copolymer PCL–PEG–PCL and α-cyclodextrin

Supramolecular hydrogels (SMGel) have attracted much attention as a drug and gene delivery system in recent years. In this study, SMGels based on the tri-block copolymer of poly-ε-caprolactone–polyethylene glycol–poly-ε-caprolactone (PCL–PEG–PCL) and α-cyclodextrin (α-CD) were prepared and evaluated for the delivery of two model drugs, naltrexone hydrochloride and vitamin B₁₂. Tri-block copolymers were synthesized easily in 15 min by ring-opening polymerization using the microwave irradiation technique, and their structures were determined by gel permeation chromatography and nuclear magnetic resonance methods. SMGels composed of various concentrations of the copolymer and α-CD were prepared and characterized for their rheological behaviour, their gel formation time and in vitro drug release profile. The results indicated that copolymers with a PCL to PEG ratio of 1:4 are suitable for SMGel preparation. The most viscose system with good syringeability was prepared by mixing 12 % wt α-CD and 10 % wt of copolymer. The gelation was found to occur within a minute after mixing. The viscosity of the hydrogel systems was determined as a function of shear rate. Finally, in vitro B₁₂ release through the hydrogel systems was studied. Up to 80 % of Vitamin B₁₂ was released through this system during a period of 20 days. Rheological evaluation revealed that the hydrogel has shear thinning properties, and the system regained its ground rheological state in a time dependent manner. Polymer concentration did not affect the drug release profiles. Finally, it was concluded that such systems are appropriate drug delivery systems due to their ability to provide a controlled drug release profile and their shear thinning thixotropic behaviour, which makes them syringeable and injectable.     

Inclusion complexes with cyclodextrin and usnic acid

Molecular inclusion complexes of usnic acid (UA) with β-cyclodextrin (β-CD) and 2-hydroxypropyl β-cyclodextrin (HP β-CD) were prepared by the co-precipitation method in the solid state in the molar ratio of 1:1. Structural complexes characterization was based on different methods, FTIR, ¹H NMR, XRD and DSC. Parallel to the complex by the above methods, corresponding physical mixtures of UA with cyclodextrins and complexing agents (β-CD, HP β-CD and UA) were analyzed. The results of DSC analysis showed that, at around 200 °C, the endothermal peak in the complexes with cyclodextrins originating from the UA melting has disappeared. Complex diffractogram patterns do not contain peaks characteristic for the pure UA. They are more appropriate to cyclodextrin diffractogram. This fact points to the molecular encapsulation of UA in the cyclodextrin cavity. Chemical shifts in ¹H NMR spectra after the inclusion of UA into the cyclodextrin cavity, especially H-3 protons (0.0012 and 0.0102 ppm in the β-CD and HP β-CD, respectively) and H-5 and H-6 (0.0134 ppm) and hydrogen from CH₃ (0.0073 ppm) HP β-CD also points to the formation of molecular inclusion complexes. The improved solubility of UA in water was achieved by molecular incapsulation. In the complex with β-CD the solubility is 0.3 mg/cm³, with HP β-CD 4.2 mg/cm³ while the uncomplexed UA solubility is 0.06 mg/cm³. The microbial activity of UA and both complexes was tested against eight bacteria and two fungi and during the test no reduced activity of UA in the complexes was observed.     

Formulation and evaluation of gel containing nanostructured lipid carriers of tretinoin–Epi-β-CD binary complex for topical delivery

The objective of present research work was to formulate and evaluate topical gel containing tretinoin–cyclodextrin (CD) binary complex loaded into nanostructured lipid carriers (NLCs). Use of cyclodextrin and nanolipid carrier together in a system produced a synergistic effect by increasing the drug release and skin permeation, thus improving the overall therapeutic effect. Two different cyclodextrins i.e. β-CD and its water soluble polymeric derivative epichlorohydrin-β-cyclodextrin (EPI-β-CD) were used to obtain binary inclusion complex of drug-cyclodextrin (D-CD) systems by two different techniques (kneading and co-evaporation). The prepared solid complexes were characterized by FTIR, DSC, XRD etc. and the best system was selected for loading into nanolipid carriers. NLC comprising glyceryl mono stearate (GMS) and oleic acid were obtained by slightly modified emulsification evaporation method. Four different formulations of NLCs were suitability characterized for particle size, zeta potential, entrapment efficiency, drug loading and drug release. EPI-β-CD was found to be more effective than β-CD in enhancing solubility and dissolution properties of tretinoin. The most effective NLC formulation was incorporated into carbopol hydrogel which showed better permeation properties than that of the reference gel (0.1%).     

Development and evaluation of orodispersible sustained release formulation of amisulpride–γ-cyclodextrin inclusion complex

Amisulpride (AMI) is an atypical antipsychotic having poor aqueous solubility and poor oral bioavailability. Inclusion complex between AMI and gamma cyclodextrin (γ-CD) was prepared by kneading method using 1:1 stoichiometry. Solubility of AMI was enhanced by 3.74 times after inclusion complex formation. Amisulpride–γ-cyclodextrin inclusion complex was characterized by FTIR, DSC and XRD techniques. Further sustained release granules of Amisulpride–γ-cyclodextrin inclusion complex (CDSR) were prepared by treating complex with molten stearic acid. Drug release from CDSR granules was sustained up to 12 h with 100 % stearic acid proportion. The integrity of AMI–γ-CD inclusion complex in lipid phase was assessed by XRD study. Finally orodispersible tablets of CDSR granules (OD-CDSR) were prepared using Ac-Di-Sol and microcrystalline cellulose. Disintegration time was assessed by both pharmacopoeial and modified method. Optimized formulation was rapidly disintegrated within 25 s. Thus solubility enhancement and sustained release of AMI was achieved by orodispersion of CDSR granules for improvement of patient compliance.     

Study of benznidazole–cyclodextrin inclusion complexes, cytotoxicity and trypanocidal activity

The current chemotherapy for Chagas disease is still based on benznidazole, which has low solubility, but complexation with cyclodextrins provides a way of increasing the solubility. The objective of this work was to characterize the inclusion complexes formed between benznidazole (BNZ) and randomly 2-methyled-β-cyclodextrin (RM-β-CD) in aqueous solution and study cytotoxicity and trypanocidal. BNZ:RM-β-CD solution complex systems were prepared and characterized using the phase solubility diagram, nuclear magnetic resonance and a photostability assays, also to investigate the in vitro trypanocidal activity with epimastigote forms of Trypanossoma cruzi and the study of cytotoxicity against mammal cells. The phase-solubility diagram displayed an A _L-type feature, providing evidence of the formation of soluble inclusion complexes. The continuous variation method showed the existence of a complex with 1:1 stoichiometry. Toxicity assays demonstrated that inclusion complexes were able to reduce the toxic effects caused by benznidazole alone and that this did not interfere with the trypanocidal activity of the benznidazole. The use of inclusion complexes benznidazole:cyclodextrin is thus a promising alternative for the development of a safe and stable liquid formulation and a new option for the treatment of Chagas disease.     

Polybenzimidazoles,new thermally stable polymeres

Wholly aromatic polybenzimidazoles were synthesized from aromatic tetraamines and difunctional aromatic acids and characterized as new thermally stable polymers. The melt polycondensation of aromatic tetraamines and the diphenyl esters of aromatic dicarboxylic acids was developed as a general procedure of wide applicability. Polybenzimidazoles containing mixed aromatic units in the chain backbone were prepared from 3,3′-diaminobenzidine, 1,2,4,5-tetraaminobenzene and a variety of aromatic diphenyl dicarboxylates. Phenyl 3,4-diaminobenzoate could also be polymerized by melt condensation to give poly-2,5(6)-benzimidazole. The polymers were characterized by a high degree of stability, showing great resistance to treatment with hydrolytic media and an ability to withstand continued exposure to elevated temperatures. Most of the polymers were infusible, but some had melting points above about 400°C. Many of the polymers exhibited no change in properties on being heated to 550°C, and showed a weight loss of less than 5% when heated under nitrogen for several hours to 600°C. The polymers were soluble in concentrated sulfuric acid and formic acid, producing stable solutions. Many of the polymers were soluble in dimethyl sulfoxide and some also in dimethylformamide. The inherent viscosities of a number of polymers in 0.5% dimethyl sulfoxide solution ranged from approximately 0.4 to 1.1. The higher polymers could be cast into stiff and tough films from formic acid and dimethyl sulfoxide solutions.     

Enhancement of Dissolution Behavior of Aceclofenac by Complexation with β-Cyclodextrin-Choline Dichloride Coprecipitate

The objective of the present investigation was to study the effect of presence of choline dichloride (CDC) in β-cyclodextrin (β-CD) on in vitro dissolution of aceclofenac (AF) from molecular inclusion complexes. The molecular inclusion complexes of AF with β-CD coprecipitated with CDC in 1:1 and 1:2 M ratio were prepared using kneading method. In vitro dissolution of pure drug, physical mixtures, and cyclodextrin inclusion complexes (AF-β-CD-CDC) were carried out. Molecular inclusion complexes of aceclofenac with coprecipitated β-CD showed considerable increase in the dissolution rate in comparison with physical mixture and pure drug in 0.1 N HCl, pH 1.2 and phosphate buffer, pH, 7.4. Inclusion complexes with 1:2 M ratio showed maximum dissolution rate in comparison to other ratios. FTIR spectroscopy and differential scanning calorimetry studies indicated no interaction between AF and β-CD-CDC in complexes in solid state. Dissolution enhancement was attributed to the formation of water soluble inclusion complexes with the precipitated form of β-CD. The in vitro release from all the formulations was best described by first order kinetics (R ² = 0.9354 and 0.9268 in 0.1 N HCl and phosphate buffer, respectively) followed by Higuchi release model (R ² = 0.9029 and 0.9578 in 0.1 N HCl and phosphate buffer, respectively). In conclusion, dissolution of aceclofenac can be enhanced by using the β-CD-CDC coprecipitate as a host molecule.     

Spectroscopic characterization of the binding and isomerization cycle of Brooker’s merocyanine with α-, β-, and γ-cyclodextrins

Complexes of Brooker’s merocyanine dye with α-, β- and γ-cyclodextrin (CD) have been characterized to determine the relative strength and thermodynamics of binding, as well as the effect of binding on the protolytic-photochemical isomerization cycle of the dye. It was found that the dye binds most tightly to β-CD, with a binding equilibrium constant of 430 M^?1, in agreement with previous results (Hamasaki et al. J. Incl. Phenom. Mol. Rec. Chem. 13, 349–359 (1992)), while α-CD and γ-CD complexes have a binding constant of approximately 110 M^?1 and 70 M^?1, respectively, determined using absorbance and fluorescence spectroscopy. The isomerization cycle for the dye in α- and γ-CD complexes was found to be the same as for the free dye. Complexation with β-CD, however, resulted in depressed trans-to-cis photoisomerization in acidic conditions followed by spontaneous cis-to-trans isomerization (with the addition of base). Thermodynamic results also indicated differences between α-CD (ΔS° = ?48 J K^?1) and β-CD (ΔS° =  +12 J K^?1) complexes. There was no temperature dependence observed for the γ-CD complexes. These results can be justified in terms of the location of the dye molecule within the cyclodextrin cavity for each of the complexes.     

环糊精葡萄糖基转移酶的固定化及其应用──Ⅲ．固定化环糊精葡萄糖基转移酶制备环糊精的研究

用固定化环糊精葡萄糖基转移酶催化淀粉环化反应,考察了反应时间、乙醇浓度和淀粉液化程度对环糊精产率的影响。环糊精产率最高达54%,固定化酶经多次重复使用或长时间连续操作,酶活力降低较少,产品经纸色谱分离后用碘显色,发现产品主要为β-环糊精。     

Evaluation the effect of cyclodextrin complexation on aqueous solubility of fluorometholone to achieve ophthalmic solution

In this study, the effect of different CDs including α-CD, β-CD, γ-CD, hydroxypropyl β-CD (HP β-CD), sulphobutylether β-CD (SBE β-CD) and HP γ-CD on aqueous solubility of fluorometholone (Flu) was investigated. Also the phase solubility studies were performed in the presence of eye drop excipients such as benzalkonium chloride, hydroxypropyl methylcellulose (HPMC) and buffers. The aqueous solubility of Flu was increased by 8, 15, 5, 100, 65 and 135 folds in the presence of 20% w/v α-CD, β-CD, γ-CD, HP β-CD, HP γ-CD and SBE β-CD, respectively. Aqueous solubility of Flu was 0.43 ± 0.08 and 1.16 ± 0.04 mg/mL in systems containing 5% w/v HP γ-CD and SBE β-CD, respectively. The aqueous solubility of Flu in the presence of HP γ-CD was not influenced by buffer type while the phosphate buffer caused a reduction in the aqueous solubility in the presence of SBE-β-CD. Also, investigations on the solubility of Flu in water in the presence of 5% HP γ-CD and SBE-β-CD and the additives such as benzalkonium chloride and HPMC indicated that these components had no remarkable effect on the aqueous solubility of Flu. In conclusion, CD complexation is able to improve the aqueous solubility of Flu and it would be possible to prepare ophthalmic solution of Flu by this method.     

Poly-2-oxazolidones: Preparation and characterization

Poly-2-oxazolidones were synthesized by the 1,3-cycloaddition of bisglycidyl ethers to diisocyanates with the use of N,N-dimethylformamide and lithium chloride as solvent and catalyst, respectively. A variety of arylene and alkylene diisocyanates and coreactant bisepoxides were used in the polymer-forming reaction. The polymers, obtained in high yield, were generally soluble in methylene dichloride, chloroform, N,N-dimethylformamide, and dimethyl sulfoxide. They had intrinsie viscosities up to 0.42 dl/g and could be cast into films. In several cases molecular weights were determined by vapor pressure osmometry. The poly-2-oxazolidone based upon 1,6-hexamethylene diisocyanate and the bisglycidyl ether of isopropylidene diphenol gave the highest molecular weight. Confirmation that the base unit of the polymers contains the 2-oxazolidone ring was obtained by elemental analysis, infrared and NMR spectroscopy. The poly-2-oxazolidones synthesized were found to be amorphous by x-ray diffraction. Thermogravimetric analyses indicated that a majority of the poly-2-oxazolidones were stable in dry air up to 300°C. In a number of cases Tg's were also determined by using differential scanning calorimetry.     

Synthesis of alkyl glycosides from cyclodextrin using cyclodextrin glycosyltransferase from Paenibacillus sp. RB01

Alkyl glycosides have potential use as biodegradable detergents due to their high surface activity with low toxicity. Recent progress in the application of enzymes to the preparation of these surface-active compounds demonstrates the advantages to the chemical synthesis. In this work, alkyl glycosides were, for the first time, synthesized from cyclodextrin (CD) and various soluble alcohols by transglycosylation reaction using cyclodextrin glycosyltransferase (CGTase) from Paenibacillus sp. RB01. Several alcohols (methanol, ethanol, 1-propanol, 2-propanol, 1-butanol and 2-butanol) as glycosyl-acceptor substrates were evaluated. It was found that the reaction products which were analyzed by TLC were maximum for 30% methanol, 20?C30% ethanol, 10?C20% 1-propanol, 10% 2-propanol, 8% 1-butanol and 5?C10% 2-butanol. In addition, the increase in the yield of alkyl glycoside formation was achieved by using methanol as an acceptor. Optimal reaction conditions for methyl glycoside synthesis from CD were to incubate 1.2% (w/v) ??-CD and 240 U/mL of CGTase in a water/methanol system containing 30% (v/v) methanol, pH 6.0 and a temperature of 40???C. At least three main methyl glycoside products were formed having 1?C3 monosaccharide units attached to methanol which were in accordance with the results of MS analysis.     

Synthesis of fusible and soluble conducting polyfluorene derivatives and their characteristics

Conducting polyfluorene derivatives with alkyl chains—poly(9-alkylfluorene)s and poly-(9,9-dialkylfluorene)s—have been synthesized by chemical polymerization utilizing FeCl₃ as an oxidizing agent. The polymers obtained are found to be soluble in conventional organic solvents such as chloroform and have been characterized by ¹H- and ¹³C-NMR. The results indicate that the fluorene moeities are mainly linked in the 2,7′-fashion to yield the straight chain polymer. The degree of polymerization is estimated (by gel permeation chromatography) to be of the order of 10. The polymers are found to be fusible and the thermal properties of the polymers have been characterized by differential scanning calorimetry. The glass transition temperature is found to decrease with an increase of the alkyl chain length. © 1993 John Wiley & Sons, Inc.     

碱性水溶液中单6-氧-对甲苯磺酰-β-环糊精酯的非均相合成

不引入有机溶剂,低温下将对甲苯磺酰氯与β-环糊精在NaOH水溶液中进行非均相反应,得到了单6-氧-对甲苯磺酰-β-环糊精酯(6-OTs-β-CD).借助1H NMR谱证实了环糊精单磺酰化机理.考察了产物的水解因素,研究了反应条件对产率的影响.实验结果表明,投料摩尔比n(CD)∶n(TsCl) =4∶1,碱液浓度0.75...