ABSTRACT
Here, we report a new version of the extended Rate Constants Distribution (RCD) model for metal ion sorption, which includes complex-formation equilibria. With the RCD-complex model, one can predict sorbent performance in the presence of complexing agents using data on metal ion sorption from ligand-free solutions and a set of coefficients for sorption rate constants of different ionic species. The RCD-complex model was applied to breakthrough curves of Cu(II) sorption from acetate and tartrate solutions on polyethyleneimine (PEI) monolith cryogel at different flow rates and ionic speciation. We have shown that, despite the lower stability of Cu(II)-acetate complex, at high flow rates, acetate has a more pronounced negative effect on sorption kinetics than tartrate. The RCD model was successfully used to predict the shape of the breakthrough curves at an arbitrary acetate concentration but failed to predict Cu(II) sorption from tartrate solutions in a broad range of ligand concentrations. Since a twofold increase in sorption capacity was observed at low tartrate concentrations, the latter fact was related to an alteration in the sorption mechanism of Cu(II)-ions, which depended on Cu(II) ionic speciation. The obtained results emphasize the importance of information about sorption kinetics of different ionic forms for the optimization of sorption filter performance in the presence of complexing agents.
Subject(s)
Cryogels , Polyethyleneimine , Kinetics , Tartrates , Hydrogen-Ion Concentration , Metals , Ions , Acetates , Adsorption , Copper , SolutionsABSTRACT
Here, we have presented a new method of 1,1,3-triglycidyloxypropane (TGP) synthesis and investigated how cross-linker branching affects mechanical properties and cytotoxicity of chitosan scaffolds in comparison with those cross-linked using diglycidyl ethers of 1,4-butandiol (BDDGE) and poly(ethylene glycol) (PEGDGE). We have demonstrated that TGP is an efficient cross-linker for chitosan at a subzero temperature at TGP:chitosan molar ratios from 1:1 to 1:20. Although the elasticity of chitosan scaffolds increased in the following order of the cross-linkers PEGDGE > TGP > BDDGE, TGP provided cryogels with the highest compressive strength. Chitosan-TGP cryogels have shown low cytotoxicity for colorectal cancer HCT 116 cell line and supported the formation of 3D multicellular structures of the spherical shape and size up to 200 µm, while in more brittle chitosan-BDDGE cryogel this cell culture formed epithelia-like sheets. Hence, the selection of the cross-linker type and concentration for chitosan scaffold fabrication can be used to mimic the solid tumor microenvironment of certain human tissue, control matrix-driven changes in the morphology of cancer cell aggregates, and facilitate long-term experiments with 3D tumor cell cultures.
ABSTRACT
The potential of chitosan and carboxymethyl chitosan (CMC) cryogels cross-linked with diglycidyl ether of 1,4-butandiol (BDDGE) and poly(ethylene glycol) (PEGDGE) have been compared in terms of 3D culturing HEK-293T cell line and preventing the bacterial colonization of the scaffolds. The first attempts to apply cryogels for the 3D co-culturing of bacteria and human cells have been undertaken toward the development of new models of host-pathogen interactions and bioimplant-associated infections. Using a combination of scanning electron microscopy, confocal laser scanning microscopy, and flow cytometry, we have demonstrated that CMC cryogels provided microenvironment stimulating cell-cell interactions and the growth of tightly packed multicellular spheroids, while cell-substrate interactions dominated in both chitosan cryogels, despite a significant difference in swelling capacities and Young's modulus of BDDGE- and PEGDGE-cross-linked scaffolds. Chitosan cryogels demonstrated only mild antimicrobial properties against Pseudomonas fluorescence, and could not prevent the formation of Staphylococcus aureus biofilm in DMEM media. CMC cryogels were more efficient in preventing the adhesion and colonization of both P. fluorescence and S. aureus on the surface, demonstrating antifouling properties rather than the ability to kill bacteria. The application of CMC cryogels to 3D co-culture HEK-293T spheroids with P. fluorescence revealed a higher resistance of human cells to bacterial toxins than in the 2D co-culture.
Subject(s)
Chitosan , Cryogels , Humans , Cryogels/pharmacology , Cryogels/chemistry , Chitosan/pharmacology , Chitosan/chemistry , Coculture Techniques , HEK293 Cells , Staphylococcus aureus , Polyethylene Glycols , Kidney , EthersABSTRACT
Macroporous scaffolds (cryogels) for the 3D cell culturing of colorectal cancer micro-tumors have been fabricated by cross-linking chitosan and carboxymethyl chitosan (CMC) with 1,4-butandiol diglycidyl ether (BDDGE) under subzero temperature. Due to the different intrinsic properties and reactivity of CMC and chitosan under the same cross-linking conditions, Young's moduli and swelling of the permeable for HCT 116 cells cryogels varied in the broad range 3-41 kPa and 3500-6000%, respectively. We have demonstrated that the morphology of micro-tumors can be controlled via selection of the polymer for the scaffold fabrication. Although both types of the cryogels had low cytotoxicity and supported fast cell proliferation, round-shaped tightly packed HCT 116 spheroids with an average size of 104 ± 30 µm were formed in CMC cryogels (Young's moduli 3-6 kPa), while epithelia-like continuous sheets with thickness up to 150 µm grew in chitosan cryogel (Young's modulus 41 kPa). There was an explicit similarity between HCT 116 micro-tumor morphology in soft (CMC cryogel) or stiff (chitosan cryogel) and in ultra-low attachment or adhesive culture plates, respectively, but cryogels provided the better control of the micro-tumor's size distribution and the possibility to perform long-term investigations of drug-response, cell-cell and cell-matrix interactions in vitro.
ABSTRACT
Here we demonstrate the possibility of using acyclic diethylacetal of acetaldehyde (ADA) with low cytotoxicity for the fabrication of hydrogels via Schiff bases formation between chitosan and acetaldehyde generated in situ from acetals in chitosan acetate solution. This approach is more convenient than a direct reaction between chitosan and acetaldehyde due to the better commercial availability and higher boiling point of the acetals. Rheological data confirmed the formation of intermolecular bonds in chitosan solution after the addition of acetaldehyde diethyl acetal at an equimolar NH2: acetal ratio. The chemical structure of the reaction products was determined using elemental analysis and 13C NMR and FT-IR spectroscopy. The formed chitosan-acetylimine underwent further irreversible redox transformations yielding a mechanically stable hydrogel insoluble in a broad pH range. The reported reaction is an example of when an inappropriate selection of acid type for chitosan dissolution prevents hydrogel formation.
ABSTRACT
Here, we discuss the applicability of (methylenebis(salicylaldehyde)-MbSA) for the fabrication of the stimuli-responsive N-carboxyethylchitosan (CEC) hydrogels with a tunable dissolution rate under physiological conditions. In comparison with non-covalent salicylimine hydrogels, MbSA cross-linking via covalent bis('imine clip') and non-covalent hydrophobic interactions allowed the fabrication of hydrogels with storage moduli > 1 kPa at ten-fold lower aldehyde/CEC molar ratio with the preservation of pH- and amino-acid responsive behavior. Although MbSA-cross-linked CEC hydrogels were stable at neutral and weakly alkaline pH, their disassembly in cell growth medium (Dulbecco's modified Eagle's medium, DMEM) under physiological conditions was feasible due to transimination reaction with amino acids contained in DMEM. Depending on the cross-linking density, the complete dissolution time of the fabricated hydrogels varied from 28 h to 11 days. The cytotoxicity of MbSA cross-linked CEC hydrogels toward a human colon carcinoma cell line (HCT 116) and primary human dermal fibroblasts (HDF) was remarkably lower in comparison with CEC-salicylimine hydrogels. Fast gelation, relatively low cytotoxicity, and tunable stimuli-induced disassembly under physiological conditions make MbSA cross-linked CEC hydrogels promising for drug encapsulation and release, 3D printing, cell culturing, and other biomedical applications.
ABSTRACT
Here we report on the properties of hydrogels of carboxyalkylchitosans-salicylimines depending on the salicylaldehyde (SA) grafting density, type of carboxyalkyl substitution, pH, and presence of amino acids. The mechanism of SA grafting has been investigated using 13C NMR and FT-IR spectroscopy and elemental analysis. We have found that, despite lower SA grafting density to carboxyalkylchitosans, gelation in these solutions occurred at much lower SA:polymer molar ratios than for chitosan-salicylimines, being the highest for a N-carboxyethylchitosan with a medium substitution degree. Controlled disassembly of supramolecular architecture of hydrogel of N-carboxyethylchitosan-salicylimine at physiological pH was achieved via the transimination reaction in the presence of amino acids with the efficiency decreased in the order: lysine > arginine ≥ serine. Application of carboxyalkylchitosans opens a new window for development of salicylimine-based hydrogels with lower SA grafting density, better mechanical properties, and reversibility in a broader pH range than it was earlier known for chitosan-based biodynamers.
Subject(s)
Chitosan/analogs & derivatives , Hydrogels/chemistry , Chitosan/chemistry , RheologyABSTRACT
Here we report the method of fabrication of supermacroporous monolith sorbents (cryogels) via covalent cross-linking of polyallylamine (PAA) with diglycidyl ether of 1,4-butandiol. Using comparative analysis of the permeability and sorption performance of the obtained PAA cryogels and earlier developed polyethyleneimine (PEI) cryogels, we have demonstrated the advantages and disadvantages of these polymers as sorbents of heavy metal ions (Cu(II), Zn(II), Cd(II), and Ni(II)) in fixed-bed applications and as supermacroporous matrices for the fabrication of composite cryogels containing copper ferrocyanide (CuFCN) for cesium ion sorption. Applying the rate constant distribution (RCD) model to the kinetic curves of Cu(II) ion sorption on PAA and PEI cryogels, we have elucidated the difference in sorption/desorption rates and affinity constants of these materials and showed that physical sorption contributed to the Cu(II) uptake by PAA, but not to that by PEI cryogels. It was shown that PAA cryogels had significantly higher selectivity for Cu(II) sorption in the presence of Zn(II) and Cd(II) ions in comparison with that of PEI cryogels, while irreversible sorption of Co(II) ions by PEI can be used for the separation of Ni(II) and Co(II) ions. Using IR and Mössbauer spectroscopy, we have demonstrated that strong complexation of Cu(II) ions with PEI significantly affects the in situ formation of Cu(II) ferrocyanide nanosorbents leading to their inefficiency for Cs+ ions selective uptake, whereas PAA cryogel was applicable for the fabrication of efficient monolith composites via the in situ formation of CuFCN or loading of ex situ formed CuFCN colloids.
Subject(s)
Adsorption/drug effects , Chelating Agents/chemistry , Cryogels/chemistry , Metals, Heavy/isolation & purification , Hydrogen-Ion Concentration , Ions/chemistry , Ions/isolation & purification , Metals, Heavy/chemistry , Polyamines/chemistry , Polyhydroxyethyl Methacrylate/chemistry , Sorption DetoxificationABSTRACT
Here we propose a metal-chelate approach to removal of fluoroquinolones from aqueous solutions using their ability to bind strongly divalent and trivalent metal ions immobilized in a polymer matrix. Metal-affine sorbents for ciprofloxacin uptake have been fabricated via chelation of Cu(II), Al(III), and Fe(III) ions by supermacroporous cryogel of carboxyalkyl chitosan derivative (N-(2-carboxyethyl)chitosan, CEC) cross-linked with hexamethylene diisocyanate in aqeous medium. We have shown that virgin CEC cryogel adsorbed ciprofoxacin in a cationic form via electrostatic interactions at pHâ¯>â¯pICEC, but the efficacy of recovery was below 50% and strongly pH-dependent. Modification of CEC cryogel with Cu(II) and Al(III) ions improved the ciprofloxacin (CIP) recovery by up to 98% in the pH range 7-10, the sorption capacity and affinity for CIP of metal-chelate sorbents increased with metal content and reached maximum values of 280 and 390â¯mg/g for Cu(II) and Al(III)-chelated cryogels, respectively. The metal-chelated CEC cryogels were efficient for ciprofloxacin removal from solutions with environmentally relevant concentration (50⯵g/L) and were applicable as monolith sorbents under dynamic conditions.
Subject(s)
Aluminum/chemistry , Chelating Agents/chemistry , Chitosan/analogs & derivatives , Ciprofloxacin/chemistry , Copper/chemistry , Cryogels/chemistry , Adsorption , Chitosan/chemistry , Fluoroquinolones/chemistry , Hydrogen-Ion Concentration , Microscopy, Electron, Scanning , Molecular Structure , Water Pollutants, ChemicalABSTRACT
Here we report a new simple method for fabrication of supermacroporous beads and monoliths via cross-linking of carboxyalkylated chitosan derivatives with hexamethylene diisocyanate in aqueous solution at subzero temperature. These materials provide high filtration rate and good mass-transfer that in combination with high binding capacity toward metal ions allows their application as a universal platform for fabrication of composite catalysts, sorbents, and metal-affine chromatography stationary phases. Using N-(2-carboxyethyl)chitosan (CEC), we have demonstrated that optimum chitosan carboxylation degree for cryogels synthesis is close to 1.0. Cu(II)-chelated CEC cryogels have shown high efficiency as metal-affinity sorbents for ciprofloxacin recovery. Co(II)-chelated CEC cryogels have been used for fabrication of Co(II) ferrocyanide-containing composite with the distribution coefficient for 137Cs of 140,000 ml/g and the adsorption capacity of Ë1 mmol/g. Composite Pd-catalysts supported on CEC cryogel provided tenfold higher reaction rate in 4-nitrophenol reduction in comparison with Pd-catalyst supported on chitosan beads.
ABSTRACT
Here we show that the efficacy of the chitosan interaction with diglycidyl ethers of glycols significantly depends on pH and the nature of acid used to dissolve chitosan. In solutions of hydrochloric acid, cross-linking with diglycidyl ethers of ethylene glycol (EGDGE) and polyethylene glycol (PEGDGE) at room and subzero temperatures yields mechanically stable chitosan gels and cryogels, while in acetic acid solutions only weak chitosan gels can be formed under the same conditions. A combination of elemental analysis, FT-IR spectroscopy, and solid state 13C and 15N NMR spectroscopy was used to elucidate possible differences in the mechanism of chitosan cross-linking in alkaline and acidic media at room and subzero temperatures. We have proved that in acidic media diglycidyl ethers of glycols interacted with chitosan mainly via hydroxyl groups at the C6 position of the glucosamine unit. Besides, not only cross-linkages but also grafts were formed at room temperature. The cryo-concentration effect facilitates cross-linkages formation at -10 °C and, despite lower modification degrees compared to those of gels obtained at room temperature, supermacroporous chitosan cryogels with Young's moduli up to 90 kPa can be fabricated in one step. Investigations of chitosan cryogels biocompatibility in a mouse model have shown that a moderate inflammatory reaction around the implants is accompanied by formation of a normal granulation tissue. No toxic, immunosuppressive, and sensitizing effects on the recipient's tissues have been observed.
Subject(s)
Cross-Linking Reagents/chemistry , Cryogels , Drugs, Chinese Herbal , Ethylene Glycol/chemistry , Materials Testing , Polyethylene Glycols/chemistry , Animals , Cryogels/chemical synthesis , Cryogels/chemistry , Cryogels/pharmacology , Drugs, Chinese Herbal/chemical synthesis , Drugs, Chinese Herbal/chemistry , Drugs, Chinese Herbal/pharmacology , Elastic Modulus , Hydrogen-Ion Concentration , Male , Mice , Mice, Inbred CBA , Nuclear Magnetic Resonance, Biomolecular , Porosity , Spectroscopy, Fourier Transform InfraredABSTRACT
Binding of Cu(2+), Ni(2+) and Ag(+) ions to polyallylamine (PAA), polyethylenimine (PEI), poly(N-2-(2-pyridyl)ethylallylamine) (PEPAA), poly(N-2-(2-pyridyl)ethylethylenimine) (PEPEI), and N-2-(2-pyridyl)ethylchitosan (PEC) has been investigated using batch sorption experiments, spectrophotometric titration, ESR, and XPS to elucidate how the structure of polymer precursors affects the ion binding efficiency of their pyridylethylated derivatives. It has been shown that pyridylethylation increases the sorption capacities of PAA and PEI cross-linked with epichlorohydrin toward Ag(+) and Ni(2+) ions, but does not improve or decrease that toward Cu(2+) ions. PEC was the most efficient material for Ag(+) ion sorption with the sorption capacity of 1.21 mmol g(-1). The highest sorption capacity for Ni(2+) (0.62 mmol g(-1)) was found for PEPEI. According to density functional theory (DFT) calculations, lower Cu(2+) binding efficiency to PEPEI results from the "looser" structure of this complex in comparison with unmodified PEI. DFT calculations have also suggested that the Cu(2+) ion is four-coordinated in the complexes with PEPAA and PAA and five-coordinated in all other complexes, which have the structures of distorted square pyramids with Cu-N bond lengths varying significantly depending on the ligand nature. The results of the theoretical investigations of the Cu(2+) complex structures were supported by the ESR data, which revealed the decrease of Aâ and the increase of gâ values with increasing deviation from the square planar geometry of complexes in the ligands in the order PEI < PEPEI < PEPAA.
ABSTRACT
Water soluble luminescent gold nanoparticles with average size 2.3nm were for the first time synthesized by completely green method of Au(III) reduction using chitosan derivative-biocompatible nontoxic N-(4-imidazolyl)methylchitosan (IMC) as both reducing and stabilizing agent. Reduction of Au(III) to gold nanoparticles in IMC solution is a slow process, in which coordination power of biopolymer controls both reducing species concentration and gold crystal growth rate. Gold nanoparticles formed in IMC solution do not manifest surface plasmon resonance, but exhibit luminescence at 375nm under UV light excitation at 230nm. Due to biological activity of imidazolyl-containing polymers and their ability to bind proteins and drugs, the obtained ultra-small gold nanoparticles can find an application for biomolecules detection, bio-imaging, drug delivery, and catalysis. Very high catalytic activity (as compared to gold nanoparticles obtained by other green methods) was found for Au/IMC nanoparticles in the model reaction of p-nitrophenol reduction providing complete conversion of p-nitrophenol to p-aminophenol within 180-190s under mild conditions.
Subject(s)
Gold/chemistry , Imidazoles/chemistry , Luminescent Agents/chemistry , Luminescent Agents/chemical synthesis , Metal Nanoparticles/chemistry , Biocompatible Materials/chemical synthesis , Biocompatible Materials/chemistry , Chemistry Techniques, Synthetic , Green Chemistry TechnologyABSTRACT
Here we report "green" synthesis of gold nanoparticles in solutions of heterocyclic chitosan derivatives (N-(4-imidazolyl)methylchitosan (IMC), N-2-(2-pyridyl)ethylchitosan (2-PEC), and N-2-(4-pyridyl)ethylchitosan (4-PEC)) and show how efficiency of Au(III) binding to polymer influences the Au(III) reduction rate and the size of the gold nanoparticles formed using only the reducing power of these chitosan derivatives. Rheology measurements and (1)H NMR spectroscopy data have confirmed that cleavage of glycosidic bond is a common mechanism of reducing species generation in solutions of chitosan and its N-heterocyclic derivatives. However, the emerging additional reducing species in 2-PEC and 4-PEC solutions due to vinylpyridine elimination promotes Au(III) reduction and gold nanoparticles growth despite lower efficiency of glycosidic bond cleavage in pyridyl derivatives. The decrease of the average size of gold nanoparticles in the row chitosan>2-PEC>IMC supported assumption that the increase of ligand nucleophilicity and stability of Au(III)-polymer complex results in formation of smaller nanoparticles.
