Your search keyword '"Grøndahl, L."' showing total 7 results

1. Evaluation of the in vivo fate of ultrapure alginate in a BALB/c mouse model.

Author

A A, Fletcher NL, Houston ZH, Thurecht KJ, and Grøndahl L

Subjects

Animals, Flow Cytometry methods, Liver metabolism, Macrophages metabolism, Mice, Mice, Inbred BALB C, Optical Imaging methods, Positron-Emission Tomography methods, Seaweed chemistry, Spleen metabolism, Tissue Distribution, Alginates metabolism

Abstract

The linear anionic polysaccharide alginate (ALG) has been comprehensively studied for biomedical applications, yet thus far the in vivo fate of this polymer has not been explored in detail. The current study therefore evaluates the biodistribution of ultrapure ALG (M/G ratio ≥ 0.67 with a measured M w of 530 kg/mol and polydispersity index; PDI of 1.49) over a 14-day period in BALB/c mice. The biodistribution pattern over 2-days after sample administration using PET imaging with 64 Cu-labelled ALG showed liver and spleen uptake. This was confirmed by the 14-day biodistribution profile of cyanine 5-labelled ALG from in vivo and ex vivo fluorescence imaging. Using MacGreen mice confirmed the uptake of the ALG by macrophages in the spleen at the 2-day time point. This extended biodistribution study confirmed the clearance of only a portion of the administered ALG biopolymer, but also uptake by macrophage populations in the spleen over a 14-day period., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

2. Interactions between Chitosan and Alginate Dialdehyde Biopolymers and Their Layer-by-Layer Assemblies.

Author

Aston R, Wimalaratne M, Brock A, Lawrie G, and Grøndahl L

Subjects

Glass chemistry, Hydrogels chemistry, Silicon Dioxide chemistry, Alginates chemistry, Chitosan chemistry

Abstract

Biopolymers are researched extensively for their applications in biomaterials science and drug delivery including structures and complexes of more than one polymer. Chemical characterization of complexes formed between chitosan (CHI) and alginate dialdehyde (ADA) biopolymers established that while electrostatic interactions dominate (as determined from X-ray photoelectron spectroscopy (XPS)) covalent cross-linking between these biopolymers also contribute to their stability (evidenced from immersion in salt solution). It was furthermore found that imine bond formation could not be directly detected by any of the techniques XPS, FTIR, (1)H NMR, or fluorescence. The layer-by-layer assemblies of the biopolymers formed on silica colloids, glass slides, and alginate hydrogel beads were evaluated using XPS, as well as zeta potential measurements for the silica colloids and changes to hydration properties for the hydrogels. It was found that the degree of oxidation of ADA affected the LbL assemblies in terms of a greater degree of CHI penetration observed when using the more conformationally flexible biopolymer ADA (higher degree of oxidation).

Published

2015

3. Delivery of dermatan sulfate from polyelectrolyte complex-containing alginate composite microspheres for tissue regeneration.

Author

Wen Y, Grøndahl L, Gallego MR, Jorgensen L, Møller EH, and Nielsen HM

Subjects

Animals, Biocompatible Materials administration & dosage, Cell Proliferation, Cells, Cultured, Fibroblasts cytology, Fibroblasts drug effects, Hydrogen-Ion Concentration, Mice, Tissue Engineering, Alginates administration & dosage, Chitosan administration & dosage, Dermatan Sulfate administration & dosage, Drug Delivery Systems, Electrolytes chemistry, Microspheres, Regeneration drug effects

Abstract

Dermatan sulfate (DS) is a glycosaminoglycan (GAG) with a great potential as a new therapeutic agent in tissue engineering. The aim of the present study was to investigate the formation of polyelectrolyte complexes (PECs) between chitosan and dermatan sulfate (CS/DS) and delivery of DS from PEC-containing alginate/chitosan/dermatan sulfate (Alg/CS/DS) microspheres for application in tissue regeneration. The CS/DS complexes were initially formed at different conditions including varying CS/DS ratio (positive/negative charge ratio), buffer, and pH. The obtained CS/DS complexes exhibited stronger electrostatic interaction, smaller complex size, and more stable colloidal structure when chitosan was in large excess (CS/DS 3:1) and prepared at pH 3.5 as compared to pH 5 using acetate buffer. The CS/DS complexes were subsequently incorporated into an alginate matrix by spray drying to form Alg/CS/DS composite microspheres with a DS encapsulation efficiency of 90-95%. The excessive CS induced a higher level of sustained DS release into Tris buffer (pH 7.4) from the microspheres formulated at pH 3.5; however, the amount of CS did not have a significant effect on the release from the microspheres formulated at pH 5. Significant cell proliferation was stimulated by the DS released from the microspheres in vitro. The present results provide a promising drug delivery strategy using PECs for sustained release of DS from microspheres intended for site-specific drug delivery and ultimately for use in tissue engineering.

Published

2012

4. Phosphorylation of alginate: synthesis, characterization, and evaluation of in vitro mineralization capacity.

Author

Coleman RJ, Lawrie G, Lambert LK, Whittaker M, Jack KS, and Grøndahl L

Subjects

Alginates chemical synthesis, Chromatography, Gel, Glucuronic Acid chemical synthesis, Glucuronic Acid chemistry, Hexuronic Acids chemical synthesis, Hexuronic Acids chemistry, Magnetic Resonance Spectroscopy, Phosphorylation, Spectroscopy, Fourier Transform Infrared, Alginates chemistry, Minerals chemistry

Abstract

Phosphorylation of alginate was achieved using a heterogeneous urea/phosphate reaction. The degree and stereoselectivity of phosphorylation as well as the effects on the physical properties of the polysaccharide were investigated by Fourier transform infrared (FTIR) and nuclear magnetic resonance (NMR) spectroscopies, inductively coupled plasma optical-emission spectroscopy (ICP-OES), and size exclusion chromatography (SEC). Multidimensional NMR studies of the phosporylated alginate revealed that phosphorylation of the M residues occurred predominantly at the C3 (equatorial) carbon of the polysaccharide ring. In addition, a more comprehensive assignment of the (1)H NMR spectrum of alginate, compared with those previously reported in the literature, is provided here. Hydrogel materials were formed from ionically cross-linked blends of phosphorylated alginate and alginate. These blended hydrogels showed an enhanced resistance to degradation by chelating agents compared with cross-linked alginate hydrogels and a reduction in their mineralization potential.

Published

2011

5. A novel strategy for preparing mechanically robust ionically cross-linked alginate hydrogels.

Author

Jejurikar A, Lawrie G, Martin D, and Grøndahl L

Subjects

Barium chemistry, Calcium chemistry, Cryoelectron Microscopy methods, Diffusion, Gels chemistry, Glucuronic Acid chemistry, Hexuronic Acids chemistry, Magnetic Resonance Spectroscopy methods, Materials Testing, Microscopy, Electron, Scanning methods, Models, Chemical, Spectroscopy, Fourier Transform Infrared methods, Tensile Strength, Alginates chemistry, Cross-Linking Reagents chemistry, Hydrogels chemistry, Ions

Abstract

The properties of alginate films modified using two cross-linker ions (Ca(2+) and Ba(2+)), comparing two separate cross-linking techniques (the traditional immersion (IM) method and a new strategy in a pressure-assisted diffusion (PD) method), are evaluated. This was achieved through measuring metal ion content, water uptake and film stability in an ionic solution ([Ca(2+)] = 2 mM). Characterization of the internal structure and mechanical properties of hydrated films were established by cryogenic scanning electron microscopy and tensile testing, respectively. It was found that gels formed by the PD technique possessed greater stability and did not exhibit any delamination after 21 day immersion as compared to gels formed by the IM technique. The Ba(2+) cross-linked gels possessed significantly higher cross-linking density as reflected in lower water content, a more dense internal structure and higher Young's modulus compared to Ca(2+) cross-linked gels. For the Ca(2+) cross-linked gels, a large improvement in the mechanical properties was observed in gels produced by the PD technique and this was attributed to thicker pore walls observed within the hydrogel structure. In contrast, for the Ba(2+) cross-linked gels, the PD technique resulted in gels that had lower tensile strength and strain energy density and this was attributed to phase separation and larger macropores in this gel.

Published

2011

6. Encapsulation of a glycosaminoglycan in hydroxyapatite/alginate capsules.

Author

Tan CS, Jejurikar A, Rai B, Bostrom T, Lawrie G, and Grøndahl L

Subjects

Bone and Bones metabolism, Capsules chemistry, Heparin chemistry, Humans, Hydrogel, Polyethylene Glycol Dimethacrylate chemistry, Hydrogels chemistry, Kinetics, Materials Testing, Stress, Mechanical, Viscosity, Alginates chemistry, Biocompatible Materials chemistry, Bone Substitutes, Durapatite chemistry, Glycosaminoglycans chemistry

Abstract

The development of suitable vehicles for the delivery of growth-inducing factors to fracture sites is a challenging area of bone repair. Bone-specific glycosaminoglycan molecules are of particular interest because of their high stability and proven effect on bone growth. Calcium alginate capsules are popular as delivery vehicles because of their low immunogenic response; they offer a versatile route that enables the controlled release of heparin (a member of the glycosaminoglycan family). In this study, hydroxyapatite (HA)/alginate composite capsules are explored as novel drug delivery vehicles for heparin, using both medium- and low-viscosity alginates. The composition, structure, and stability of the capsules are fully characterized and correlated to the release of heparin in vitro. Heparin is found to associate both with the alginate matrix through polymeric flocculation and also with the HA crystals in the composite beads. The mechanism by which heparin is released is dictated by the stability of the capsule in a particular release media and by the composition of the capsule. The use of medium-viscosity alginate is advantageous with respect to both drug loading and prolonging the release. The inclusion of HA increases the encapsulation efficiency, but because of its destabilizing effect to the alginate hydrogel matrix, it also increases the rate of heparin release. The bioactivity of heparin is fully retained throughout the assembly and release processes., (Copyright 2008 Wiley Periodicals, Inc.)

Published

2009

7. Interactions between alginate and chitosan biopolymers characterized using FTIR and XPS.

Author

Lawrie G, Keen I, Drew B, Chandler-Temple A, Rintoul L, Fredericks P, and Grøndahl L

Subjects

Biopolymers chemistry, Calcium Chloride chemistry, Glucuronic Acid chemistry, Hexuronic Acids chemistry, Spectroscopy, Fourier Transform Infrared, X-Rays, Alginates chemistry, Chitosan chemistry

Abstract

This study investigates alginate-chitosan polyelectrolyte complexes (PECs) in the form of a film, a precipitate, as well as a layer-by-layer (LbL) assembly. The focus of this study is to fully characterize, using the complementary techniques of Fourier transform infrared (FTIR) spectroscopy and X-ray photoelectron spectroscopy (XPS) in combination with solution stability evaluation, the interactions between alginate and chitosan in the PECs. In the FTIR spectra, no significant change in the band position of the two carbonyl vibrations from alginate occurs upon interaction with different ionic species. However, protonation of the carboxylate group causes a new band to appear at 1710 cm(-1), as anticipated. Partial protonation of the amine group of chitosan causes the appearance of one new band ( approximately 1530 cm(-1)) due to one of the -NH3+ vibrational modes (the other mode overlaps the amide I band). Importantly, the position of the two main bands in the spectral region of interest in partly protonated chitosan films is not dependent on the extent of protonation. XPS N 1s narrow scans can, however, be used to assess the degree of amine protonation. In our alginate-chitosan film, precipitate, and LbL assembly, the bands observed in the FTIR correspond to the species -COO- and -NH3+, but their position is not different from each of the single components. Thus, the conclusion of the study is that FTIR cannot be used directly to identify the presence of PECs. However, in combination with XPS (survey and narrow N 1s scans) and solution stability evaluation, a more complete description of the structure can be obtained. This conclusion challenges the assignment of FTIR spectra in the literature.

Published

2007