Your search keyword '"Berit L. Strand"' showing total 3 results

1. The induction of cytokines by polycation containing microspheres by a complement dependent mechanism

Author

John D. Lambris, Igor Lacík, Gudmund Skjåk-Bræk, Anne Mari Rokstad, Ole-Lars Brekke, Liv Ryan, Bjørg Steinkjer, Tom Eirik Mollnes, Terje Espevik, Gabriela Kolláriková, and Berit L. Strand

Subjects

Vascular Endothelial Growth Factor A, Chemokine, Materials science, Alginates, medicine.medical_treatment, Biophysics, Biocompatible Materials, Bioengineering, Inflammation, Guanidines, Peptides, Cyclic, Proinflammatory cytokine, Biomaterials, Polyamines, medicine, Humans, Polylysine, Complement Activation, Chemokine CCL3, biology, Interleukin-6, Interleukin-8, Complement C3, Polyelectrolytes, Molecular biology, Microspheres, C3-convertase, Interleukin-10, Cell biology, Complement system, Interleukin 1 Receptor Antagonist Protein, Interleukin 10, Cytokine, Mechanics of Materials, Tumor Necrosis Factors, Ceramics and Composites, biology.protein, Cytokines, Tumor necrosis factor alpha, Inflammation Mediators, medicine.symptom

Abstract

The cytokine-inducing potential of various microspheres were evaluated in a short-time screening assay of lepirudin-anticoagulated human whole blood utilizing the Bio-Plex Human cytokine 27-plex system. The inflammatory cytokines IL-1β, TNF and IL-6; the anti-inflammatory mediators IL-1ra and IL-10; the chemokines IL-8, MIP-1α and MCP-1; and the growth factor VEGF were induced by polycation (poly-l-lysine or poly(methylene-co-guanidine)) containing microspheres. Alginate microspheres without polycations did not induce the corresponding cytokine panel, nor did soluble alginate. By inhibiting complement C3 using compstatin analog CP20, a total inhibition of complement activation as well as the inflammatory mediators was achieved, indicating that complement activation alone was responsible for the induced cytokines. A strong deposition of C3c on the poly-l-lysine containing surface, while not on the microspheres lacking polycations, also points to the formation of C3 convertase as involved in the biomaterial-induced cytokine induction. These results show that complement is responsible for the induction of cytokines by polycation containing microspheres. We point to complement as an important initiator of inflammatory responses to biomaterials and the lepirudin anticoagulated whole blood assay as an important tool to identify the most tolerable and safe materials for implantation to humans.

Published

2013

2. Multiscale requirements for bioencapsulation in medicine and biotechnology

Author

Marijke M. Faas, Berit L. Strand, Peter Gemeiner, Alica Vikartovská, Marek Bučko, Dennis Poncelet, Gorka Orive, José Luis Pedraz, Marion B. Ansorge-Schumacher, Paul de Vos, Yrr A. Mørch, Igor Lacík, Juraj Svitel, Gudmund Skjåk-Bræk, Marian Navratil, and Gabriela Kolláriková

Subjects

Surface analysis, ASPERGILLUS-NIGER CELLS, Semipermeable membranes, Future studies, Alginates, Polymers, GEL BEADS, XPS (X-ray photoelectron spectroscopy), Biophysics, Capsules, ALGINATE-PLL CAPSULES, Bioengineering, Biology, Microbiology, Biomaterials, In vivo biocompatibility, CALCIUM-ALGINATE, Glucuronic Acid, Bioartificial pancreas, Animals, Humans, LIVING CELLS, Microencapsulation, L-LYSINE MICROCAPSULES, Biomedicine, business.industry, Hexuronic Acids, Dominant factor, PANCREATIC-ISLETS, Biocompatible material, Biotechnology, BACILLUS-SUBTILIS CELLS, Pharmaceutical Preparations, Mechanics of Materials, SIZE-EXCLUSION CHROMATOGRAPHY, Ceramics and Composites, Biocompatibility, business, IN-VIVO BIOCOMPATIBILITY

Abstract

Bioencapsulation involves the envelopment of tissues or biological active substances in semipermeable membranes. Bioencapsulation has been shown to be efficacious in mimicking the cell's natural environment and thereby improves the efficiency of production of different metabolites and therapeutic agents. The field of application is broad. It is being applied in bioindustry and biomedicine. it is clinically applied for the treatment of a wide variety of endocrine diseases. During the past decades many procedures to fabricate capsules have been described. Unfortunately, most of these procedures lack an adequate documentation of the characterization of the biocapsules. As a result many procedures show an extreme lab-to-lab variation and many results cannot be adequately reproduced. The characterization of capsules can no longer be neglected, especially since new clinical trials with bioencapsulated therapeutic cells have been initiated and the industrial application of bioencapsulation is growing. In the present review we discuss novel Approached to produce and characterize biocapsules in view of clinical and industrial application. A dominant factor in bioencapsulation is selection and characterization of suitable polymers. We present the adequacy of using high-resolution NMR for characterizing polymers. These polymers are applied for producing semipermeable membranes. We present the pitfalls of the currently applied methods and provide recommendations for standardization to avoid lab-to-lab variations. Also, we compare and present methodologies to produce biocompatible biocapsules for specific fields of applications and we demonstrate how physico-chemical technologies such as FT-IR, XPS, and TOF-SIMS contribute to reproducibility and standardization of the bioencapsulation process. During recent years it has become more and more clear that bioencapsulation requires a multidisciplinary approach in which biomedical, physical, and chemical technologies are combined. For adequate reproducibility and for understanding variations in outcome of biocapsules it is advisable if not mandatory to include the characterization processes presented in this review in future studies. Crown Copyright (C) 2009 Published by Elsevier Ltd. All rights reserved.

Published

2009

3. Cell-compatible covalently reinforced beads obtained from a chemoenzymatically engineered alginate

Author

Anne Mari Rokstad, Massimiliano Borgogna, Jose Oberholzer, Berit L. Strand, Ivan Donati, Gudmund Skjåk-Bræk, Terje Espevik, ROKSTAD A., M, Donati, Ivan, Borgogna, MASSIMILIANO ANTONIO, Oberholzer, J, STRAND B., L, Espevik, T, and SKJÅK BRÆK, G.

Subjects

Cell viability, Materials science, Alginate bead, Alginates, Cell Survival, Cell Transplantation, Cell, Biophysics, Alginate beads, Chemoenzymatic engineering, Photocross-linking, Stability, Islets, Cell Culture Techniques, Bioengineering, Biocompatible Materials, Methacrylate, Cell Line, Biomaterials, Myoblasts, Islets of Langerhans, Mice, Bioreactors, Drug Delivery Systems, Polymer chemistry, Insulin Secretion, Materials Testing, medicine, Bioreactor, Animals, Humans, Insulin, Viability assay, Tissue Engineering, Pancreatic islets, Chemical Engineering, Combinatorial chemistry, Microspheres, Enzymes, medicine.anatomical_structure, Cross-Linking Reagents, Polymerization, Mechanics of Materials, Covalent bond, Ceramics and Composites, C2C12

Abstract

A chemoenzymatic strategy has been exploited to make covalently linked alginate beads with high stability. This was achieved by grafting mannuronan (alginate with 100% mannuronic acid (M)) with methacrylate moieties and then performing two enzymatic steps converting M to guluronic acid (G) in alternating sequences (MG-blocks) and in G-blocks. In this way a methacrylate grafted alginate with better gel-forming ability was achieved. Covalent bindings were introduced into the beads by using a photoinitiating system that initiated polymerization of the methacrylate moieties. The covalent links were demonstrated by beads remaining intact after treatment with EDTA. The new chemoenzymatic photocrosslinked (CEPC) beads were compatible with cells with low post-encapsulation ability like C2C12 myoblasts and human pancreatic islets. The islets continued secreting insulin after encapsulation. On contrary, cells with a high post-encapsulation proliferative ability like 293-endo cells died within 2-week post-encapsulation. The exceptional stability and the cell compatibility of the new CEPC beads make them interesting as bioreactors for delivering therapeutic proteins in future applications.

Published

2005