Your search keyword '"Alain Despont"' showing total 4 results

1. The architecture of the IgG anti-carbohydrate repertoire in primary antibody deficiencies

Author

Richard D. Cummings, Mai M. Abdelhafez, Bodo Grimbacher, Robert Rieben, Peter Jandus, Camilla Jandus, Stephan von Gunten, Hans-Uwe Simon, Dagmar Simon, Kayluz Frias Boligan, David F. Smith, Elisabeth de Graauw, Nicolai V. Bovin, and Alain Despont

Subjects

Male, Glycan, Immunobiology and Immunotherapy, Primary Immunodeficiency Diseases, Immunology, Carbohydrates, 610 Medicine & health, medicine.disease_cause, Autoantigens, Biochemistry, Immunoglobulin G, Epitope, Autoimmunity, Epitopes, Immune system, Antibody Repertoire, Antigen, medicine, Humans, ddc:616, biology, Repertoire, Cell Biology, Hematology, biology.protein, Female

Abstract

Immune system failure in primary antibody deficiencies (PADs) has been linked to recurrent infections, autoimmunity, and cancer, yet clinical judgment is often based on the reactivity to a restricted panel of antigens. Previously, we demonstrated that the human repertoire of carbohydrate-specific immunoglobulin G (IgG) exhibits modular organization related to glycan epitope structure. The current study compares the glycan-specific IgG repertoires between different PAD entities. Distinct repertoire profiles with extensive qualitative glycan-recognition defects were observed, which are characterized by the common loss of Galα and GalNAc reactivity and disease-specific recognition of microbial antigens, self-antigens, and tumor-associated carbohydrate antigens. Antibody repertoire analysis may provide a useful tool to elucidate the degree and the clinical implications of immune system failure in individual patients.

Published

2019

2. 3D artificial round section micro-vessels to investigate endothelial cells under physiological flow conditions

Author

Robert Rieben, Riccardo Sfriso, Colette A. Bichsel, O. Steck, Shengye Zhang, Alain Despont, and Olivier T. Guenat

Subjects

0301 basic medicine, Swine, Xenotransplantation, medicine.medical_treatment, Transplantation, Heterologous, Cell Culture Techniques, Pulsatile flow, Gene Expression, lcsh:Medicine, 610 Medicine & health, Context (language use), 030230 surgery, Models, Biological, Article, law.invention, 03 medical and health sciences, 0302 clinical medicine, Confocal microscopy, law, Lab-On-A-Chip Devices, E-selectin, medicine, Animals, Humans, lcsh:Science, Complement Activation, Aorta, Microscopy, Confocal, Multidisciplinary, biology, Dextran Sulfate, lcsh:R, Endothelial Cells, Complement System Proteins, Complement system, Cell biology, Transplantation, Complement Inactivating Agents, 030104 developmental biology, Cell culture, Pulsatile Flow, biology.protein, Cytokines, Intercellular Signaling Peptides and Proteins, 570 Life sciences, lcsh:Q, E-Selectin, Rheology

Abstract

In the context of xenotransplantation, in ischemia/reperfusion injury as well as in cardiovascular research, the study of the fascinating interplay between endothelial cells (EC) and the plasma cascade systems often requires in vitro models. Blood vessels are hardly reproducible with standard flat-bed culture systems and flow-plate assays are limited in their low surface-to-volume ratio which impedes the study of the anticoagulant properties of the endothelial cells. According to the 3R regulations (reduce, replace and refine animal experimentation) we developed a closed circuit microfluidic in vitro system in which endothelial cells are cultured in 3D round section microchannels and subjected to physiological, pulsatile flow. In this study, a 3D monolayer of porcine aortic EC was perfused with human serum to mimic a xenotransplantation setting. Complement as well as EC activation was assessed in the presence or absence of complement inhibitors showing the versatility of the model for drug testing. Complement activation products as well as E-selectin expression were detected and visualized in situ by high resolution confocal microscopy. Furthermore, porcine pro-inflammatory cytokines as well as soluble complement components in the recirculating fluid phase were detected after human serum perfusion providing a better overview of the artificial vascular environment.

Published

2018

3. siRNA mediated knockdown of tissue factor expression in pigs for xenotransplantation

Author

Dennis Rataj, Andrea Lucas-Hahn, Ulrich Baulain, Sonja Werwitzke, Anjan K. Bongoni, Heiner Niemann, Hellen Ahrens, Robert Rieben, Joachim Denner, Reinhard Schwinzer, Doris Herrmann, Petra Hassel, Wiebke Baars, Alain Despont, Wilfried A. Kues, Andreas Tiede, Maren Ziegler, P. S. Garimella, and Bjoern Petersen

Subjects

Graft Rejection, Male, Xenotransplantation, medicine.medical_treatment, Sus scrofa, Transplantation, Heterologous, Down-Regulation, Biology, Thromboplastin, Animals, Genetically Modified, Tissue factor, Downregulation and upregulation, Testis, medicine, Animals, Humans, Immunology and Allergy, Gene silencing, Pharmacology (medical), RNA, Small Interfering, Blood Coagulation, Transplantation, Messenger RNA, Gene knockdown, Thrombosis, Transfection, Fibroblasts, Molecular biology, Genetic Techniques, Clotting time, RNA Interference

Abstract

Acute vascular rejection (AVR), in particular microvascular thrombosis, is an important barrier to successful pig-to-primate xenotransplantation. Here, we report the generation of pigs with decreased tissue factor (TF) levels induced by small interfering (si)RNA-mediated gene silencing. Porcine fibroblasts were transfected with TF-targeting small hairpin (sh)RNA and used for somatic cell nuclear transfer. Offspring were analyzed for siRNA, TF mRNA and TF protein level. Functionality of TF downregulation was investigated by a whole blood clotting test and a flow chamber assay. TF siRNA was expressed in all twelve liveborn piglets. TF mRNA expression was reduced by 94.1 ± 4.7% in TF knockdown (TFkd) fibroblasts compared to wild-type (WT). TF protein expression in PAEC stimulated with 50 ng/mL TNF-α was significantly lower in TFkd pigs (mean fluorescence intensity TFkd: 7136 ± 136 vs. WT: 13 038 ± 1672). TF downregulation significantly increased clotting time (TFkd: 73.3 ± 8.8 min, WT: 45.8 ± 7.7 min, p

Published

2015

4. S100A1 and S100B Expression Patterns Identify Differentiation Status of Human Articular Chondrocytes

Author

Chantal Pauli, Alain Despont, Jose Diaz-Romero, Matthias A. Zumstein, Dobrila Nesic, Aurelie Quintin, Eric Schoenholzer, and Sandro Kohl

Subjects

medicine.diagnostic_test, Physiology, Cartilage, Cellular differentiation, Regeneration (biology), Clinical Biochemistry, Cell Biology, Biology, Chondrogenesis, Molecular biology, S100 protein, medicine.anatomical_structure, Western blot, Gene expression, medicine, Aggrecan

Abstract

Many studies in the field of cell-based cartilage repair have focused on identifying markers associated with the differentiation status of human articular chondrocytes (HAC) that could predict their chondrogenic potency. A previous study from our group showed a correlation between the expression of S100 protein in HAC and their chondrogenic potential. The aims of the current study were to clarify which S100 proteins are associated with HAC differentiation status and to provide an S100-based assay for measuring HAC chondrogenic potential. The expression patterns of S100A1 and S100B were investigated in cartilage and in HAC cultured under conditions promoting dedifferentiation (monolayer culture) or redifferentiation (pellet culture or BMP4 treatment in monolayer culture), using characterized antibodies specifically recognizing S100A1 and S100B, by immunohistochemistry, immunocytochemistry, Western blot, and gene expression analysis. S100A1 and S100B were expressed homogeneously in all cartilage zones, and decreased during dedifferentiation. S100A1, but not S100B, was re-expressed in pellets and co-localized with collagen II. Gene expression analysis revealed concomitant modulation of S100A1, S100B, collagen type II, and aggrecan: down-regulation during monolayer culture and up-regulation upon BMP4 treatment. These results strongly support an association of S100A1, and to a lesser extent S100B, with the HAC differentiated phenotype. To facilitate their potential application, we established an S100A1/B-based flow cytometry assay for accurate assessment of HAC differentiation status. We propose S100A1 and S100B expression as a marker to develop potency assays for cartilage regeneration cell therapies, and as a redifferentiation readout in monolayer cultures aiming to investigate stimuli for chondrogenic induction.

Published

2014