Your search keyword '"Korevaar, Sander S."' showing total 16 results

1. Interactions of the Immune System with Human Kidney Organoids.

Author

Shankar, Anusha S., Tejeda-Mora, Hector, Zhaoyu Du, Nlandu, Quincy, Palomares-Cabeza, Virginia, van den Bosch, Thierry P. P., Korevaar, Sander S., Da Costa Gonçalves, Fabiany, Bindels, Eric M. J., Kramann, R., Reinders, Marlies E. J., Clahsen-van Groningen, Marian C., Hoorn, Ewout J., Gribnau, Joost, Baan, Carla C., and Hoogduijn, Martin J.

Subjects

*MONONUCLEAR leukocytes, *ORGANOIDS, *IMMUNE system, *KIDNEYS

Abstract

Kidney organoids are an innovative tool in transplantation research. The aim of the present study was to investigate whether kidney organoids are susceptible for allo-immune attack and whether they can be used as a model to study allo-immunity in kidney transplantation. Human induced pluripotent stem cell-derived kidney organoids were co-cultured with human peripheral blood mononuclear cells (PBMC), which resulted in invasion of allogeneic T-cells around nephron structures and macrophages in the stromal cell compartment of the organoids. This process was associated with the induction of fibrosis. Subcutaneous implantation of kidney organoids in immune-deficient mice followed by adoptive transfer of human PBMC led to the invasion of diverse T-cell subsets. Single cell transcriptomic analysis revealed that stromal cells in the organoids upregulated expression of immune response genes upon immune cell invasion. Moreover, immune regulatory PD-L1 protein was elevated in epithelial cells while genes related to nephron differentiation and function were downregulated. This study characterized the interaction between immune cells and kidney organoids, which will advance the use of kidney organoids for transplantation research. [ABSTRACT FROM AUTHOR]

Published

2024

2. The Importance of Dosing, Timing, and (in)Activation of Adipose Tissue-Derived Mesenchymal Stromal Cells on Their Immunomodulatory Effects.

Author

Lee, Olivia J., Luk, Franka, Korevaar, Sander S., Koch, Thomas G., Baan, Carla C., Merino, Ana, and Hoogduijn, Martin J.

Subjects

*STROMAL cells, *TREATMENT effectiveness, *CLINICAL trials, *CELLULAR therapy, *ADIPOSE tissues, *LUNGS

Abstract

Mesenchymal stromal cells (MSCs) are attractive candidates for immunomodulatory cell therapy. However, it remains unknown how far therapeutic efficacy and potency are dependent on the dosage and activity of the MSCs. We previously observed that infusion of MSCs leads to rapid and transient changes in cytokine expression in blood, lung, and liver. In the present study, increasing doses of syngeneic adipose tissue-derived MSCs were infused in healthy mice and systemic changes in G-CSF, IL6, IL-10, and CXCL5 were detected 2 h after administration of 3 × 105 MSCs per animal, but not at lower doses. In lung and liver tissue, dose-dependent effects of MSCs on cytokine mRNA expression levels were detected from doses as low as 3 × 103 MSCs. Infusion of secretome-deficient or IFNγ-activated MSCs in healthy mice had similar effects on systemic cytokine levels as control MSCs, suggesting that in vivo at least the initial systemic effect of MSC administration is independent of the level of activity of MSCs, but depends on the response of host cells to MSCs. The results of this study reveal a rapid dose-dependent effect of MSCs and stress the important role of host cells in MSC treatment. This knowledge contributes to the design of rational MSC trials and to the quest for clinical efficacy of MSC therapy. [ABSTRACT FROM AUTHOR]

Published

2020

3. Inactivated Mesenchymal Stem Cells Maintain Immunomodulatory Capacity.

Author

Luk, Franka, de Witte, Samantha F. H., Korevaar, Sander S., Franquesa, Marcella, Strini, Tanja, Betjes, Michiel G. H., Baan, Carla C., Hoogduijn, Martin J., Rhijn, Marieke Roemeling-van, van den Engel, Sandra, Dor, Frank J. M. F., de Bruin, Ron W. F., Gargesha, Madhusudhana, Roy, Debashish, and Horwitz, Edwin M.

Subjects

*MESENCHYMAL stem cells, *IMMUNOREGULATION, *IMMUNOLOGIC diseases, *MACROPHAGES, *IMMUNOSUPPRESSION, *THERAPEUTICS

Abstract

Mesenchymal stem cells (MSC) are studied as a cell therapeutic agent for treatment of various immune diseases. However, therapy with living culture-expanded cells comes with safety concerns. Furthermore, development of effective MSC immunotherapy is hampered by lack of knowledge of the mechanisms of action and the therapeutic components ofMSC. Such knowledge allows better identification of diseases that are responsive toMSC treatment, optimization of the MSC product, and development of therapy based on functional components ofMSC. To close in on the components that carry the therapeutic immunomodulatory activity of MSC, we generated MSC that were unable to respond to inflammatory signals or secrete immunomodulatory factors, but preserved their cellular integrity [heat-inactivated MSC (HI-MSC)]. Secretome-deficient HI-MSC and control MSC showed the same biodistribution and persistence after infusion in mice with ischemic kidney injury. Both control andHI-MSC induced mild inflammatory responses in healthy mice and dramatic increases in interleukin-10, and reductions in interferon gamma levels in sepsis mice. In vitro experiments showed that opposite to control MSC, HI-MSC lacked the capability to suppress T-cell proliferation or induce regulatory B-cell formation. However, both HI-MSC and control MSC modulated monocyte function in response to lipopolysaccharides. The results of this study demonstrate that, in particular diseasemodels, the immunomodulatory effect of MSC does not depend on their secretome or active crosstalk with immune cells, but on recognition ofMSC by monocytic cells. These findings provide a new view on MSCinduced immunomodulation and help identify key components of the therapeutic effects of MSC. [ABSTRACT FROM AUTHOR]

Published

2016

4. The effect of rabbit antithymocyte globulin on human mesenchymal stem cells.

Author

Franquesa, Marcella, Baan, Carla C., Korevaar, Sander S., Engela, Anja U., Roemeling-van Rhijn, Marieke, Weimar, Willem, Betjes, Michiel G. H., Grinyo, Josep M., and Hoogduijn, Martin J.

Subjects

*MESENCHYMAL stem cells, *AUTOIMMUNITY, *GLOBULINS, *CD8 antigen, *T cells

Abstract

Mesenchymal stem cells ( MSCs) possess immunomodulatory properties which are of key interest for their application in autoimmunity and transplantation. In transplantation, administration of MSCs has shown promising results in preclinical models and has recently moved to clinical trials. Therefore, it is important to study the interactions between MSCs and immunosuppressive drugs currently used in transplantation. We aimed to analyze the effect of rabbit antithymocyte globulin ( rATG) MSCs. MSCs were obtained from perirenal fat of kidney donors and exposed to ranging doses of rATG (Thymoglobulin®, Genzyme; 0.5-100 μg/ml). Binding of rATG, effects on viability and susceptibility to be killed by cytotoxic lymphocytes as well as effects on their immunosuppressive potential of MSCs were tested. rATG binds dose-dependently to MSCs. This binding was associated with slightly impaired viability after 48 and 72 h when compared with nonexposed MSCs. In contrast to nontreated MSCs, rATG preexposed MSCs were susceptible to be lysed by cytokine-activated CD8+ cytotoxic cells and NKT cells. The capacity of MSCs to suppress the proliferation of anti-CD3/CD28 activated CD4 and CD8 T cells were reduced by the presence of rATG in the culture. rATG reduces the viability and antiproliferative capacity of MSCs in a dose-dependent manner and converts them into targets for CD8 T cells and NKT cell lysis. [ABSTRACT FROM AUTHOR]

Published

2013

5. FOXP3 mRNA expression analysis in the peripheral blood and allograft of heart transplant patients.

Author

Dijke, I. Esmé, Caliskan, Kadir, Korevaar, Sander S., Maat, Alex P. W. M., Zondervan, Pieter E., Balk, Aggie H. M. M., Weimar, Willem, and Baan, Carla C.

Subjects

*HEART transplantation, *GENE expression, *BIOPSY, *MESSENGER RNA, *HOMOGRAFTS, *T cells

Abstract

Previously, we demonstrated in heart transplant patients that FOXP3, a gene required for the development and function of regulatory T cells, was highly expressed in the graft during an acute cellular rejection. In this study, we analyzed whether the FOXP3 gene expression in the peripheral blood also reflects anti-donor immune responses, and therefore may provide clues for non-invasive detection of non-responsiveness or acute rejection. We examined the FOXP3 expression patterns of peripheral blood mononuclear cells (PBMC; n = 69) of 19 heart transplant patients during quiescence and rejection in comparison with those of endomyocardial biopsies (EMB; n=75) of 24 heart transplant patients. While the FOXP3 mRNA levels were abundantly expressed in rejecting EMB (ISHLT rejection grade > 1R) compared with EMB without histological evidence of myocardial damage (ISHLT rejection grade OR-1R; p=O.OO3), no association with rejection or non-responsiveness was found for the FOXP3 mRNA levels in the peripheral blood. Thus, in contrast to intragraft FOXP3 gene expression, the peripheral FOXP3 mRNA levels lack correlation with anti-donor immune responses in the graft, and, consequently, FOXP3 does not appear to be a potential candidate gene for non- invasive diagnosis of non-responsiveness or rejection. [ABSTRACT FROM AUTHOR]

Published

2008

6. Vitamin D metabolism in human kidney organoids.

Author

Shankar, Anusha S, Berg, Sjoerd A A van den, Mora, Hector Tejeda, Du, Zhaoyu, Lin, Hui, Korevaar, Sander S, van der Wal, Ronald, Bosch, Thierry P P van den, Groningen, Marian C Clahsen-van, Gribnau, Joost, Hoorn, Ewout J, Baan, Carla C, and Hoogduijn, Martin J

Subjects

*VITAMIN D metabolism, *ORGANOIDS, *ERGOCALCIFEROL, *KIDNEYS, *CHOLECALCIFEROL, *VITAMIN D receptors

Published

2022

7. Identification of Predictive Markers for the Generation of Well-Differentiated Human Induced Pluripotent Stem Cell-Derived Kidney Organoids.

Author

Du, Zhaoyu, Shankar, Anusha S., van den Bosch, Thierry P.P., Korevaar, Sander S., Clahsen-van Groningen, Marian, Hoorn, Ewout J., Gribnau, Joost, Reinders, Marlies E.J., Baan, Carla C., and Hoogduijn, Martin J.

Subjects

*PLURIPOTENT stem cells, *FIBROBLAST growth factor 2, *ORGANOIDS, *KIDNEY development, *PROXIMAL kidney tubules, *KIDNEYS, *INDUCED pluripotent stem cells

Abstract

Human-induced pluripotent stem cell (iPSC)-derived kidney organoids have the potential to advance studies to kidney development and disease. However, reproducible generation of kidney organoids is a challenge. A large variability in the percentage of nephron structures and the expression of kidney-specific genes was observed among organoids, showing no association with iPSC lines. To associate the quality of kidney organoid differentiation with predictive markers, a ranking system was developed based on the ratio of nephron structure determined by histological examination. Well-differentiated organoids were defined as organoids with >30% nephron structure and vice versa. Subsequently, correlations were made with expression profiles of iPSC markers, early kidney development markers, and fibrosis markers. Higher expression of sex-determining region Y-box 2 (SOX2) during differentiation was associated with poorly differentiated kidney organoid. Furthermore, early secretion of basic fibroblast growth factor (FGF2) predicted poorly differentiated kidney organoid. Of interest, whereas cadherin-1 (CDH1) expression in kidney organoids indicates distal tubules formation, onefold higher CDH1 expression in iPSC predicted poor differentiation. High expression of the stromal progenitor marker Forkhead Box D1 (FOXD1) and significantly increased TGFβ levels were found in well-differentiated kidney organoids. These early expression profiles could predict the outcome of kidney organoid formation. This study helps to improve the robustness of kidney organoid protocols. [ABSTRACT FROM AUTHOR]

Published

2021

8. Membrane particles from mesenchymal stromal cells reduce the expression of fibrotic markers on pulmonary cells.

Author

Merino, Ana, Hoogduijn, Martin J., Molina-Molina, Maria, Arias-Salgado, Elena G., Korevaar, Sander S., Baan, Carla C., and Montes-Worboys, Ana

Subjects

*STROMAL cells, *IDIOPATHIC pulmonary fibrosis, *PULMONARY fibrosis, *MYOFIBROBLASTS, *LUNG diseases, *TELOMERES

Abstract

Background: Idiopathic pulmonary fibrosis (IPF) is a devastating lung disease with limited treatment options in which the telomere shortening is a strong predictive factor of poor prognosis. Mesenchymal stromal cells (MSC) administration is probed in several experimental induced lung pathologies; however, MSC might stimulate fibrotic processes. A therapy that avoids MSC side effects of transformation would be an alternative to the use of living cells. Membranes particles (MP) are nanovesicles artificially generated from the membranes of MSC containing active enzymes involved in ECM regeneration. We aimed to investigate the anti-fibrotic role of MP derived from MSC in an in vitro model of pulmonary fibrosis. Methods: Epithelial cells (A549) and lung fibroblasts, from IPF patients with different telomere length, were co-cultured with MP and TGF-β for 48h and gene expression of major pro-fibrotic markers were analyzed. Results: About 90% of both types of cells effectively took up MP without cytotoxic effects. MP decreased the expression of profibrotic proteins such as Col1A1, Fibronectin and PAI-1, in A549 cells. In fibroblasts culture, there was a different response in the inhibitory effect of MP on some pro-fibrotic markers when comparing fibroblast from normal telomere length patients (FN) versus short telomere length (FS), but both types showed an inhibition of Col1A1, Tenascin-c, PAI-1 and MMP-1 gene expression after MP treatment. Conclusions: MP conserve some of the properties attributed to the living MSC. This study shows that MP target lung cells, via which they may have a broad anti-fibrotic effect. [ABSTRACT FROM AUTHOR]

Published

2021

9. Epigenetic changes in umbilical cord mesenchymal stromal cells upon stimulation and culture expansion.

Author

De Witte, Samantha F.H., Peters, Fleur S., Merino, Ana, Korevaar, Sander S., Van Meurs, Joyce B.J., O'Flynn, Lisa, Elliman, Steve J., Newsome, Philip N., Boer, Karin, Baan, Carla C., and Hoogduijn, Martin J.

Subjects

*STROMAL cells, *MESENCHYMAL stem cells, *UMBILICAL cord, *EPIGENETICS, *TRANSFORMING growth factors

Abstract

Abstract Background Mesenchymal stromal cells (MSCs) are studied for their immunotherapeutic potential. Prior to therapeutic use, MSCs are culture expanded to obtain the required cell numbers and, to improve their efficacy, MSCs may be primed in vitro. Culture expansion and priming induce phenotypical and functional changes in MSCs and thus standardisation and quality control measurements come in need. We investigated the impact of priming and culturing on MSC DNA methylation and examined the use of epigenetic profiling as a quality control tool. Methods Human umbilical cord–derived MSCs (ucMSCs) were cultured for 3 days with interferon (IFN)γ, transforming growth factor (TGF)β or a multi-factor combination (MC; IFNγ, TGFβ and retinoic acid). In addition, ucMSCs were culture expanded for 14 days. Phenotypical changes and T-cell proliferation inhibition capacity were examined. Genome-wide DNA methylation was measured with Infinium MethylationEPIC Beadchip. Results Upon priming, ucMSCs exhibited a different immunophenotype and ucMSC(IFNγ) and ucMSC(MC) had an increased capacity to inhibit T-cell proliferation. DNA methylation patterns were minimally affected by priming, with only one significantly differentially methylated site (DMS) in IFNγ- and MC-primed ucMSCs associated with autophagy activity. In contrast, 14 days after culture expansion, ucMSCs displayed minor phenotypical and functional changes but showed >4000 significantly DMSs, mostly concerning genes involved in membrane composition, cell adhesion and transmembrane signalling. Discussion These data show that DNA methylation of MSCs is only marginally affected by priming, whereas culture expansion and subsequent increased cellular interactions have a large impact on methylation. On account of this study, we suggest that DNA methylation analysis is a useful quality control tool for culture expanded therapeutic MSCs. [ABSTRACT FROM AUTHOR]

Published

2018

10. Cytokine treatment optimises the immunotherapeutic effects of umbilical cord-derived MSC for treatment of inflammatory liver disease.

Author

de Witte, Samantha F. H., Merino, Ana M., Franquesa, Marcella, Strini, Tanja, van Zoggel, Johanna A. A., Korevaar, Sander S., Luk, Franka, Gargesha, Madhu, O'Flynn, Lisa, Roy, Debashish, Elliman, Steve J., Newsome, Philip N., Baan, Carla C., and Hoogduijn, Martin J.

Subjects

*THERAPEUTIC use of cytokines, *LIVER diseases, *IMMUNOLOGICAL adjuvants, *INTERLEUKINS, *VITAMINS

Abstract

Background: Mesenchymal stromal cells (MSC) possess immunomodulatory properties and low immunogenicity, both crucial properties for their development into an effective cellular immunotherapy. They have shown benefit in clinical trials targeting liver diseases; however the efficacy of MSC therapy will benefit from improvement of the immunomodulatory and immunogenic properties of MSC. Methods: MSC derived from human umbilical cords (ucMSC) were treated for 3 days in vitro with various inflammatory factors, interleukins, vitamins and serum deprivation. Their immunogenicity and immunomodulatory capacity were examined by gene-expression analysis, surface-marker expressions, IDO activity, PGE2 secretion and inhibition of T cell proliferation and IFNΥ production. Furthermore, their activation of NK cell cytotoxicity was investigated via CD107a expression on NK cells. The immunomodulatory capacity, biodistribution and survival of pre-treated ucMSC were investigated in a CCl4-induced liver disease mouse model. In addition, capacity of pre-treated MSC to ameliorate liver inflammation was examined in an ex vivo liver inflammation co-culture model. Results: IFN-Υ and a multiple cytokine cocktail (MC) consisting of IFN-Υ, TGFβ and retinoic acid upregulated the expression of immunomodulatory factor PD-L1 and IDO activity. Subsequently, both treatments enhanced the capacity of ucMSC to inhibit CD4 and CD8 T cell proliferation and IFN-Υ production. The susceptibility of ucMSC for NK cell lysis was decreased by IFN-β, TGFβ and MC treatment. In vivo, no immunomodulation was observed by the ucMSC. Four hours after intravenous infusion in mice with CCl4-induced inflammatory liver injury, the majority of ucMSC were trapped in the lungs. Rapid clearance of ucMSC(VitB6), ucMSC(Starv + VitB6) and ucMSC(MC) and altered bio-distribution of ucMSC(TGFβ) compared to untreated ucMSC was observed. In the ex vivo co-culture system with inflammatory liver slices ucMSC(MC) showed significantly enhanced modulatory capacity compared to untreated ucMSC. Conclusions: The present study demonstrates the responsiveness of ucMSC to in vitro optimisation treatment. The observed improvements in immunomodulatory capacity as well as immunogenicity after MC treatment may improve the efficacy of ucMSC as immunotherapy targeted towards liver inflammation [ABSTRACT FROM AUTHOR]

Published

2017

11. Adipose Tissue-Derived Mesenchymal Stem Cells Have a Heterogenic Cytokine Secretion Profile.

Author

Wu, Yongkang, Hoogduijn, Martin J., Baan, Carla C., Korevaar, Sander S., Kuiper, Ronella de, Yan, Lin, Wang, Lanlan, and Besouw, Nicole M. van

Subjects

*MESENCHYMAL stem cells, *IMMUNOMODULATORS, *CELLULAR therapy, *INTERLEUKIN-6, *ADIPOSE tissues, *FLOW cytometry, *THERAPEUTICS

Abstract

Mesenchymal stem cells derived from adipose tissue (ASC) have immune regulatory function, which makes them interesting candidates for cellular therapy. ASC cultures are however heterogeneous in phenotype. It is unclear whether all ASC contribute equally to immunomodulatory processes. ASC are also responsive to cytokine stimulation, which may affect the ratio between more and less potent ASC populations. In the present study, we determined IL-6 receptor (CD126 and CD130 subunits) and IFN-γ receptor (CD119) expression on ASC by flow cytometry. The production of IL-6 and IFN-γ was measured by ELISA and the frequency of IL-6 and IFN-γ secreting cells by ELISPOT. The results showed that ASC did not express CD126, and only 10–20% of ASC expressed CD130 on their surface, whereas 18–31% of ASC expressed CD119. ASC produced high levels of IL-6 and 100% of ASC were capable of secreting IL-6. Stimulation by IFN-γ or TGF-β had no effect on IL-6 secretion by ASC. IFN-γ was produced by only 1.4% of ASC, and TGF-β significantly increased the frequency to 2.7%. These results demonstrate that ASC cultures are heterogeneous in their cytokine secretion and receptor expression profiles. This knowledge can be employed for selection of potent, cytokine-producing, or responsive ASC subsets for cellular immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2017

12. Effects of Freeze-Thawing and Intravenous Infusion on Mesenchymal Stromal Cell Gene Expression.

Author

Hoogduijn, Martin J., de Witte, Samantha F.H., Luk, Franka, van den Hout-van Vroonhoven, Mirjam C.G.N., Ignatowicz, Lech, Catar, Rusan, Strini, Tanja, Korevaar, Sander S., van IJcken, Wilfred F.J., Betjes, Michiel G.H., Franquesa, Marcella, Moll, Guido, and Baan, Carla C.

Subjects

*INTRAVENOUS therapy, *MESENCHYMAL stem cells, *IMMUNOLOGIC diseases, *DEGENERATION (Pathology), *IMMUNOLOGY, *THERAPEUTICS

Abstract

Mesenchymal stromal cells (MSC) are increasingly used as an investigative therapeutic product for immune disorders and degenerative disease. Typically, MSC are isolated from human tissue, expanded in culture, and cryopreserved until usage. The safety and efficacy of MSC therapy will depend on the phenotypical and functional characteristics of MSC. The freeze-thawing procedure may change these characteristics. Furthermore, the cells encounter a microenvironment after administration that may impact their properties. It has been demonstrated that the majority of MSC localize to the lungs after intravenous infusion, making this the site to study the effects of the in vivo milieu on administered MSC. In this study, we investigated the effect of freeze-thawing and the mouse lung microenvironment on human adipose tissue-derived MSC. There were effects of freeze-thawing on the whole genome expression profile of MSC, although the effects did not exceed interdonor differences. There were no major changes in the expression of hemostatic regulators on transcriptional level, but significantly increased expression of procoagulant tissue factor on the surface of thawed adipose MSC, correlating with increased procoagulant activity of thawed cells. Exposure for 2 h to the lung microenvironment had a major effect on MSC gene expression and affected several immunological pathways. This indicates that MSC undergo functional changes shortly after infusion and this may influence the efficacy of MSC to modulate inflammatory responses. The results of this study demonstrate that MSC rapidly alter in response to the local milieu and disease-specific conditions may shape MSC after administration. [ABSTRACT FROM AUTHOR]

Published

2016

13. No Evidence for Circulating Mesenchymal Stem Cells in Patients with Organ Injury.

Author

Hoogduijn, Martin J., Verstegen, Monique M.A., Engela, Anja U., Korevaar, Sander S., Roemeling-van Rhijn, Marieke, Merino, Ana, Franquesa, Marcella, de Jonge, Jeroen, Ijzermans, Jan N., Weimar, Willem, Betjes, Michiel G.H., Baan, Carla C., and van der Laan, Luc J.W.

Subjects

*MESENCHYMAL stem cells, *ORGANS (Anatomy), *IMMUNOREGULATION, *CELL migration, *TRANSPLANTATION of organs, tissues, etc., *WOUNDS & injuries

Abstract

Mesenchymal stem cells (MSC) are present in the bone marrow, from where they are thought to migrate through the blood stream to the sites of injury. However, virtually all tissues contain resident MSC that may contribute to local regenerative and immunomodulatory processes, thereby hypothetically preempting the need for recruiting MSC through the bloodstream. Although there is some indication for circulating MSC in animal models, there is little solid evidence for the mobilization and migration of MSC in the human circulation. In the present study, we were unable to detect MSC in the blood of healthy individuals. We then searched for MSC in the blood of ten patients with end-stage renal disease, ten patients with end-stage liver disease, and in eight heart transplant patients with biopsy-proven rejection by culturing of mononuclear cells under MSC-supporting culture conditions. In none of these patient categories, MSC were identified in the blood. MSC were, however, found in the blood of a severe trauma patient with multiple fractures, suggesting that disruption of bone marrow leads to the release of MSC into the blood stream. The conclusion of this study is that MSC are not recruited into the circulation in patients with injured solid organs and during aggressive immune responses after transplantation. [ABSTRACT FROM AUTHOR]

Published

2014

14. Mesenchymal Stem Cells Induce an Inflammatory Response After Intravenous Infusion.

Author

Hoogduijn, Martin J., Roemeling-van Rhijn, Marieke, Engela, Anja U., Korevaar, Sander S., Mensah, Fane K. F., Franquesa, Marcella, de Bruin, Ron W. F., Betjes, Michiel G. H., Weimar, Willem, and Baan, Carla C.

Subjects

*MESENCHYMAL stem cells, *INFLAMMATION, *INTRAVENOUS therapy, *IMMUNOSUPPRESSIVE agents, *LIPOPOLYSACCHARIDES, *AUTOIMMUNE diseases, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Mesenchymal stem cells (MSCs) have potent immunosuppressive effects in vitro and are considered as a therapeutic option for autoimmune disease and organ transplantation. While MSCs show beneficial effects on immune disease progression and transplant survival in animal models, the immunomodulatory mechanisms involved are largely unknown. In the present study, we show that intravenously infused C57BL/6- green fluorescent protein (GFP) MSCs home to the lungs in C57BL/6 recipient mice and induce an inflammatory response. This response was characterized by increased mRNA expression of monocyte chemoattractant protein- 1 (MCP1), IL1-β, and TNF-α and an increase in macrophages in lung tissue 2 h after MSC infusion. Simultaneously, serum levels of proinflammatory IL6, CXCL1, and MCP1 protein increased, demonstrating systemic immune activation after MSC infusion. In liver tissue, no C57BL/6-GFP MSCs were detected, but MCP1 and TNF-α mRNA levels peaked 4 h after MSC infusion. The expression of the anti-inflammatory cytokines TGF-β, IL4, and IL10 was only marginally affected. Nevertheless, 3 days after MSC infusion, animals developed a milder inflammatory response to lipopolysaccharides. Our results suggest that the in vivo immunomodulatory effects of MSCs originate from an inflammatory response that is induced by the infusion of MSCs, which is followed by a phase of reduced immune reactivity. [ABSTRACT FROM AUTHOR]

Published

2013

15. Mesenchymal stem cells derived from adipose tissue are not affected by renal disease.

Author

Roemeling-van Rhijn, Marieke, Reinders, Marlies E J, de Klein, Annelies, Douben, Hannie, Korevaar, Sander S, Mensah, Fane K F, Dor, Frank J M F, IJzermans, Jan N M, Betjes, Michiel G H, Baan, Carla C, Weimar, Willem, and Hoogduijn, Martin J

Subjects

*MESENCHYMAL stem cells, *ADIPOSE tissues, *IMMUNOSUPPRESSION, *CHRONIC kidney failure, *KIDNEY transplantation, *UREMIA

Abstract

Mesenchymal stem cells are a potential therapeutic agent in renal disease and kidney transplantation. Autologous cell use in kidney transplantation is preferred to avoid anti-HLA reactivity; however, the influence of renal disease on mesenchymal stem cells is unknown. To investigate the feasibility of autologous cell therapy in patients with renal disease, we isolated these cells from subcutaneous adipose tissue of healthy controls and patients with renal disease and compared them phenotypically and functionally. The mesenchymal stem cells from both groups showed similar morphology and differentiation capacity, and were both over 90% positive for CD73, CD105, and CD166, and negative for CD31 and CD45. They demonstrated comparable population doubling times, rates of apoptosis, and were both capable of inhibiting allo-antigen- and anti-CD3/CD28-activated peripheral blood mononuclear cell proliferation. In response to immune activation they both increased the expression of pro-inflammatory and anti-inflammatory factors. These mesenchymal stem cells were genetically stable after extensive expansion and, importantly, were not affected by uremic serum. Thus, mesenchymal stem cells of patients with renal disease have similar characteristics and functionality as those from healthy controls. Hence, our results indicate the feasibility of their use in autologous cell therapy in patients with renal disease. [ABSTRACT FROM AUTHOR]

Published

2012

16. Donor-specific Cytotoxic Hyporesponsiveness Associated With High Interleukin-10 Messenger RNA Expression in Cardiac Allograft Patients

Author

Dijke, I. Esmé, Velthuis, Jurjen H.L., Balk, Aggie H.M.M., Korevaar, Sander S., Maat, Alex P.W.M., Weimar, Willem, and Baan, Carla C.

Subjects

*INTERLEUKIN-10, *CD4 antigen, *MESSENGER RNA, *HOMOGRAFTS, *HEART transplant recipients

Abstract

Background: After transplantation, CD4+CD25+FOXP3+ and interleukin (IL) 10-producing regulatory cells might regulate immune responses toward donor antigens. In this study, we determined whether cardiac allograft recipients show donor-specific hyporesponsiveness and studied the underlying mechanisms. Methods: We analyzed the donor-specific T-cell responses by mixed lymphocyte reactions and limiting dilution assays to define whether cardiac allograft recipients (n = 21) show proliferative and cytotoxic hyporesponsiveness to donor antigens long after transplantation (range, 1.5–7 years). The mechanisms controlling immune responses, that is, FOXP3+/GITR+ T cells, and IL-10–producing cells, were studied by quantitative real-time polymerase chain reaction. Results: In the presence of a proliferative response to donor antigens, no cytotoxic responsiveness could be measured in a number of patients in the absence (73%) and presence of exogenous IL-2 (29%), IL-15 (31%), and IL-15 plus IL2Rα blockade (88%). Overall, the cytotoxic response to donor cells was significantly lower than the reactivity to third-party cells after the addition of IL-2 (p = 0.004) and IL-15 plus IL2Rα blockade (p < 0.001). After donor stimulation, the peripheral blood mononuclear cells expressed higher messenger RNA (mRNA) levels of IL-10, but not of FOXP3 or GITR, than after third-party stimulation (p = 0.003). Moreover, the IL-10 mRNA expression was inversely correlated with the donor-specific cytotoxic responsiveness (p = 0.01). Conclusions: A significant proportion of patients showed donor-specific cytotoxic hyporesponsiveness long after heart transplantation, which was associated with high mRNA levels of IL-10 but not of FOXP3 or GITR. This observation suggests that IL-10–producing cells participate in the donor-specific cytotoxic hyporeactivity. [Copyright &y& Elsevier]

Published

2006