Search

Your search keyword '"Samsom J"' showing total 96 results
Start Over Author "Samsom J" Search Limiters Full Text
96 results on '"Samsom J"'

1. IL-10 signaling in dendritic cells controls IL-1β-mediated IFNγ secretion by human CD4+ T cells: relevance to inflammatory bowel disease

Author

Veenbergen, S., Li, P., Raatgeep, H. C., Lindenbergh-Kortleve, D. J., Simons-Oosterhuis, Y., Farrel, A., Costes, L. M. M., Joosse, M. E., van Berkel, L. A., de Ruiter, L. F., van Leeuwen, M. A., Winter, D., Holland, S. M., Freeman, A. F., Wakabayashi, Y., Zhu, J., de Ridder, L., Driessen, G. J., Escher, J. C., Leonard, W. J., and Samsom, J. N.

Published
2019
Full Text
View/download PDF

4. TGFβR signalling determines CD103+CD11b+ dendritic cell development in the intestine

Author

Bain, C. C., Montgomery, J., Scott, C L, Kel, J M, Girard-Madoux, M J H, Martens, L, Zangerle-Murray, T F P, Ober-Blobaum, J, Lindenbergh-Kortleve, D, Samsom, J N, Henri, S., Lawrence, T, Saeys, Y, Malissen, B., Dalod, M., Clausen, B E, and Mowat, Alan McI.

Subjects
TheoryofComputation_ANALYSISOFALGORITHMSANDPROBLEMCOMPLEXITY, chemical and pharmacologic phenomena, hemic and immune systems
Abstract

CD103+CD11b+ dendritic cells (DCs) are unique to the intestine, but the factors governing their differentiation are unclear. Here we show that transforming growth factor receptor 1 (TGFβR1) has an indispensable, cell intrinsic role in the development of these cells. Deletion of Tgfbr1 results in markedly fewer intestinal CD103+CD11b+ DCs and a reciprocal increase in the CD103−CD11b+ dendritic cell subset. Transcriptional profiling identifies markers that define the CD103+CD11b+ DC lineage, including CD101, TREM1 and Siglec-F, and shows that the absence of CD103+CD11b+ DCs in CD11c-Cre.Tgfbr1 fl/fl mice reflects defective differentiation from CD103−CD11b+ intermediaries, rather than an isolated loss of CD103 expression. The defect in CD103+CD11b+ DCs is accompanied by reduced generation of antigen-specific, inducible FoxP3+ regulatory T cells in vitro and in vivo, and by reduced numbers of endogenous Th17 cells in the intestinal mucosa. Thus, TGFβR1-mediated signalling may explain the tissue-specific development of these unique DCs.

Published
2017
Full Text
View/download PDF

5. TGFβR signalling controls CD103+CD11b+ dendritic cell development in the intestine

Author

Bain, C. C., Montgomery, J., Scott, C. L., Kel, J. M., Girard-Madoux, M. J. H., Martens, L., Zangerle-Murray, T. F. P., Ober-Blöbaum, J., Lindenbergh-Kortleve, D., Samsom, J. N., Henri, S., Lawrence, T., Saeys, Y., Malissen, B., Dalod, M., Clausen, B. E., and Mowat, A. McI.

Subjects
HOMEOSTASIS, Science, Receptor, Transforming Growth Factor-beta Type I, chemical and pharmacologic phenomena, IL-17-PRODUCING T-CELLS, Protein Serine-Threonine Kinases, LAMINA PROPRIA, T-Lymphocytes, Regulatory, Article, Mice, Antigens, CD, Medicine and Health Sciences, Animals, Cell Lineage, MACROPHAGES, Intestinal Mucosa, lcsh:Science, Immunity, Mucosal, Mice, Knockout, RETINOIC-ACID, CD11b Antigen, Lymphopoiesis, Biology and Life Sciences, LANGERHANS CELLS, hemic and immune systems, Cell Differentiation, Dendritic Cells, Colitis, Intestines, MICE, DIFFERENTIATION, Th17 Cells, lcsh:Q, IMMUNE-SYSTEM, LYMPHOID-TISSUE-RESIDENT, Integrin alpha Chains, Receptors, Transforming Growth Factor beta
Abstract

CD103+CD11b+ dendritic cells (DCs) are unique to the intestine, but the factors governing their differentiation are unclear. Here we show that transforming growth factor receptor 1 (TGFβR1) has an indispensable, cell intrinsic role in the development of these cells. Deletion of Tgfbr1 results in markedly fewer intestinal CD103+CD11b+ DCs and a reciprocal increase in the CD103−CD11b+ dendritic cell subset. Transcriptional profiling identifies markers that define the CD103+CD11b+ DC lineage, including CD101, TREM1 and Siglec-F, and shows that the absence of CD103+CD11b+ DCs in CD11c-Cre.Tgfbr1 fl/fl mice reflects defective differentiation from CD103−CD11b+ intermediaries, rather than an isolated loss of CD103 expression. The defect in CD103+CD11b+ DCs is accompanied by reduced generation of antigen-specific, inducible FoxP3+ regulatory T cells in vitro and in vivo, and by reduced numbers of endogenous Th17 cells in the intestinal mucosa. Thus, TGFβR1-mediated signalling may explain the tissue-specific development of these unique DCs., Developmental cues for the different dendritic cell (DC) subsets in the intestine are yet to be defined. Here the authors show that TGFβR1 signalling is needed for development of CD103+CD11b+ intestinal DCs from CD103−CD11b+ cells and that they contribute to the generation of Th17 and regulatory T cells

Published
2017

6. Macrophage-mediated gliadin degradation and concomitant IL-27 production drive IL-10- and IFN-γ 3-secreting Tr1-like-cell differentiation in a murine model for gluten tolerance

Author

Van Leeuwen, M. A., Costes, L. M.M., Van Berkel, L. A., Simons-Oosterhuis, Y., Du Pré, M. F., Kozijn, A. E., Raatgeep, H. C., Lindenbergh-Kortleve, D. J., Van Rooijen, N., Koning, F., Samsom, J. N., and Molecular cell biology and Immunology

Subjects
food and beverages, nutritional and metabolic diseases, digestive system, digestive system diseases
Abstract

Celiac disease is caused by inflammatory T-cell responses against the insoluble dietary protein gliadin. We have shown that, in humanized mice, oral tolerance to deamidated chymotrypsin-digested gliadin (CT-TG2-gliadin) is driven by tolerogenic interferon (IFN)-γ 3- and interleukin (IL)-10-secreting type 1 regulatory T-like cells (Tr1-like cells) generated in the spleen but not in the mesenteric lymph nodes. We aimed to uncover the mechanisms underlying gliadin-specific Tr1-like-cell differentiation and hypothesized that proteolytic gliadin degradation by splenic macrophages is a decisive step in this process. In vivo depletion of macrophages caused reduced differentiation of splenic IFN-γ 3- and IL-10-producing Tr1-like cells after CT-TG2-gliadin but not gliadin peptide feed. Splenic macrophages, rather than dendritic cells, constitutively expressed increased mRNA levels of the endopeptidase Cathepsin D; macrophage depletion significantly reduced splenic Cathepsin D expression in vivo and Cathepsin D efficiently degraded recombinant γ 3-gliadin in vitro. In response to CT-TG2-gliadin uptake, macrophages enhanced the expression of Il27p28, a cytokine that favored differentiation of gliadin-specific Tr1-like cells in vitro, and was previously reported to increase Cathepsin D activity. Conversely, IL-27 neutralization in vivo inhibited splenic IFN-γ 3- and IL-10-secreting Tr1-like-cell differentiation after CT-TG2-gliadin feed. Our data infer that endopeptidase mediated gliadin degradation by macrophages and concomitant IL-27 production drive differentiation of splenic gliadin-specific Tr1-like cells.

Published
2017
Full Text
View/download PDF

7. TGF beta R signalling controls CD103(+)CD11b(+) dendritic cell development in the intestine

Author

Bain, C. C., Montgomery, J., Scott, C. L., Kel, J. M., Girard-Madoux, M. J. H., Martens, L., Zangerle-Murray, T. F. P., Ober-Blobaum, J., Lindenbergh-Kortleve, D., Samsom, J. N., Henri, S., Lawrence, T., Saeys, Y., Malissen, Bernard, Dalod, M., Clausen, B. E., Mowat, A. Mcl., Immunology, Pediatrics, University of Glasgow, Centre d'Immunologie de Marseille - Luminy (CIML), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), Erasmus University Medical Center [Rotterdam] (Erasmus MC), Universiteit Gent = Ghent University [Belgium] (UGENT), Department of Applied Mathematics and Computer Science [Ghent], Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), and Universiteit Gent = Ghent University (UGENT)

Subjects
[SDV.IMM]Life Sciences [q-bio]/Immunology, chemical and pharmacologic phenomena, hemic and immune systems
Abstract

International audience; CD103(+)CD11b(+) dendritic cells (DCs) are unique to the intestine, but the factors governing their differentiation are unclear. Here we show that transforming growth factor receptor 1 (TGF beta beta R1) has an indispensable, cell intrinsic role in the development of these cells. Deletion of Tgfbr1 results in markedly fewer intestinal CD103(+)CD11b(+) DCs and a reciprocal increase in the CD103(-)CD11b(+) dendritic cell subset. Transcriptional profiling identifies markers that define the CD103(+)CD11b(+) DC lineage, including CD101, TREM1 and Siglec-F, and shows that the absence of CD103(+)CD11b(+) DCs in CD11c-Cre. Tgfbr1(fl/fl) mice reflects defective differentiation from CD103(-)CD11b(+) intermediaries, rather than an isolated loss of CD103 expression. The defect in CD103(+)CD11b(+) DCs is accompanied by reduced generation of antigen-specific, inducible FoxP3(+) regulatory T cells in vitro and in vivo, and by reduced numbers of endogenous Th17 cells in the intestinal mucosa. Thus, TGF beta R1-mediated signalling may explain the tissue-specific development of these unique DCs.

Published
2017
Full Text
View/download PDF

13. Colonic tolerance develops in the iliac lymph nodes and can be established independent of CD103+ dendritic cells

Author

Veenbergen, S, primary, van Berkel, L A, additional, du Pré, M F, additional, He, J, additional, Karrich, J J, additional, Costes, L M M, additional, Luk, F, additional, Simons-Oosterhuis, Y, additional, Raatgeep, H C, additional, Cerovic, V, additional, Cupedo, T, additional, Mowat, A M, additional, Kelsall, B L, additional, and Samsom, J N, additional

Published
2016
Full Text
View/download PDF

15. No association between transient hypothyroxinemia of prematurity and neurodevelopmental outcome in young adulthood

Author

Hollanders, Jonneke J., Israëls, Joël, Van Der Pal, Sylvia M., Verkerk, Paul H., Rotteveel, Joost, Finken, Martijn J J, Hille, E. T M, De Groot, C. H., Kloosterboer-Boerrigter, H., Den Ouden, A. L., Rijpstra, A., Verloove-Vanhorick, S. P., Vogelaar, J. A., Kok, J. H., Ilsen, A., Van Der Lans, M., Boelen-Van Der Loo, W. J C, Lundqvist, T., Heymans, H. S A, Duiverman, E. J., Geven, W. B., Duiverman, M. L., Geven, L. I., Vrijlandt, E. J L E, Mulder, A. L M, Gerver, A., Kollée, L. A A, Reijmers, L., Sonnemans, R., Wit, J. M., Dekker, F. W., Finken, M. J J, Weisglas-Kuperus, N., Keijzer-Veen, M. G., Van Der Heijden, A. J., Van Goudoever, J. B., Van Weissenbruch, M. M., Cranendonk, A., Delemarre-Van De Waal, H. A., De Groot, L., Samsom, J. F., De Vries, L. S., Rademaker, K. J., Moerman, E., Voogsgeerd, M., De Kleine, M. J K, Andriessen, P., Dielissen-Van Helvoirt, C. C M, Mohamed, I., Van Straaten, H. L M, Baerts, W., Veneklaas Slots-Kloosterboer, G. W., Tuller-Pikkemaat, E. M J, Ens-Dokkum, M. H., Van Steenbrugge, G. J., Hollanders, Jonneke J., Israëls, Joël, Van Der Pal, Sylvia M., Verkerk, Paul H., Rotteveel, Joost, Finken, Martijn J J, Hille, E. T M, De Groot, C. H., Kloosterboer-Boerrigter, H., Den Ouden, A. L., Rijpstra, A., Verloove-Vanhorick, S. P., Vogelaar, J. A., Kok, J. H., Ilsen, A., Van Der Lans, M., Boelen-Van Der Loo, W. J C, Lundqvist, T., Heymans, H. S A, Duiverman, E. J., Geven, W. B., Duiverman, M. L., Geven, L. I., Vrijlandt, E. J L E, Mulder, A. L M, Gerver, A., Kollée, L. A A, Reijmers, L., Sonnemans, R., Wit, J. M., Dekker, F. W., Finken, M. J J, Weisglas-Kuperus, N., Keijzer-Veen, M. G., Van Der Heijden, A. J., Van Goudoever, J. B., Van Weissenbruch, M. M., Cranendonk, A., Delemarre-Van De Waal, H. A., De Groot, L., Samsom, J. F., De Vries, L. S., Rademaker, K. J., Moerman, E., Voogsgeerd, M., De Kleine, M. J K, Andriessen, P., Dielissen-Van Helvoirt, C. C M, Mohamed, I., Van Straaten, H. L M, Baerts, W., Veneklaas Slots-Kloosterboer, G. W., Tuller-Pikkemaat, E. M J, Ens-Dokkum, M. H., and Van Steenbrugge, G. J.

Published
2015

16. No association between transient hypothyroxinemia of prematurity and neurodevelopmental outcome in young adulthood

Author

Nefrologie patientenzorg, Child Health, UMC Utrecht, MS Neonatologie, Brain, Hollanders, Jonneke J., Israëls, Joël, Van Der Pal, Sylvia M., Verkerk, Paul H., Rotteveel, Joost, Finken, Martijn J J, Hille, E. T M, De Groot, C. H., Kloosterboer-Boerrigter, H., Den Ouden, A. L., Rijpstra, A., Verloove-Vanhorick, S. P., Vogelaar, J. A., Kok, J. H., Ilsen, A., Van Der Lans, M., Boelen-Van Der Loo, W. J C, Lundqvist, T., Heymans, H. S A, Duiverman, E. J., Geven, W. B., Duiverman, M. L., Geven, L. I., Vrijlandt, E. J L E, Mulder, A. L M, Gerver, A., Kollée, L. A A, Reijmers, L., Sonnemans, R., Wit, J. M., Dekker, F. W., Finken, M. J J, Weisglas-Kuperus, N., Keijzer-Veen, M. G., Van Der Heijden, A. J., Van Goudoever, J. B., Van Weissenbruch, M. M., Cranendonk, A., Delemarre-Van De Waal, H. A., De Groot, L., Samsom, J. F., De Vries, L. S., Rademaker, K. J., Moerman, E., Voogsgeerd, M., De Kleine, M. J K, Andriessen, P., Dielissen-Van Helvoirt, C. C M, Mohamed, I., Van Straaten, H. L M, Baerts, W., Veneklaas Slots-Kloosterboer, G. W., Tuller-Pikkemaat, E. M J, Ens-Dokkum, M. H., Van Steenbrugge, G. J., Nefrologie patientenzorg, Child Health, UMC Utrecht, MS Neonatologie, Brain, Hollanders, Jonneke J., Israëls, Joël, Van Der Pal, Sylvia M., Verkerk, Paul H., Rotteveel, Joost, Finken, Martijn J J, Hille, E. T M, De Groot, C. H., Kloosterboer-Boerrigter, H., Den Ouden, A. L., Rijpstra, A., Verloove-Vanhorick, S. P., Vogelaar, J. A., Kok, J. H., Ilsen, A., Van Der Lans, M., Boelen-Van Der Loo, W. J C, Lundqvist, T., Heymans, H. S A, Duiverman, E. J., Geven, W. B., Duiverman, M. L., Geven, L. I., Vrijlandt, E. J L E, Mulder, A. L M, Gerver, A., Kollée, L. A A, Reijmers, L., Sonnemans, R., Wit, J. M., Dekker, F. W., Finken, M. J J, Weisglas-Kuperus, N., Keijzer-Veen, M. G., Van Der Heijden, A. J., Van Goudoever, J. B., Van Weissenbruch, M. M., Cranendonk, A., Delemarre-Van De Waal, H. A., De Groot, L., Samsom, J. F., De Vries, L. S., Rademaker, K. J., Moerman, E., Voogsgeerd, M., De Kleine, M. J K, Andriessen, P., Dielissen-Van Helvoirt, C. C M, Mohamed, I., Van Straaten, H. L M, Baerts, W., Veneklaas Slots-Kloosterboer, G. W., Tuller-Pikkemaat, E. M J, Ens-Dokkum, M. H., and Van Steenbrugge, G. J.

Published
2015

17. IL-10 signaling in dendritic cells controls IL-1β-mediated IFNγ secretion by human CD4+T cells: relevance to inflammatory bowel disease

Author

Veenbergen, S., Li, P., Raatgeep, H., Lindenbergh-Kortleve, D., Simons-Oosterhuis, Y., Farrel, A., Costes, L., Joosse, M., Berkel, L., Ruiter, L., Leeuwen, M., Winter, D., Holland, S., Freeman, A., Wakabayashi, Y., Zhu, J., Ridder, L., Driessen, G., Escher, J., Leonard, W., and Samsom, J.

Abstract

Uncontrolled interferon γ (IFNγ)-mediated T-cell responses to commensal microbiota are a driver of inflammatory bowel disease (IBD). Interleukin-10 (IL-10) is crucial for controlling these T-cell responses, but the precise mechanism of inhibition remains unclear. A better understanding of how IL-10 exerts its suppressive function may allow identification of individuals with suboptimal IL-10 function among the heterogeneous population of IBD patients. Using cells from patients with an IL10RAdeficiency or STAT3mutations, we demonstrate that IL-10 signaling in monocyte-derived dendritic cells (moDCs), but not T cells, is essential for controlling IFNγ-secreting CD4+T cells. Deficiency in IL-10 signaling dramatically increased IL-1β release by moDCs. IL-1β boosted IFNγ secretion by CD4+T cells either directly or indirectly by stimulating moDCs to secrete IL-12. As predicted a signature of IL-10 dysfunction was observed in a subgroup of pediatric IBD patients having higher IL-1β expression in activated immune cells and macroscopically affected intestinal tissue. In agreement, reduced IL10RAexpression was detected in peripheral blood mononuclear cells and a subgroup of pediatric IBD patients exhibited diminished IL-10 responsiveness. Our data unveil an important mechanism by which IL-10 controls IFNγ-secreting CD4+T cells in humans and identifies IL-1β as a potential classifier for a subgroup of IBD patients.

Published
2019
Full Text
View/download PDF

18. IL-10 signaling prevents gluten-dependent intraepithelial CD4+cytotoxic T lymphocyte infiltration and epithelial damage in the small intestine

Author

Costes, L. M. M., Lindenbergh-Kortleve, D. J., van Berkel, L. A., Veenbergen, S., Raatgeep, H. (R). C., Simons-Oosterhuis, Y., van Haaften, D. H., Karrich, J. J., Escher, J. C., Groeneweg, M., Clausen, B. E., Cupedo, T., and Samsom, J. N.

Abstract

Breach of tolerance to gluten leads to the chronic small intestinal enteropathy celiac disease. A key event in celiac disease development is gluten-dependent infiltration of activated cytotoxic intraepithelial lymphocytes (IELs), which cytolyze epithelial cells causing crypt hyperplasia and villous atrophy. The mechanisms leading to gluten-dependent small intestinal IEL infiltration and activation remain elusive. We have demonstrated that under homeostatic conditions in mice, gluten drives the differentiation of anti-inflammatory T cells producing large amounts of the immunosuppressive cytokine interleukin-10 (IL-10). Here we addressed whether this dominant IL-10 axis prevents gluten-dependent infiltration of activated cytotoxic IEL and subsequent small intestinal enteropathy. We demonstrate that IL-10 regulation prevents gluten-induced cytotoxic inflammatory IEL infiltration. In particular, IL-10 suppresses gluten-induced accumulation of a specialized population of cytotoxic CD4+CD8αα+IEL (CD4+CTL) expressing Tbx21, Ifng, and Il21, and a disparate non-cytolytic CD4+CD8α−IEL population expressing Il17a, Il21, and Il10. Concomitantly, IL-10 suppresses gluten-dependent small intestinal epithelial hyperproliferation and upregulation of stress-induced molecules on epithelial cells. Remarkably, frequencies of granzyme B+CD4+CD8α+IEL are increased in pediatric celiac disease patient biopsies. These findings demonstrate that IL-10 is pivotal to prevent gluten-induced small intestinal inflammation and epithelial damage, and imply that CD4+CTL are potential new players into these processes.

Published
2019
Full Text
View/download PDF

19. Herkenning en bestrijding van ridderzuring met een robot

Author

van Evert, F.K., Samsom, J., Polder, G., Vijn, M.P., van Dooren, H.J.C., Lamaker, A., van der Heijden, G.W.A.M., Kempenaar, C., van der Zalm, T., and Lotz, L.A.P.

Subjects
dairy farming, weed control, begrazing, globale plaatsbepalingssystemen, onkruidbestrijding, detection, PPO Arable Farming, Multifunctional Agriculture and Field Production of Vegetables, onkruiden, PRI Agrosysteemkunde, organic farming, weeds, grazing, voederwaardering, feed evaluation, precision agriculture, research, detectie, precisielandbouw, farm management, onderzoek, PRI Bioscience, PRI Biometris, rumex obtusifolius, biologische landbouw, global positioning systems, melkveehouderij, Agrosystems, agrarische bedrijfsvoering, PPO Akkerbouw, Groene Ruimte en Vollegrondsgroente
Abstract

Ridderzuring (Rumex obtusifolius L.) is een veelvoorkomend en lastig te bestrijden onkruid dat vooral biologische melkveehouders grote problemen bezorgt. Op initiatief van de sector wordt daarom een robot ontwikkeld die geheel zelfstandig ridderzuring opspoort en vernietigt.

Published
2010

20. TGFβR signalling controls CD103+CD11b+ dendritic cell development in the intestine.

Author

Bain, C. C., Montgomery, J., Scott, C. L., Kel, J. M., Girard-Madoux, M. J. H., Martens, L., Zangerle-Murray, T. F. P., Ober-Blöbaum, J., Lindenbergh-Kortleve, D., Samsom, J. N., Henri, S., Lawrence, T., Saeys, Y., Malissen, B., Dalod, M., Clausen, B. E., and Mowat, A. McI.

Abstract

CD103+CD11b+ dendritic cells (DCs) are unique to the intestine, but the factors governing their differentiation are unclear. Here we show that transforming growth factor receptor 1 (TGFβR1) has an indispensable, cell intrinsic role in the development of these cells. Deletion of Tgfbr1 results in markedly fewer intestinal CD103+CD11b+ DCs and a reciprocal increase in the CD103-CD11b+ dendritic cell subset. Transcriptional profiling identifies markers that define the CD103+CD11b+ DC lineage, including CD101, TREM1 and Siglec-F, and shows that the absence of CD103+CD11b+ DCs in CD11c-Cre.Tgfbr1 fl/fl mice reflects defective differentiation from CD103-CD11b+ intermediaries, rather than an isolated loss of CD103 expression. The defect in CD103+CD11b+ DCs is accompanied by reduced generation of antigen-specific, inducible FoxP3+ regulatory T cells in vitro and in vivo, and by reduced numbers of endogenous Th17 cells in the intestinal mucosa. Thus, TGFβR1-mediated signalling may explain the tissue-specific development of these unique DCs.Developmental cues for the different dendritic cell (DC) subsets in the intestine are yet to be defined. Here the authors show that TGFβR1 signalling is needed for development of CD103+CD11b+ intestinal DCs from CD103-CD11b+ cells and that they contribute to the generation of Th17 and regulatory T cells. [ABSTRACT FROM AUTHOR]

Published
2017
Full Text
View/download PDF

22. Campylobacter jejuni Translocation across Intestinal Epithelial Cells Is Facilitated by Ganglioside-Like Lipooligosaccharide Structures

Author

Louwen, R., Nieuwenhuis, E.E.S., van Marrewijk, L., Horst-Kreft, D., de Ruiter, L., Heikema, A.P., van Wamel, W.J., Wagenaar, J.A., Endtz, H.P., Samsom, J., van Baarlen, P., Akhmanova, A., van Belkum, A., Louwen, R., Nieuwenhuis, E.E.S., van Marrewijk, L., Horst-Kreft, D., de Ruiter, L., Heikema, A.P., van Wamel, W.J., Wagenaar, J.A., Endtz, H.P., Samsom, J., van Baarlen, P., Akhmanova, A., and van Belkum, A.

Abstract

Translocation across intestinal epithelial cells is an established pathogenic feature of the zoonotic bacterial species Campylobacter jejuni. The number of C. jejuni virulence factors known to be involved in translocation is limited. In the present study, we investigated whether sialylation of C. jejuni lipooligosaccharide (LOS) structures, generating human nerve ganglioside mimics, is important for intestinal epithelial translocation. We here show that C. jejuni isolates expressing ganglioside-like LOS bound in larger numbers to the Caco-2 intestinal epithelial cells than C. jejuni isolates lacking such structures. Next, we found that ganglioside-like LOS facilitated endocytosis of bacteria into Caco-2 cells, as visualized by quantitative microscopy using the early and late endosomal markers early endosome-associated protein 1 (EEA1), Rab5, and lysosome-associated membrane protein 1 (LAMP-1). This increased endocytosis was associated with larger numbers of surviving and translocating bacteria. Next, we found that two different intestinal epithelial cell lines (Caco-2 and T84) responded with an elevated secretion of the T-cell attractant CXCL10 to infection by ganglioside-like LOS-expressing C. jejuni isolates. We conclude that C. jejuni translocation across Caco-2 cells is facilitated by ganglioside-like LOS, which is of clinical relevance since C. jejuni ganglioside-like LOS-expressing isolates are linked with severe gastroenteritis and bloody stools in C. jejuni-infected patients.

Published
2012

23. A robot to detect and control broad-leaved dock (Rumex obtusifolius L.) in grassland

Author

van Evert, F.K., Samsom, J., Polder, G., Vijn, M.P., van Dooren, H.J.C., Lamaker, E.J.J., van der Heijden, G.W.A.M., Kempenaar, C., van der Zalm, A.J.A., Lotz, L.A.P., van Evert, F.K., Samsom, J., Polder, G., Vijn, M.P., van Dooren, H.J.C., Lamaker, E.J.J., van der Heijden, G.W.A.M., Kempenaar, C., van der Zalm, A.J.A., and Lotz, L.A.P.

Abstract

Broad-leaved dock is a common and troublesome grassland weed with a wide geographic distribution. In conventional farming the weed is normally controlled by using a selective herbicide, but in organic farming manual removal is the best option to control this weed. The objective of our work was to develop a robot that can navigate a pasture, detect broad-leaved dock, and remove any weeds found. A prototype robot was constructed that navigates by following a predefined path using centimeter-precision global positioning system (GPS). Broad-leaved dock is detected using a camera and image processing. Once detected, weeds are destroyed by a cutting device. Tests of aspects of the system showed that path following accuracy is adequate but could be improved through tuning of the controller or adoption of a dynamic vehicle model, that the success rate of weed detection is highest when the grass is short and when the broad-leaved dock plants are in rosette form, and that 75% of weeds removed did not grow back. An on-farm field test of the complete system resulted in detection of 124 weeds of 134 encountered (93%), while a weed removal action was performed eight times without a weed being present. Effective weed control is considered to be achieved when the center of the weeder is positioned within 0.1 m of the taproot of the weed—this occurred in 73% of the cases. We conclude that the robot is an effective instrument to detect and control broad-leaved dock under the conditions encountered on a commercial farm. © 2010 Wiley Periodicals, Inc.

Published
2011

24. Robotic control of broad-leaved dock

Author

van Evert, F.K., Samsom, J., Polder, G., Vijn, M.P., van Dooren, H.J.C., Lamaker, E.J.J., van der Heijden, G.W.A.M., Kempenaar, C., van der Zalm, A.J.A., Lotz, L.A.P., van Evert, F.K., Samsom, J., Polder, G., Vijn, M.P., van Dooren, H.J.C., Lamaker, E.J.J., van der Heijden, G.W.A.M., Kempenaar, C., van der Zalm, A.J.A., and Lotz, L.A.P.

Published
2009

27. O01 CD1D-DEPENDENT REGULATION OF BACTERIAL COLONIZATION IN THE INTESTINE

Author

Nieuwenhuis, E.E.S., primary, Matsumoto, T., additional, Lindenbergh-Kortleve, D., additional, Middendorp, S., additional, Willemsen, R., additional, Kaser, A., additional, Simons-Oosterhuis, Y., additional, Brugman, S., additional, Yamaguchi, K., additional, Ishikawa, H., additional, Aiba, Y., additional, Koga, Y., additional, Samsom, J., additional, Oshima, K., additional, Kikuchi, M., additional, Escher, J.C., additional, Hattori, M., additional, Onderdonk, A.B., additional, and Blumberg, R.S., additional

Published
2009
Full Text
View/download PDF

29. Muscle power in 'high-risk' preterm infants at 12 and 24 weeks corrected age:a measure for early detection

Author

Samsom, J. F., Groot, L. De, Hopkins, Brian, Samsom, J. F., Groot, L. De, and Hopkins, Brian

Abstract

A group of 72 "high-risk" preterm infants was studied at the corrected ages of 12 and 24 wk. Onlyinfants with a high risk for developmental deviance with gestational ages below 32 wk and/or birthweights of less than 1500 g were included in the study. In addition, the infants were categorized according to their medical history, as confirmed by the "Neonatal Medical Index" (NMI I to V), with category I describing infants with few medical problems and V characterizing those with the most serious complications. In this study we included only "high-risk" infants as categorized in NMI III to V, since infants with a "low risk" have been described earlier. Apart from the standard paediatric follow-up, an age-adequate neurological assessment was made, with special emphasis on the relationship between active and passive muscle power. When development is optimal, these two components of muscle power should be in balance in order to create a stable posture and fluent motility. We compared muscle power at the corrected ages of 12 and 24 wk to determine whether the method employed to assess muscle power could enhance early detection of deviant development. At 12 wk of age, only 5 infants showed overall optimal muscle power, while at 24 wk this figure had increased to 27. Significantly more infants in NMI III had optimal outcomes at 24 wk of age. When muscle power in the different parts of the body was studied separately at 24 wk, outcomes in shoulders and trunk still showed significant discrepancies in all NMI groups. At this age, fewer asymmetries were found compared to outcomes at 12 wk. Conclusion: Our method of assessing muscle power is useful in detecting preterm infants at risk for pathological development.

Published
2001

31. Colonic tolerance develops in the iliac lymph nodes and can be established independent of CD103+dendritic cells

Author

Veenbergen, S, van Berkel, L A, du Pré, M F, He, J, Karrich, J J, Costes, L M M, Luk, F, Simons-Oosterhuis, Y, Raatgeep, H C, Cerovic, V, Cupedo, T, Mowat, A M, Kelsall, B L, and Samsom, J N

Abstract

Tolerance to harmless exogenous antigens is the default immune response in the gastrointestinal tract. Although extensive studies have demonstrated the importance of the mesenteric lymph nodes (MLNs) and intestinal CD103+dendritic cells (DCs) in driving small intestinal tolerance to protein antigen, the structural and immunological basis of colonic tolerance remain poorly understood. We show here that the caudal and iliac lymph nodes (ILNs) are inductive sites for distal colonic immune responses and that colonic T cell-mediated tolerance induction to protein antigen is initiated in these draining lymph nodes and not in MLNs. In agreement, colonic tolerance induction was not altered by mesenteric lymphadenectomy. Despite tolerance development, CD103+CD11b+DCs, which are the major migratory DC population in the MLNs, and the tolerance-related retinoic acid-generating enzyme RALDH2 were virtually absent from the ILNs. Administration of ovalbumin (OVA) to the distal colon did increase the number of CD11c+MHCIIhimigratory CD103−CD11b+and CD103+CD11b−DCs in the ILNs. Strikingly, colonic tolerance was intact in Batf3-deficient mice specifically lacking CD103+CD11b−DCs, suggesting that CD103−DCs in the ILNs are sufficient to drive tolerance induction after protein antigen encounter in the distal colon. Altogether, we identify different inductive sites for small intestinal and colonic T-cell responses and reveal that distinct cellular mechanisms are operative to maintain tolerance at these sites.

Published
2016
Full Text
View/download PDF

35. Tumour necrosis factor, but not interferon-γ, is essential for acquired resistance to <em>Listeria monocytogenes</em> during a secondary infection in mice.

Author

Samsom, J. N., Langermans, J. A. M., Savelkoult, H. F. J., and van Furth, R.

Subjects
*LISTERIA monocytogenes, *CELLULAR immunity, *TUMOR necrosis factors, *ANTINEOPLASTIC agents, *BLOOD plasma, *LABORATORY mice
Abstract

Mice with a secondary Listeria monocytogenes infection eliminate the bacteria much faster and more efficiently from their organs than mice with a primary infection. During the course of a secondary infection, serum concentrations of interferon-γ (IFN-γ) and tumour necrosis factor-α (TNF) are higher than during a primary infection. The aim of the present study was to determine whether these cytokines are involved in the acquired resistance to L. monocytogenes during a secondary infection in mice. In order to neutralize cytokines, alginate-encapsulated cells, which form anti-cytokine monoclonal antibodies, were injected into the nuchal region of mice during a Listeria infection. Mice recovered from a sublethal primary Listeria infection, which acquired cell-mediated immunity, received a subcutaneous injection of anti-lFN-γ-forming cells, or anti-TNF-forming cells, and 4 days later received an intravenous injection with 10 50% lethal dose (LD50) L. monocytogenes. The number of bacteria recovered from the liver and spleen of immune mice treated with anti-IFN-γ-forming cells was slightly larger (∼1 log10) than that found for immune mice treated with anti-β-galactosidase-forming cells, called immune control mice. The organs of immune mice treated with anti-TNF-forming cells yielded significantly more (∼4 log10) bacteria than those of immune control mice, more than those of immune mice treated with anti-IFN-γ-forming cells, and comparable numbers to those of non-immune mice. Taken together, these results demonstrate that TNF is essential in acquired resistance to L. monocytogenes during a secondary infection in mice, while IFN-γ plays a minor role. [ABSTRACT FROM AUTHOR]

Published
1995

37. Interleukin-10 has different effects on proliferation of Listeria monocytogenes in livers and spleens of mice.

Author

Samsom, J N, Annema, A, Geertsma, M F, Langermans, J A, Groeneveld, P H, de Heer, E, and van Furth, R

Abstract

The aim of this study was to investigate the effect of interleukin-10 (IL-10) on the course of Listeria monocytogenes infection in naive and immune mice. Treatment with IL-10 during the course of a primary infection significantly decreased the number of bacteria in the spleen and did not affect the number in the liver. During a secondary infection in immune mice treated with IL-10, the number of bacteria was significantly lower in the spleen but significantly higher in the liver in comparison to mock-treated immune mice. IL-10 treatment during a primary Listeria infection decreased the concentration of gamma interferon (IFN-gamma) in plasma and the toxoplasmastatic activity of macrophages, whereas it increased the percentage of mildly CD3-positive T cells in the spleen. During a secondary infection, the concentration of IFN-gamma in plasma was decreased on day 1 but remained unaffected during later days of infection. From these results, we conclude that IL-10 has different effects on the proliferation of L. monocytogenes in the spleen and liver during primary and secondary Listeria infections.

Published
2000

38. Gender differences in respiratory symptoms in 19-year-old adults born preterm

Author

Vrijlandt, Elianne J. L. E., Gerritsen, Jorrit, Boezen, H. Marike, Duiverman, Eric J., Hille, E. T. M., de Groot, C. H., Kloosterboer-Boerrigter, H., den Ouden, A. L., Rijpstra, A., Verloove-Vanhorick, S. P., Vogelaar, J. A., Kok, J. H., Ilsen, A., van der Lans, M., Boelen-van der Loo, W. J. C., Lundqvist, T., Heymans, H. S. A., Geven, W. B., Duiverman, M. L., Geven, L. I., Mulder, A. L. M., Gerver, A., Kollée, L. A. A., Reijmers, L., Sonnemans, R., Wit, J. M., Dekker, F. W., Finken, M. J. J., Weisglas-Kuperus, N., Keijzer-Veen, M. G., van der Heijden, A. J., van Goudoever, J. B., van Weissenbruch, M. M., Cranendonk, A., Delemarre-van de Waal, H. A., de Groot, L., Samsom, J. F., de Vries, L. S., Rademaker, K. J., Moerman, E., Voogsgeerd, M., de Kleine, M. J. K., Andriessen, P., Dielissen-van Helvoirt, C. C. M., Mohamed, I., van Straaten, H. L. M., Baerts, W., Veneklaas Slots-Kloosterboer, G. W., Tuller-Pikkemaat, E. M. J., Ens-Dokkum, M. H., van Steenbrugge, G. J., Life Course Epidemiology (LCE), Groningen Research Institute for Asthma and COPD (GRIAC), Neonatology, Other Research, Plastic, Reconstructive and Hand Surgery, and TNO Kwaliteit van Leven

Subjects
Lung Diseases, Male, Pediatrics, Newborn disease, Hay fever, Health Status, Eczema, CHILDHOOD, INFANTS, Cohort Studies, Risk Factors, Prevalence, Symptomatology, Prospective Studies, Netherlands, education.field_of_study, Atopy, Respiratory tract disease, PREMATURITY, HYALINE-MEMBRANE DISEASE, Health survey, PULMONARY SEQUELAE, Statistical significance, Europe, Health, Premature birth, DISTRESS SYNDROME, Premature Birth, Female, Cohort analysis, medicine.symptom, Prematurity, Human, Cohort study, Adult, Pulmonary and Respiratory Medicine, medicine.medical_specialty, Birth weight, Population, Population research, Major clinical study, Risk Assessment, Sex Factors, Wheeze, medicine, Humans, Prospective study, education, Exercise, Asthma, lcsh:RC705-779, Wheezing, Questionnaire, business.industry, Research, Infant, Newborn, Gestational age, Follow up, lcsh:Diseases of the respiratory system, BRONCHOPULMONARY DYSPLASIA, Sex difference, medicine.disease, Dyspnea, Bronchopulmonary dysplasia, Physician, CHRONIC LUNG-DISEASE, Lung disease, ASTHMA, business, FOLLOW-UP, Controlled study, Follow-Up Studies
Abstract

ObjectiveTo study the prevalence of respiratory and atopic symptoms in (young) adults born prematurely, differences between those who did and did not develop Bronchopulmonary Disease (BPD) at neonatal age and differences in respiratory health between males and females.MethodsDesign: Prospective cohort study.Setting:Nation wide follow-up study, the Netherlands.Participants:690 adults (19 year old) born with a gestational age below 32 completed weeks and/or with a birth weight less than 1500 g. Controls were Dutch participants of the European Community Respiratory Health Survey (ECRHS).Main outcome measures:Presence of wheeze, shortness of breath, asthma, hay fever and eczema using the ECRHS-questionnaireResultsThe prevalence of doctor-diagnosed asthma was significantly higher in the ex-preterms than in the general population, whereas eczema and hay fever were significant lower. Women reported more symptoms than men. Preterm women vs controls: asthma 13% vs 5% (p < 0.001); hay fever 8% vs 20% (p < 0.001); eczema 10% vs 42% (p < 0.001). Preterm men vs controls: asthma 9% vs 4% (p = 0.007); hay fever 8% vs 17% (p = 0.005); eczema 9% vs 31% (p < 0.001) Preterm women reported more wheeze and shortness of breath during exercise (sob) than controls: wheeze 30% vs 22% (p = 0.009); sob 27% vs 16% (p < 0.001); 19-year-old women with BPD reported a higher prevalence of doctor diagnosed asthma compared to controls (24% vs 5% p < 0.001) and shortness of breath during exercise (43% vs 16% p = 0.008). The prevalence of reported symptoms by men with BPD were comparable with the controls.ConclusionOur large follow-up study shows a higher prevalence of asthma, wheeze and shortness of breath in the prematurely born young adults. 19-year-old women reported more respiratory symptoms than men. Compared to the general population atopic diseases as hay fever and eczema were reported less often.

Full Text
View/download PDF

39. Robotic control of broad-leaved dock

Author

Evert, F. K., Samsom, J., Gerrit Polder, Vijn, M., Dooren, H. -J, Lamaker, E. J. J., Heijden, G. W. A. M., Kempenaar, C., Zalm, A. J. A., and Lotz, L. A. P.

Subjects
Organic farming, PRI Facility Services, Research, Rumex obtusifolius L, PPO Arable Farming, Multifunctional Agriculture and Field Production of Vegetables, Machine vision, PRI Agrosysteemkunde, PRI Bioscience, PRI Biometris, Agrosystems, IT Infrastructuur, PPO Akkerbouw, Groene Ruimte en Vollegrondsgroente, Onderzoek

42. Reovirus infection triggers inflammatory responses to dietary antigens and development of celiac disease

Author

Mine R. Ikizler, Fengling Hu, Matthew A. Zurenski, Bana Jabri, Karl W. Boehme, Hans Christian Reinecker, Chaitan Khosla, Brad A. Palanski, Sangman M. Kim, Romain Bouziat, Jason A. Iskarpatyoti, Valentina Discepolo, Ian Lawrence, Jordan D. Ernest, Léa M.M. Costes, Valérie Abadie, Mukund Varma, Janneke N. Samsom, Terence S. Dermody, Solomiia Khomandiak, Ramnik J. Xavier, Carol E. Semrad, Marlies Meisel, Andrea J. Pruijssers, Jennifer E. Stencel-Baerenwald, Nicole McAllister, Sonia S. Kupfer, Reinhard Hinterleitner, Toufic Mayassi, Pavithra Aravamudhan, Stefano Guandalini, Luis B. Barreiro, Judy J. Brown, Aylwin Ng, Bouziat, R., Hinterleitner, R., Brown, J. J., Stencel-Baerenwald, J. E., Ikizler, M., Mayassi, T., Meisel, M., Kim, S. M., Discepolo, V., Pruijssers, A. J., Ernest, J. D., Iskarpatyoti, J. A., Costes, L. M. M., Lawrence, I., Palanski, B. A., Varma, M., Zurenski, M. A., Khomandiak, S., Mcallister, N., Aravamudhan, P., Boehme, K. W., Hu, F., Samsom, J. N., Reinecker, H. -C., Kupfer, S. S., Guandalini, S., Semrad, C. E., Abadie, V., Khosla, C., Barreiro, L. B., Xavier, R. J., Ng, A., Dermody, T. S., Jabri, B., and Pediatrics

Subjects
0301 basic medicine, viruses, Autoimmunity, Receptor, Interferon alpha-beta, Disease, Mice, 0302 clinical medicine, Interferon, Reoviridae Infection, Pathogen, Multidisciplinary, Effector, Intestine, Intestines, medicine.anatomical_structure, Antigen, Interferon Type I, 030211 gastroenterology & hepatology, Genetic Engineering, Human, medicine.drug, Glutens, Regulatory T cell, Mice, Transgenic, Biology, Reoviridae, Article, Virus, 03 medical and health sciences, Immunity, Immune Tolerance, medicine, Animals, Humans, Antigens, Autoantibodies, Inflammation, Transglutaminases, Animal, Th1 Cells, biochemical phenomena, metabolism, and nutrition, Virology, Diet, Reoviridae Infections, Mice, Inbred C57BL, Celiac Disease, Disease Models, Animal, 030104 developmental biology, IRF1, Immunology, Gluten, Interferon Regulatory Factor-1
Abstract

Viral infections have been proposed to elicit pathological processes leading to the initiation of T helper 1 (TH1) immunity against dietary gluten and celiac disease (CeD). To test this hypothesis and gain insights into mechanisms underlying virus-induced loss of tolerance to dietary antigens, we developed a viral infection model that makes use of two reovirus strains that infect the intestine but differ in their immunopathological outcomes. Reovirus is an avirulent pathogen that elicits protective immunity, but we discovered that it can nonetheless disrupt intestinal immune homeostasis at inductive and effector sites of oral tolerance by suppressing peripheral regulatory T cell (pTreg) conversion and promoting TH1 immunity to dietary antigen. Initiation of TH1 immunity to dietary antigen was dependent on interferon regulatory factor 1 and dissociated from suppression of pTreg conversion, which was mediated by type-1 interferon. Last, our study in humans supports a role for infection with reovirus, a seemingly innocuous virus, in triggering the development of CeD.

Published
2017
Full Text
View/download PDF

43. Small-molecule targeting AMPA-mediated excitotoxicity has therapeutic effects in mouse models for multiple sclerosis.

Author

Zhai D, Yan S, Samsom J, Wang L, Su P, Jiang A, Zhang H, Jia Z, Wallach I, Heifets A, Zanato C, Tseng CC, Wong AHC, Greig IR, and Liu F

Subjects
Mice, Animals, alpha-Amino-3-hydroxy-5-methyl-4-isoxazolepropionic Acid pharmacology, Excitatory Amino Acid Antagonists pharmacology, Receptors, AMPA, Neurons metabolism, Multiple Sclerosis
Abstract

While most research and treatments for multiple sclerosis (MS) focus on autoimmune reactions causing demyelination, it is possible that neurodegeneration precedes the autoimmune response. Hence, glutamate receptor antagonists preventing excitotoxicity showed promise in MS animal models, though blocking glutamate signaling prevents critical neuronal functions. This study reports the discovery of a small molecule that prevents AMPA-mediated excitotoxicity by targeting an allosteric binding site. A machine learning approach was used to screen for small molecules targeting the AMPA receptor GluA2 subunit. The lead candidate has potent effects in restoring neurological function and myelination while reducing the immune response in experimental autoimmune encephalitis and cuprizone MS mouse models without affecting basal neurotransmission or learning and memory. These findings facilitate development of a treatment for MS with a different mechanism of action than current immune modulatory drugs and avoids important off-target effects of glutamate receptor antagonists. This class of MS therapeutics could be useful as an alternative or complementary treatment to existing therapies.

Published
2023
Full Text
View/download PDF

44. Serum amyloid P component (SAP) modulates antidepressant effects through promoting membrane insertion of the serotonin transporter.

Author

Su P, Yan S, Yang J, Tong J, Samsom J, You F, Li Y, Chen Q, Jiang A, Zhai D, Chen J, Sun Z, Zhou J, Liu M, Lee FJS, Xu ZD, Wang X, Vasdev N, Wong AHC, and Liu F

Subjects
Humans, Mice, Animals, Escitalopram, Antidepressive Agents pharmacology, Selective Serotonin Reuptake Inhibitors pharmacology, Serotonin Plasma Membrane Transport Proteins metabolism, Serum Amyloid P-Component metabolism
Abstract

Serum amyloid P component (SAP) is a universal constituent of human amyloid deposits including those in Alzheimer's disease. SAP has been observed to be elevated in patients with depression, and higher SAP levels are associated with better response to the antidepressant escitalopram. The mechanisms underlying these clinical observations remain unclear. We examined the effect of SAP on serotonin transporter (SERT) expression and localization using Western blot, confocal microscopy, and positron emission tomography with the radioligand [ 11 C]DASB. We also investigated the effect of SAP on treatment response to escitalopram in mice with the forced swim test (FST), a classical behaviour paradigm to assess antidepressant effects. SAP reduced [ 11 C]DASB binding as an index of SERT levels, consistent with Western blots showing decreased total SAP protein because of increased protein degradation. In conjunction with the global decrease in SERT levels, SAP also promotes VAMP-2 mediated SERT membrane insertion. SAP levels are correlated with behavioural despair and SSRI treatment response in mice with FST. In MDD patients, the SAP and membrane SERT levels are correlated with response to SSRI treatment. SAP has complex effects on SERT levels and localization, thereby modulating the effect of SSRIs, which could partially explain clinical variability in antidepressant treatment response. These results add to our understanding of the mechanism for antidepressant drug action, and with further work could be of clinical utility., (© 2022. The Author(s), under exclusive licence to American College of Neuropsychopharmacology.)

Published
2023
Full Text
View/download PDF

45. The D2R-DISC1 protein complex and associated proteins are altered in schizophrenia and normalized with antipsychotic treatment.

Author

Wang J, Su P, Yang J, Xu L, Yuan A, Li C, Zhang T, Dong F, Zhou J, Samsom J, Wong AHC, and Liu F

Subjects
Female, Humans, Male, Proteomics, Antipsychotic Agents therapeutic use, Nerve Tissue Proteins genetics, Receptors, Dopamine D2 genetics, Schizophrenia genetics
Abstract

Background: For decades, the dopamine D2 receptor (D2R) has been known as the main target of antipsychotic medications, but the mechanism for antipsychotic effects beyond this pharmacological target remains unclear. Disrupted-in-schizophrenia 1 ( DISC1 ) is a gene implicated in the etiology of schizophrenia, and we have found elevated levels of the D2R-DISC1 complex in the postmortem brain tissue of patients with schizophrenia., Methods: We used coimmunoprecipitation to measure D2R-DISC1 complex levels in peripheral blood samples from patients with schizophrenia and unaffected controls in 3 cohorts (including males and females) from different hospitals. We also used label-free mass spectrometry to conduct proteomic analysis of these samples., Results: Levels of the D2R-DISC1 complex were elevated in the peripheral blood samples of patients with schizophrenia from 3 independent cohorts, and were normalized with antipsychotic treatment. Proteomic analysis of the blood samples from patients with high D2R-DISC1 complex levels that were normalized with antipsychotic treatment revealed a number of altered proteins and pathways associated with D2R, DISC1 and the D2R-DISC1 complex. We identified additional proteins and pathways that were associated with antipsychotic treatment in schizophrenia, and that may also be novel targets for schizophrenia treatment., Limitations: Sample sizes were relatively small, but were sufficient to detect associations between D2R-DISC1 levels, schizophrenia and treatment response. The relevance of leukocyte changes to the symptoms of schizophrenia is unknown. The coimmunoprecipitation lanes included several nonspecific bands., Conclusion: Levels of the D2R-DISC1 complex were elevated in patients with schizophrenia and reduced with antipsychotic treatment. This finding reinforces the independent role of each protein in schizophrenia. Our results enhanced our understanding of the molecular pathways involved in schizophrenia and in antipsychotic medications, and identified novel potential molecular targets for treating schizophrenia., Competing Interests: Competing interests: A.H.C. Wong reports consulting fees and stock from FSD Pharma. No other competing interests declared., (© 2022 CMA Impact Inc. or its licensors.)

Published
2022
Full Text
View/download PDF

46. Inhibition of the G9a/GLP histone methyltransferase complex modulates anxiety-related behavior in mice.

Author

Wang DY, Kosowan J, Samsom J, Leung L, Zhang KL, Li YX, Xiong Y, Jin J, Petronis A, Oh G, and Wong AHC

Subjects
Animals, Diazepam therapeutic use, Dose-Response Relationship, Drug, Epigenesis, Genetic, Female, Histones genetics, Histones metabolism, Male, Methylation, Mice, Inbred C57BL, Protein Processing, Post-Translational, Venlafaxine Hydrochloride therapeutic use, Anti-Anxiety Agents therapeutic use, Histone-Lysine N-Methyltransferase antagonists & inhibitors, Indoles therapeutic use, Quinazolines therapeutic use, Spiro Compounds therapeutic use
Abstract

Epigenetic gene-regulation abnormalities have been implicated in various neuropsychiatric disorders including schizophrenia and depression, as well as in the regulation of mood and anxiety. In addition, epigenetic mechanisms are involved in the actions of psychiatric drugs. Current anxiolytic drugs have significant shortcomings, and development of new medications is warranted. Two proteins, G9a (also known as EHMT2 or KMT1C) and GLP (G9a-like protein, also known as EHMT1 or KMT1D), which methylate lysine 9 of histone H3 (H3K9), could be promising anxiolytic targets. Postnatal genetic knock-out of G9a reduces anxiety-related behavior, consistent with the reduction of G9a levels by some medications used to treat anxiety (amitriptyline, imipramine and paroxetine). Conversely, there is increased anxiety-like behavior in mice with GLP haplodeficiency. We sought to determine whether two pharmacological inhibitors of G9a/GLP, UNC0642 and A-366, would have similar effects to genetic G9a/GLP insufficiency. We found that G9a/GLP inhibition with either compound reduced anxiety-like behaviors when administered to adult mice, in conjunction with decreased H3K9 methylation in the brain. In contrast, exposure to these compounds from embryonic day 9.5 (E9.5) until birth increased anxiety-like behaviors and decreased social interaction in adulthood, while H3K9 methylation was at normal levels in the brains of the adult mice. These findings reinforce genetic evidence that G9a/GLP has different effects on anxiety-like behavior at different stages of brain development, and suggest that targeting this histone methyltransferase pathway could be useful for developing new anxiolytic drugs. These data also suggest that antidepressant exposure in utero could have negative effects in adulthood, and further investigation of these effects is warranted.

Published
2018
Full Text
View/download PDF

47. Campylobacter jejuni translocation across intestinal epithelial cells is facilitated by ganglioside-like lipooligosaccharide structures.

Author

Louwen R, Nieuwenhuis EE, van Marrewijk L, Horst-Kreft D, de Ruiter L, Heikema AP, van Wamel WJ, Wagenaar JA, Endtz HP, Samsom J, van Baarlen P, Akhmanova A, and van Belkum A

Subjects
Cell Line, Chemokine CXCL10 metabolism, Endocytosis, Humans, Microscopy, Fluorescence, Bacterial Translocation, Campylobacter jejuni pathogenicity, Epithelial Cells microbiology, Gangliosides metabolism, Lipopolysaccharides metabolism
Abstract

Translocation across intestinal epithelial cells is an established pathogenic feature of the zoonotic bacterial species Campylobacter jejuni. The number of C. jejuni virulence factors known to be involved in translocation is limited. In the present study, we investigated whether sialylation of C. jejuni lipooligosaccharide (LOS) structures, generating human nerve ganglioside mimics, is important for intestinal epithelial translocation. We here show that C. jejuni isolates expressing ganglioside-like LOS bound in larger numbers to the Caco-2 intestinal epithelial cells than C. jejuni isolates lacking such structures. Next, we found that ganglioside-like LOS facilitated endocytosis of bacteria into Caco-2 cells, as visualized by quantitative microscopy using the early and late endosomal markers early endosome-associated protein 1 (EEA1), Rab5, and lysosome-associated membrane protein 1 (LAMP-1). This increased endocytosis was associated with larger numbers of surviving and translocating bacteria. Next, we found that two different intestinal epithelial cell lines (Caco-2 and T84) responded with an elevated secretion of the T-cell attractant CXCL10 to infection by ganglioside-like LOS-expressing C. jejuni isolates. We conclude that C. jejuni translocation across Caco-2 cells is facilitated by ganglioside-like LOS, which is of clinical relevance since C. jejuni ganglioside-like LOS-expressing isolates are linked with severe gastroenteritis and bloody stools in C. jejuni-infected patients.

Published
2012
Full Text
View/download PDF

48. Differences in behavioral outcome and motor development at school age after neonatal treatment for chronic lung disease with dexamethasone versus hydrocortisone.

Author

Karemaker R, Heijnen CJ, Veen S, Baerts W, Samsom J, Visser GH, Kavelaars A, van Doornen LJ, and van Bel F

Subjects
Anti-Inflammatory Agents adverse effects, Anti-Inflammatory Agents pharmacology, Child, Child Behavior physiology, Child Development drug effects, Child Development physiology, Chronic Disease, Cohort Studies, Dexamethasone adverse effects, Dexamethasone pharmacology, Female, Glucocorticoids adverse effects, Glucocorticoids pharmacology, Humans, Hydrocortisone adverse effects, Hydrocortisone pharmacology, Infant, Newborn, Male, Mental Disorders etiology, Mental Disorders physiopathology, Motor Activity physiology, Motor Skills Disorders etiology, Motor Skills Disorders physiopathology, Retrospective Studies, Surveys and Questionnaires, Treatment Outcome, Anti-Inflammatory Agents therapeutic use, Child Behavior drug effects, Dexamethasone therapeutic use, Glucocorticoids therapeutic use, Hydrocortisone therapeutic use, Motor Activity drug effects, Respiratory Distress Syndrome, Newborn drug therapy
Abstract

Neonatal dexamethasone (DEX) for chronic lung disease is associated with adverse outcome. We compared behavioral and motor development at school age of children who neonatally received DEX to children neonatally treated with hydrocortisone (HC) in a retrospective matched cohort study. DEX- and HC-treated groups matched for gestational age, birth weight and year, gender, and severity of respiratory distress syndrome were compared with a reference group (REF) and a group treated only antenatally with betamethasone (BMETH). REF and BMETH groups had a higher gestational age and less severe respiratory distress syndrome. From 192 children (DEX, n = 46; HC, n = 52; REF, n = 43; BMETH, n = 51), the Child Behavioral Checklists from parents and teachers (Teacher's Report Form) and the Movement Assessment Battery for Children to assess neuromotor function were analyzed. DEX girls had a poorer performance on nearly all behavioral scales of the Teacher's Report Form compared with HC girls. DEX boys did not differ from HC boys. The HC boys or girls did not differ from the REF or BMETH groups. Neuromotor development was poorer in DEX than the BMETH and REF groups. The HC group did not differ from REF and BMETH groups. We suggest that neonatal HC may be a "safer" alternative for DEX for the treatment of CLD.

Published
2006
Full Text
View/download PDF

49. Discrimination of different subsets of cytolytic cells in pseudorabies virus-immune and naive pigs.

Author

de Bruin TG, van Rooij EM, de Visser YE, Voermans JJ, Samsom JN, Kimman TG, and Bianchi AT

Subjects
Animals, Antibodies, Monoclonal, Antigens, CD analysis, Antigens, CD immunology, Antigens, Differentiation, T-Lymphocyte immunology, Cell Separation methods, Cells, Cultured, Immunophenotyping, Interleukin-2 pharmacology, Leukocytes, Mononuclear cytology, Lymphocyte Subsets cytology, Lymphocyte Subsets immunology, Lymphocytes cytology, Swine, Swine, Miniature, Cytotoxicity, Immunologic immunology, Herpesvirus 1, Suid immunology, Lymphocyte Subsets classification
Abstract

We previously observed that pseudorabies virus (PRV)-induced, cell-mediated cytolysis in pigs includes killing by natural killer (NK) cells. We also observed that IL-2 stimulation in vitro of naive PBMC expands porcine NK cells. The purpose of this study was to compare the phenotypes of the cytolytic subsets stimulated in vitro by PRV and by IL-2. PBMC were isolated from blood of PRV-immune and naive pigs and stimulated in vitro with PRV or IL-2. After 6 days, the frequency of various lymphocyte subsets in these cultured PBMC was determined by flow cytometry: the cells were separated with a magnet-activated cell sorter and the cytolytic activity of the separated populations was determined. When lymphocytes were separated and analysed with FACScan, the following lymphocyte subsets were discriminated: CD6(+) CD8(bright+) CD4(-) (CTL phenotype), CD6(+) CD8(dull+) CD4(+) (the fraction containing memory T helper cells), CD6(+) CD8(-) CD4(+) (T helper cell phenotype), CD6(-) CD8(dull+) CD4(-) gammadelta-T(+) ( gammadelta-T cell phenotype), CD6(-) CD8(dull+) CD4(-) gammadelta-T(-) (NK phenotype) and CD6(-) CD8(-) CD4(-) gammadelta-T(-) or gammadelta-T(+). Flow cytometry analysis demonstrated that PRV stimulation of immune PBMC resulted in the occurrence of more CD6(+) CD8(+) and CD4(+) CD8(+) and fewer CD6(-) CD8(+) and gammadelta-T(+) CD8(+) lymphocytes than IL-2 stimulation of naive PBMC (P<0.05). It was demonstrated further that killing by PRV-stimulated PBMC was mediated mainly by CD6(+) CD8(+) T lymphocytes. Killing by IL-2-stimulated PBMC was mediated mainly by CD6(-) CD8(+) T lymphocytes. These results demonstrate that both natural killing and killing by classical PRV-specific CTL were detected in PRV-immune pigs, whereas IL-2 stimulation of PBMC isolated from naive pigs mainly induced natural killing.

Published
2000
Full Text
View/download PDF

50. Changes of leukocyte phenotype and function in the broncho-alveolar lavage fluid of pigs infected with porcine reproductive and respiratory syndrome virus: a role for CD8(+) cells.

Author

Samsom JN, de Bruin TG, Voermans JJ, Meulenberg JJ, Pol JM, and Bianchi AT

Subjects
Animals, Bronchoalveolar Lavage Fluid cytology, CD8-Positive T-Lymphocytes pathology, Cell Count, Flow Cytometry, Germ-Free Life, Immunophenotyping, Killer Cells, Natural immunology, Killer Cells, Natural pathology, Lung immunology, Lung pathology, Porcine Reproductive and Respiratory Syndrome pathology, Porcine respiratory and reproductive syndrome virus pathogenicity, Specific Pathogen-Free Organisms, Swine, Bronchoalveolar Lavage Fluid immunology, CD8-Positive T-Lymphocytes immunology, Porcine Reproductive and Respiratory Syndrome immunology
Abstract

Porcine reproductive and respiratory virus (PRRSV) primarily infects and destroys alveolar macrophages of the pig. The aim of the present study was to characterize the changes of leukocyte populations in the broncho-alveolar lavage fluid (BALF) of PRRSV-infected pigs. Piglets were inoculated intranasally with PRRSV strain LV ter Huurne. On various days post-infection the piglets were sacrificed and the lungs removed, washed semi-quantitatively and analysed by flow cytometry. The total number of recovered BALF cells increased approximately 10 times between day 10 and day 21 of infection and decreased thereafter. The number of small low-autofluorescent cells (SLAC), i.e. lymphocytic and monocytic cells, increased very strongly from day 2 until day 21 of infection; in contrast, the number of large highly autofluorescent cells (LHAC), i.e. mostly macrophages, remained constant until day 14 of infection, increased slightly on day 21 and then decreased. On day 21 of infection in specific-pathogen-free piglets approximately 60% of the SLAC consisted of CD2(+)CD8(+)CD4(-)gammadeltaTCR(-) cells, which were partly CD8(+)CD6(+) and partly CD8(+)CD6(-). These phenotypes correspond to that of cytotoxic T-cells and natural killer cells respectively. From these results we can conclude that during a PRRSV infection the total number of BALF cells increases mainly due to an influx of lymphocytic cells with a cytolytic phenotype.

Published
2000
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results