Your search keyword '"Samsom, J.N. (Janneke)"' showing total 18 results

1. First-line treatment with infliximab versus conventional treatment in children with newly diagnosed moderate-to-severe Crohn's disease: An open-label multicentre randomised controlled trial

Author

Jongsma, M.M.E. (Maria), Aardoom, M.A. (Martine A.), Cozijnsen, M.A. (Maarten), Pieterson, M. (Merel) van, de Meij, T. (Tim), Groeneweg, M. (Michael), Norbruis, O.F. (Obbe), Wolters, V.M. (Victorien M.), Van Wering, H. (Herbert), Hojsak, I. (Iva), Kolho, K.-L. (Kaija-Leena), Hummel, T.Z., Stapelbroek, J.M. (Janneke), Van Der Feen, C. (Cathelijne), Rheenen, P.F. (Patrick) van, Wijk, M.P. (Michiel) van, Teklenburg-Roord, S.T.A. (Sarah T. A.), Schreurs, M.W.J. (Marco), Rizopoulos, D. (Dimitris), Doukas, M. (Michael), Escher, J.C. (Johanna C.), Samsom, J.N. (Janneke), Ridder, L. (Lissy) de, Jongsma, M.M.E. (Maria), Aardoom, M.A. (Martine A.), Cozijnsen, M.A. (Maarten), Pieterson, M. (Merel) van, de Meij, T. (Tim), Groeneweg, M. (Michael), Norbruis, O.F. (Obbe), Wolters, V.M. (Victorien M.), Van Wering, H. (Herbert), Hojsak, I. (Iva), Kolho, K.-L. (Kaija-Leena), Hummel, T.Z., Stapelbroek, J.M. (Janneke), Van Der Feen, C. (Cathelijne), Rheenen, P.F. (Patrick) van, Wijk, M.P. (Michiel) van, Teklenburg-Roord, S.T.A. (Sarah T. A.), Schreurs, M.W.J. (Marco), Rizopoulos, D. (Dimitris), Doukas, M. (Michael), Escher, J.C. (Johanna C.), Samsom, J.N. (Janneke), and Ridder, L. (Lissy) de

Abstract

Objective: In newly diagnosed paediatric patients with moderate-to-severe Crohn's disease (CD), infliximab (IFX) is initiated once exclusive enteral nutrition (EEN), corticosteroid and immunomodulator therapies have failed. We aimed to investigate whether starting first-line IFX (FL-IFX) is more effective to achieve and maintain remission than conventional treatment. Design: In this multicentre open-label randomised controlled trial, untreated patients with a new diagnosis of CD (3-17 years old, weighted Paediatric CD Activity Index score (wPCDAI) >40) were assigned to groups that received five infusions of 5 mg/kg IFX at weeks 0, 2, 6, 14 and 22 (FL-IFX), or EEN or oral prednisolone (1 mg/kg, maximum 40 mg) (conventional). The primary outcome was clinical remission on azathioprine, defined as a wPCDAI <12.5 at week 52, without need for treatment escalation, using intention-to-treat analysis. Results: 100 patients were included, 50 in the FL-IFX group and 50 in the conventional group. Four patients did not receive treatment as per protocol. At week 10, a higher proportion of patients in the FL-IFX group than in the conventional group achieved clinical (59% vs 34%, respectively, p=0.021) and endoscopic remission (59% vs 17%, respectively, p=0.001). At week 52, the proportion of patients in clinical remission was not

Published

2021

2. International prospective observational study investigating the disease course and heterogeneity of paediatric-onset inflammatory bowel disease: the protocol of the PIBD-SETQuality inception cohort study

Author

Aardoom, M.A. (Martine A.), Kemos, P. (Polychronis), Tindemans, I. (Irma), Aloi, M. (Marina), Koletzko, S. (Sybille), Levine, A. (Arie), Turner, D. (Dan), Veereman, G. (Gigi), Neyt, M. (Mattias), Russell, R.K. (Richard), Walters, T.D. (Thomas D.), Ruemmele, F.M. (Frank), Samsom, J.N. (Janneke), Croft, N.M. (Nicholas M.), Ridder, L. (Lissy) de, Aardoom, M.A. (Martine A.), Kemos, P. (Polychronis), Tindemans, I. (Irma), Aloi, M. (Marina), Koletzko, S. (Sybille), Levine, A. (Arie), Turner, D. (Dan), Veereman, G. (Gigi), Neyt, M. (Mattias), Russell, R.K. (Richard), Walters, T.D. (Thomas D.), Ruemmele, F.M. (Frank), Samsom, J.N. (Janneke), Croft, N.M. (Nicholas M.), and Ridder, L. (Lissy) de

Abstract

INTRODUCTION: Patients with paediatric-onset inflammatory bowel disease (PIBD) may develop a complicated disease course, including growth failure, bowel resection at young age and treatment-related adverse events, all of which can have significant and lasting effects on the patient's development and quality of life. Unfortunately, we are still not able to fully explain the heterogeneity between patients and their disease course and predict which patients will respond to certain therapies or are most at risk of developing a more complicated disease course. To investigate this, large prospective studies with long-term follow-up are needed. Currently, no such European or Asian international cohorts exist. In this international cohort, we aim to evaluate disease course and which patients are most at risk of therapy non-response or development of complicated disease based on patient and disease characteristics, immune pathology and environmental and socioeconomic factors. METHODS AND ANALYSIS: In this international prospective observational study, which is part of the PIBD Network for Safety, Efficacy, Treatment and Quality improvement of care (PIBD-SETQuality), children diagnosed with inflammatory bowel disease <18 years are included at diagnosis. The follow-up schedule is in line with standard PIBD care and is intended to continue up to 20 years. Patient and disease characteristics, as well as results of investigations, are collected at baseline and during follow-up. In addition, environmental factors are being assessed (eg, parent's smoking behaviour, dietary factors and antibiotic use). In specific centres with the ability to perform extensive immunological analyses, blood samples and intestinal biopsies are being collected and analysed (flow cytometry, plasma proteomics, mRNA expression and immunohistochemistry) in therapy-naïve patients and during follow-up. ETHICS AND DISSEMINATION: Medical ethical approval has been obtained prior to patient recruitment for all si

Published

2020

3. Yap1-Driven Intestinal Repair Is Controlled by Group 3 Innate Lymphoid Cells

Author

Romera Hernández, M. (Mónica), Aparicio-Domingo, P. (Patricia), Papazian, N. (Natalie), Karrich, J.J. (Julien J.), Cornelissen, F.H.J. (Ferry), Hoogenboezem, R.M. (Remco), Samsom, J.N. (Janneke), Cupedo, T. (Tom), Romera Hernández, M. (Mónica), Aparicio-Domingo, P. (Patricia), Papazian, N. (Natalie), Karrich, J.J. (Julien J.), Cornelissen, F.H.J. (Ferry), Hoogenboezem, R.M. (Remco), Samsom, J.N. (Janneke), and Cupedo, T. (Tom)

Abstract

Intestinal repair is driven by epithelial stem cells, but how these stem cells are instructed to initiate repair was unknown. Here, Romera-Hernández et al. report that epithelial proliferation after damage is independent of the stem cell-protective signal IL-22 but requires ILC3-dependent amplification of regenerative YAP1 signaling in stem cells.Tissue repair requires temporal control of progenitor cell proliferation and differentiation to replenish damaged cells. In response to acute insult, group 3 innate lymphoid cells (ILC3s) regulate intestinal stem cell maintenance and subsequent tissue repair. ILC3-derived IL-22 is important for stem cell protection, but the mechanisms of ILC3-driven tissue regeneration remain incompletely defined. Here we report that ILC3-driven epithelial proliferation and tissue regeneration are independent of IL-22. In contrast, ILC3s amplify the magnitude of Hippo-Yap1 signaling in intestinal crypt cells, ensuring adequate initiation of tissue repair and preventing excessive pathology. Mechanistically, ILC3-driven tissue repair is Stat3 indepen

Published

2020

4. Expression of Plet1 controls interstitial migration of murine small intestinal dendritic cells

Author

Karrich, J.J. (Julien J.), Romera Hernández, M. (Mónica), Papazian, N. (Natalie), Veenbergen, S. (Sharon), Cornelissen, F.H.J. (Ferry), Aparicio-Domingo, P. (Patricia), Stenhouse, F.H. (Frances), Peddie, C.D. (C. Diana), Hoogenboezem, R.M. (Remco), den Hollander, C.W.J. (Chelsea W. J.), Gaskell, T. (Terri), Medley, T. (Tanya), Boon, L. (Louis), Blackburn, C.C. (C. Clare), Withers, D.R. (David R.), Samsom, J.N. (Janneke), Cupedo, T. (Tom), Karrich, J.J. (Julien J.), Romera Hernández, M. (Mónica), Papazian, N. (Natalie), Veenbergen, S. (Sharon), Cornelissen, F.H.J. (Ferry), Aparicio-Domingo, P. (Patricia), Stenhouse, F.H. (Frances), Peddie, C.D. (C. Diana), Hoogenboezem, R.M. (Remco), den Hollander, C.W.J. (Chelsea W. J.), Gaskell, T. (Terri), Medley, T. (Tanya), Boon, L. (Louis), Blackburn, C.C. (C. Clare), Withers, D.R. (David R.), Samsom, J.N. (Janneke), and Cupedo, T. (Tom)

Abstract

Under homeostatic conditions, dendritic cells (DCs) continuously patrol the intestinal lamina propria. Upon antigen encounter, DCs init

Published

2018

5. Ceramides in tracheal aspirates of preterm infants: Marker for bronchopulmonary dysplasia

Author

Mastrigt, E. (Esther) van, Zweekhorst, S. (Salomé), Bol, B.S. (Bas), Tibboel, J. (Jeroen), Rosmalen, J.M. (Joost) van, Samsom, J.N. (Janneke), Kroon, A.A. (André A.), De Jongste, J.C. (Johan C.), Reiss, I.K.M. (Irwin), Post, M. (Martin), Pijnenburg, M.W.H. (Mariëlle), Mastrigt, E. (Esther) van, Zweekhorst, S. (Salomé), Bol, B.S. (Bas), Tibboel, J. (Jeroen), Rosmalen, J.M. (Joost) van, Samsom, J.N. (Janneke), Kroon, A.A. (André A.), De Jongste, J.C. (Johan C.), Reiss, I.K.M. (Irwin), Post, M. (Martin), and Pijnenburg, M.W.H. (Mariëlle)

Abstract

Background In an experimental mouse model we showed that ceramides play a role in the pathogenesis of bronchopulmonary dysplasia (BPD) and are a potential target for therapeutic intervention. We investigated whether ceramides are detectable in tracheal aspirates (TAs) of preterm infants and differ between infants with or without BPD. Methods Infants born 32 weeks of gestational age in need of mechanical ventilation in the first week of life were included. TAs were obtained directly after intubation and at day 1, 3, 5, 7, and 14. Ceramide concentrations were measured by tandem mass spectrometry. At 36 weeks postmenstrual age BPD was defined as having had 28 days supplemental oxygen. Results 122 infants were included, of which 14 died and 41 developed BPD. All infants showed an increase in ceramides after the first day of intubation. The ceramide profile differed significantly between preterm infants who did and did not develop BPD. However, the ceramide profile had no additional predictive value for BPD development over GA at birth, birth weight and total days of mechanical ventilation. Conclusions Ceramides are measurable in TAs of preterm born infants and may be an early marker for BPD development.

Published

2018

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

Author

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

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

7. Top-down Infliximab Study in Kids with Crohn's disease (TISKids): an international multicentre randomised controlled trial

Author

Cozijnsen, M.A. (Maarten), Pieterson, M. (Merel) van, Samsom, J.N. (Janneke), Escher, J.C. (Johanna), Ridder, L. (Lissy) de, Cozijnsen, M.A. (Maarten), Pieterson, M. (Merel) van, Samsom, J.N. (Janneke), Escher, J.C. (Johanna), and Ridder, L. (Lissy) de

Abstract

Copyright

Published

2016

8. Type 3 innate lymphoid cells maintain intestinal epithelial stem cells after tissue damage

Author

Aparicio-Domingo, P. (Patricia), Romera Hernández, M. (Mónica), Karrich, J.J. (Julien J.), Cornelissen, F.H.J. (Ferry), Papazian, N. (Natalie), Lindenbergh-Kortleve, D.J. (Dicky), Butler, J.A. (James A.), Boon, L. (Louis), Coles, M. (Mark), Samsom, J.N. (Janneke), Cupedo, T. (Tom), Aparicio-Domingo, P. (Patricia), Romera Hernández, M. (Mónica), Karrich, J.J. (Julien J.), Cornelissen, F.H.J. (Ferry), Papazian, N. (Natalie), Lindenbergh-Kortleve, D.J. (Dicky), Butler, J.A. (James A.), Boon, L. (Louis), Coles, M. (Mark), Samsom, J.N. (Janneke), and Cupedo, T. (Tom)

Abstract

Disruption of the intestinal epithelial barrier allows bacterial translocation and predisposes to destructive inflammation. To ensure proper barrier composition, crypt-residing stem cells continuously proliferate and replenish all intestinal epithelial cells within days. As a consequence of this high mitotic activity, mucosal surfaces are frequently targeted by anticancer therapies, leading to dose-limiting side effects. The cellular mechani

Published

2015

9. Faecalibacterium prausnitzii strain HTF-F and its extracellular polymeric matrix attenuate clinical parameters in DSS-induced colitis

Author

Rossi, O. (Oriana), Khan, M.T. (M. Tanweer), Schwarzer, M. (Martin), Hudcovic, T. (Tomas), Srutkova, D. (Dagmar), Duncan, S.H. (Sylvia H.), Stolte, E.H. (Ellen), Kozakova, H. (Hana), Flint, H.J. (Harry J.), Samsom, J.N. (Janneke), Harmsen, H.J.M. (Hermie J. M.), Wells, J.M. (Jerry), Rossi, O. (Oriana), Khan, M.T. (M. Tanweer), Schwarzer, M. (Martin), Hudcovic, T. (Tomas), Srutkova, D. (Dagmar), Duncan, S.H. (Sylvia H.), Stolte, E.H. (Ellen), Kozakova, H. (Hana), Flint, H.J. (Harry J.), Samsom, J.N. (Janneke), Harmsen, H.J.M. (Hermie J. M.), and Wells, J.M. (Jerry)

Abstract

A decrease in the abundance and biodiversity of intestinal bacteria within the Firmicutes phylum has been associated with inflammatory bowel disease (IBD). In particular, the anti-inflammatory bacterium Faecalibacterium prausnitzii, member of the Firmicutes phylum and one of the most abundant species in healthy human colon, is underrepresented in the microbiota of IBD patients. The aim of this study was to investigate the immunomodulatory properties of F. prausnitzii strain A2-165, the biofilm forming strain HTF-F and the extracellular polymeric matrix (EPM) isolated from strain HTF-F. For this purpose, the immunomodulatory properties of the F. prausnitzii strains and the EPM were studied in vitro using human monocyte-derived dendritic cells. Then, the capacity of the F. prausnitzii strains and the EPM of HTF-F to suppress inflammation was assessed in vivo in the mouse dextran sodium sulphate (DSS) colitis model. The F. prausnitzii strains and the EPM had anti-inflammatory effects on the clinical parameters measured in the DSS model but with different efficacy. The immunomodulatory effects of the EPM were mediated through the TLR2-dependent modulation of IL-12 and IL-10 cytokine production in antigen presenting cells, suggesting that it contributes to the anti-inflammatory potency of F. prausnitzii HTF-F. The results show that F. prausnitzii HTF-F and its EPM may have a therapeutic use in IBD.

Published

2015

10. Interleukin-10 receptor signaling in innate immune cells regulates mucosal immune tolerance and anti-inflammatory macrophage function

Author

Shouval, D.S. (Dror), Biswas, R.S. (Rajat), Goettel, J.A. (Jeremy), McCann, K. (Katelyn), Conaway, E. (Evan), Redhu, N.S. (Naresh), Mascanfroni, I.D. (Ivan), AlAdham, Z. (Ziad), Lavoie, S. (Sydney), Ibourk, M. (Mouna), Nguyen, D.D. (Deanna), Samsom, J.N. (Janneke), Escher, J.C. (Johanna), Somech, R. (Raz), Weiss, B. (Batia), Beier, R. (Rita), Conklin, L.S. (Laurie), Ebens, C.L. (Christen), Santos, F.G.M.S. (Fernanda), Ferreira, A.R. (Alexandre), Sherlock, J.K. (Jon), Bhan, A.K. (Atul), Müller, W. (Werner), Mora, J.R. (J. Rodrigo), Quintana, F.J. (Francisco), Klein, C. (Christoph), Muise, A.M. (Aleixo), Horwitz, R.I. (Ralph), Snapper, S.B. (Scott), Shouval, D.S. (Dror), Biswas, R.S. (Rajat), Goettel, J.A. (Jeremy), McCann, K. (Katelyn), Conaway, E. (Evan), Redhu, N.S. (Naresh), Mascanfroni, I.D. (Ivan), AlAdham, Z. (Ziad), Lavoie, S. (Sydney), Ibourk, M. (Mouna), Nguyen, D.D. (Deanna), Samsom, J.N. (Janneke), Escher, J.C. (Johanna), Somech, R. (Raz), Weiss, B. (Batia), Beier, R. (Rita), Conklin, L.S. (Laurie), Ebens, C.L. (Christen), Santos, F.G.M.S. (Fernanda), Ferreira, A.R. (Alexandre), Sherlock, J.K. (Jon), Bhan, A.K. (Atul), Müller, W. (Werner), Mora, J.R. (J. Rodrigo), Quintana, F.J. (Francisco), Klein, C. (Christoph), Muise, A.M. (Aleixo), Horwitz, R.I. (Ralph), and Snapper, S.B. (Scott)

Abstract

Intact interleukin-10 receptor (IL-10R) signaling on effector and T regulatory (Treg) cells are each independently required to maintain immune tolerance. Here we show that IL-10 sensing by innate immune cells, independent of its effects on Tcells, was critical for regulating mucosal homeostasis. Following wild-type (WT) CD4+ Tcell transfer, Rag2-/-Il10rb-/- mice developed severe colitis in association with profound defects in generation and function of Treg cells. Moreover, loss of IL-10R signaling impaired the generation and function of anti-inflammatory intestinal and bone-marrow-derived macrophages and their ability to secrete IL-10. Importantly, transfer of WT but not Il10rb-/- anti-inflammatory macrophages ameliorated colitis induction by

Published

2014

11. Ontogeny of human hepatic and intestinal transporter gene expression during childhood: Age matters

Author

Mooij, M.G. (Miriam), Schwarz, U.I. (Ute), Koning, B.A.E. (Barbara) de, Leeder, D., Gaedigk, R. (Roger), Samsom, J.N. (Janneke), Spaans, E. (Edwin), Goudoever, J.B. (Hans) van, Tibboel, D. (Dick), Kim, R.B. (Richard), Wildt, S.N. (Saskia) de, Mooij, M.G. (Miriam), Schwarz, U.I. (Ute), Koning, B.A.E. (Barbara) de, Leeder, D., Gaedigk, R. (Roger), Samsom, J.N. (Janneke), Spaans, E. (Edwin), Goudoever, J.B. (Hans) van, Tibboel, D. (Dick), Kim, R.B. (Richard), and Wildt, S.N. (Saskia) de

Abstract

Many drugs prescribed to children are drug transporter substrates. Drug transporters are membrane-bound proteins that mediate the cellular uptake or efflux of drugs and are important to drug absorption and elimination. Very limited data are available on the effect of age on transporter expression. Our study assessed age-related gene expression of hepatic and intestinal drug transporters. Multidrug resistance protein 2 (MRP2), organic anion transporting polypeptide 1B1 (OATP1B1), and OATP1B3 expression was determined in postmortem liver samples (fetal n = 6, neonatal n = 19, infant n = 7, child n = 2, adult n = 11) and multidrug resistance 1 (MDR1) expression in 61 pediatric liver samples. Intestinal expression of MDR1, MRP2, and OATP2B1 was determined in surgical small bowel samples (neonates n = 15, infants n = 3, adults n = 14). Using real-time reverse-transcription polymerase chain reaction, we measured fetal and pediatric gene expression relative to 18S rRNA (liver) and villin (intestines), and we compared it with adults using the 22 -Delta;Delta;Ct method. Hepatic expression of MRP2, OATP1B1, and OATP1B3 in all pediatric age groups was significantly lower than in adults. Hepatic MDR1 mRNA expression in fetuses, neonates, and infants was significantly lower than in adults. Neonatal intestinal expressions of MDR1 and MRP2 were comparable to those in adults. Intestinal OATP2B1 expression in neonates was significantly higher than in adults. We provide new data that show organ- and transporter-dependent differences in hepatic and intestinal drug transporter expression in an age-dependent fashion. This suggests that substrate drug absorption mediated by these transp

Published

2014

12. Changes in Natural Foxp3+Treg but Not Mucosally-Imprinted CD62LnegCD38+Foxp3+Treg in the Circulation of Celiac Disease Patients

Author

Van Leeuwen, M.A. (Marieke), Pré, M.F. (Fleur) du, Wanrooij, R.L.J. (Roy) van, Ruiter, L.F. (Lilian) de, Raatgeep, R.H. (Rolien), Lindenbergh-Kortleve, D.J. (Dicky), Mulder, C.J.J. (Chris), Ridder, L. (Lissy) de, Escher, J.C. (Johanna), Samsom, J.N. (Janneke), Van Leeuwen, M.A. (Marieke), Pré, M.F. (Fleur) du, Wanrooij, R.L.J. (Roy) van, Ruiter, L.F. (Lilian) de, Raatgeep, R.H. (Rolien), Lindenbergh-Kortleve, D.J. (Dicky), Mulder, C.J.J. (Chris), Ridder, L. (Lissy) de, Escher, J.C. (Johanna), and Samsom, J.N. (Janneke)

Abstract

Background:Celiac disease (CD) is an intestinal inflammation driven by gluten-reactive CD4+ T cells. Due to lack of selective markers it has not been determined whether defects in inducible regulatory T cell (Treg) differentiation are associated with CD. This is of importance as changes in numbers of induced Treg could be indicative of defects in mucosal tolerance development in CD. Recently, we have shown that, after encounter of retinoic acid during differentiation, circulating gut-imprinted T cells express CD62LnegCD38+. Using this new phenotype, we now determined whether alterations occur in the frequency of natural CD62L+Foxp3+ Treg or mucosally-imprinted CD62LnegCD38+Foxp3+ Treg in peripheral blood of CD patients. In particular, we compared pediatric CD, aiming to select for disease at onset, with adult CD.Methods:Cell surface markers, intracellular Foxp3 and Helios were determined by flow cytometry. Foxp3 expression was also detected by immunohistochemistry in duodenal tissue of CD patients.Results:In children, the percentages of peripheral blood CD4+Foxp3+ Treg were comparable between CD patients and healthy age-matched controls. Differentiation between natural and mucosally-imprinted Treg on the basis of CD62L and CD38 did not uncover differences in Foxp3. In adult patients on gluten-free diet and in refractory CD increased percentages of circulating natural CD62L+Foxp3+ Treg, but normal mucosally-imprinted CD62LnegCD38+Foxp3+ Treg frequencies were observed.Conclusions:Our data exclude that significant numeric deficiency of mucosally-imprinted or natural Foxp3+ Treg explains exuberant effector responses in CD. Changes in natural Foxp3+ Treg occur in a subset of adult patients on a gluten-free diet and in refractory CD patients.

Published

2013

13. Gene expression analysis of peripheral cells for subclassification of pediatric inflammatory bowel disease in remission

Author

Lierop, P.P.E. (Pieter) van, Swagemakers, S.M.A. (Sigrid), Bie, C.I. (Charlotte) de, Middendorp, S., Baarlen, P. (Peter) van, Samsom, J.N. (Janneke), IJcken, W.F.J. (Wilfred) van, Escher, J.C. (Johanna), Spek, P.J. (Peter) van der, Nieuwenhuis, E.E.S. (Edward), Lierop, P.P.E. (Pieter) van, Swagemakers, S.M.A. (Sigrid), Bie, C.I. (Charlotte) de, Middendorp, S., Baarlen, P. (Peter) van, Samsom, J.N. (Janneke), IJcken, W.F.J. (Wilfred) van, Escher, J.C. (Johanna), Spek, P.J. (Peter) van der, and Nieuwenhuis, E.E.S. (Edward)

Abstract

Objective: In current clinical practice, optimal treatment of inflammatory bowel disease (IBD) aims at the induction and maintenance of clinical remission. Clinical remission is apparent when laboratory markers of inflammation are normal and clinical symptoms are absent. However, sub-clinical inflammation can still be present. A detailed analysis of the immune status during this inactive state of disease may provide a useful tool to categorize patients with clinical remission into subsets with variable states of immune activation. Design: By using Affymetrix GeneChips, we analysed RNA gene expression profiles of peripheral blood leukocytes from pediatric IBD patients in clinical remission and controls. We performed (un)supervised clustering analysis of IBD-associated genes and applied Ingenuity® pathway software to identify specific molecular profiles between patients. Results: Pediatric IBD patients with disease in clinical remission display heterogeneously distributed gene expression profiles that are significantly distinct from controls. We identified three clusters of IBD patients, each displaying specific expression profiles of IBD-associated genes. Conclusion: The expression of immune- and IBD-associated genes in peripheral blood leukocytes from pediatric IBD patients in clinical remission was different from healthy controls, indicating that sub-clinical immune mechanisms are still active during remission. As such, RNA profiling of peripheral blood may allow for non-invasive patient subclassification and new perspectives in treatment regimes of IBD patients in the future.

Published

2013

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

Author

Louwen, R.P.L. (Rogier), Nieuwenhuis, E.E.S. (Edward), Marrewijk, L. (Leonie) van, Horst-Kreft, D. (Deborah), Ruiter, L.F. (Lilian) de, Heikema, A.P. (Astrid), Wamel, W.J.B. (Willem) van, Wagenaar, J.A. (Jaap), Endtz, H.P. (Hubert), Samsom, J.N. (Janneke), Baarlen, P. (Peter) van, Akhmanova, A.S. (Anna), Belkum, A.F. (Alex) van, Louwen, R.P.L. (Rogier), Nieuwenhuis, E.E.S. (Edward), Marrewijk, L. (Leonie) van, Horst-Kreft, D. (Deborah), Ruiter, L.F. (Lilian) de, Heikema, A.P. (Astrid), Wamel, W.J.B. (Willem) van, Wagenaar, J.A. (Jaap), Endtz, H.P. (Hubert), Samsom, J.N. (Janneke), Baarlen, P. (Peter) van, Akhmanova, A.S. (Anna), and Belkum, A.F. (Alex) van

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

15. Sialylation of campylobacter jejuni lipo-oligosaccharides: Impact on phagocytosis and cytokine production in mice

Author

Huizinga, R. (Ruth), Easton, A.S. (Alistair), Donachie, A.M. (Anne), Guthrie, J. (Jim), Rijs, W. (Wouter) van, Heikema, A.P. (Astrid), Boon, L. (Louis), Samsom, J.N. (Janneke), Jacobs, B.C. (Bart), Willison, H.J. (Hugh), Goodyear, C.S. (Carl), Huizinga, R. (Ruth), Easton, A.S. (Alistair), Donachie, A.M. (Anne), Guthrie, J. (Jim), Rijs, W. (Wouter) van, Heikema, A.P. (Astrid), Boon, L. (Louis), Samsom, J.N. (Janneke), Jacobs, B.C. (Bart), Willison, H.J. (Hugh), and Goodyear, C.S. (Carl)

Abstract

Background: Guillain-Barré syndrome (GBS) is a post-infectious polyradiculoneuropathy, frequently associated with antecedent Campylobacter jejuni (C. jejuni) infection. The presence of sialic acid on C. jejuni lipo-oligosaccharide (LOS) is considered a risk factor for development of GBS as it crucially determines the structural homology between LOS and gangliosides, explaining the induction of cross-reactive neurotoxic antibodies. Sialylated C. jejuni are recognised by TLR4 and sialoadhesin; however, the functional implications of these interactions in vivo are unknown. Methodology/Principal Findings: In this study we investigated the effects of bacterial sialylation on phagocytosis and cytokine secretion by mouse myeloid cells in vitro and in vivo. Using fluorescently labelled GM1a/GD1a ganglioside-mimicking C. jejuni strains and corresponding (Cst-II-mutant) control strains lacking sialic acid, we show that sialylated C. jejuni was more efficiently phagocytosed in vitro by BM-MΦ, but not by BM-DC. In addition, LOS sialylation increased the production of IL-10, IL-6 and IFN-β

Published

2012

16. Characterization of the specific interaction between sialoadhesin and sialylated Campylobacter jejuni lipooligosaccharides

Author

Heikema, A.P. (Astrid), Bergman, M.P. (Mathijs), Richards, H. (Hannah), Crocker, P.R. (Paul), Gilbert, M. (Michel), Samsom, J.N. (Janneke), Wamel, W.J.B. (Willem) van, Endtz, H.P. (Hubert), Belkum, A.F. (Alex) van, Heikema, A.P. (Astrid), Bergman, M.P. (Mathijs), Richards, H. (Hannah), Crocker, P.R. (Paul), Gilbert, M. (Michel), Samsom, J.N. (Janneke), Wamel, W.J.B. (Willem) van, Endtz, H.P. (Hubert), and Belkum, A.F. (Alex) van

Abstract

In Campylobacter jejuni-induced Guillain-Barré syndrome (GBS), molecular mimicry between C. jejuni lipooligosaccharide (LOS) and host gangliosides leads to the production of cross-reactive antibodies directed against the peripheral nerves of the host. Currently, the presence of surface exposed sialylated LOS in C. jejuni is the single known bacterial pathogenesis factor associated with the development of GBS. Using a unique, well-characterized strain collection, we demonstrate that GBS-associated C. jejuni strains bind preferentially to sialoadhesin (Sn, Siglec-1, or CD169), a sialic acid receptor found on a subset of macrophages. In addition, using a whole-cell enzyme-linked immunosorbent assay (ELISA), C. jejuni strains with sialylated

Published

2010

17. Local immune regulation of mucosal inflammation by tacrolimus

Author

Dieren, J.M. (Jolanda) van, Lambers, M.E.H. (Margaretha), Kuipers, E.J. (Ernst), Samsom, J.N. (Janneke), Woude, C.J. (Janneke) van der, Nieuwenhuis, E.E.S. (Edward), Dieren, J.M. (Jolanda) van, Lambers, M.E.H. (Margaretha), Kuipers, E.J. (Ernst), Samsom, J.N. (Janneke), Woude, C.J. (Janneke) van der, and Nieuwenhuis, E.E.S. (Edward)

Abstract

Purpose: Tacrolimus is a potent immunomodulator that is effective in the treatment of inflammatory bowel disease (IBD). However, potential toxicity and systemic effects with oral intake limit its use. Local tacrolimus treatment is effective in a subgroup

Published

2010

18. TLR4-mediated sensing of Campylobacter jejuni by dendritic cells is determined by sialylation

Author

Kuijf, M.L. (Mark), Samsom, J.N. (Janneke), Rijs, W. (Wouter) van, Bax, M. (Marieke), Huizinga, R. (Ruth), Heikema, A.P. (Astrid), Doorn, P.A. (Pieter) van, Belkum, A.F. (Alex) van, Kooyk, Y. (Yvette) van, Burgers, P.C. (Peter), Luider, T.M. (Theo), Endtz, H.P. (Hubert), Nieuwenhuis, E.E.S. (Edward), Jacobs, B.C. (Bart), Kuijf, M.L. (Mark), Samsom, J.N. (Janneke), Rijs, W. (Wouter) van, Bax, M. (Marieke), Huizinga, R. (Ruth), Heikema, A.P. (Astrid), Doorn, P.A. (Pieter) van, Belkum, A.F. (Alex) van, Kooyk, Y. (Yvette) van, Burgers, P.C. (Peter), Luider, T.M. (Theo), Endtz, H.P. (Hubert), Nieuwenhuis, E.E.S. (Edward), and Jacobs, B.C. (Bart)

Abstract

In Guillain-Barré syndrome (GBS), ganglioside mimicry of Campylobacter jejuni lipo-oligosaccharide (LOS) drives the production of cross-reactive Abs to peripheral nerve gangliosides. We determined whether sialic acid residues in C. jejuni LOS modulate dendritic cell (DC) activation and subsequent B cell proliferation as a possible mechanism for the aberrant humoral immune response in GBS. Highly purified sialylated LOS of C. jejuni isolates from three GBS patients induced human DC maturation and secretion of inflammatory cytokines that were inhibited by anti-TLR4 neutralizing Abs. The extent of TLR4 signaling and DC activation was greater with LOS of the wild type isolates than with nonsialylated LOS of the corresponding sialyltransferase gene knockout (cst-II mutant) strains, indicating that sialylation boosts the DC response to C. jejuni LOS. Supernatants of LOS-activated DCs induced B cell proliferation after cross-linking of surface Igs in the absence of T cells. Lower B cell proliferation indices were found with DC supernatants after DC stimulation with cst-II mutant or neuraminidase desialylated LOS. This study showed that sialylation of C. jejuni LOS enhances human DC activation and subsequent B cell proliferation, which may contribute to the development of cross-reactive anti-ganglioside Abs found in GBS patients following C. jejuni infection. Copyright

Published

2010