Your search keyword '"Büller, H.A. (Hans)"' showing total 12 results

1. Combined defects in epithelial and immunoregulatory factors exacerbate the pathogenesis of inflammation: Mucin 2-interleukin 10-deficient mice

Author

Sluis, M. (Maria) van der, Bouma, J. (Janneke), Vincent, A. (Audrey), Velcich, A. (Anna), Carraway, K.L. (Kermit), Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Goudoever, J.B. (Hans) van, Seuningen, I. (Isabelle) van, Renes, I.B. (Ingrid), Sluis, M. (Maria) van der, Bouma, J. (Janneke), Vincent, A. (Audrey), Velcich, A. (Anna), Carraway, K.L. (Kermit), Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Goudoever, J.B. (Hans) van, Seuningen, I. (Isabelle) van, and Renes, I.B. (Ingrid)

Abstract

Expression of the mucin MUC2, the structural component of the colonic mucus layer, is lowered in ulcerative colitis. Furthermore, interleukin (IL)-10 knockout (IL-10-/-) mice develop colitis and have reduced Muc2 levels. Our aim was to obtain insight into the role of Muc2 and IL-10 in epithelial protection. Muc2-IL-10 double-knockout (Muc2/IL-10DKO) mice were characterized and compared to Muc2 knockout (Muc2-/-), IL-10-/-and wild-type (WT) mice. Clinical symptoms, intestinal morphology and differences in epithelial-specific protein levels were analyzed. In addition, levels of the pro-inflammatory cytokines in colonic tissue and serum were determined. IL-10-/-mice were indistinguishable from WT mice throughout this experiment and showed no clinical or histological signs of colitis. Muc2/IL-10DKOand Muc2-/-mice showed significant growth retardation and clinical signs of colitis at 4 and 5 weeks, respectively. Muc2/IL-10DKOmice had a high mortality rate (50% survival/5 weeks) compared to the other types of mice (100% survival). Microscopic analysis of the colon of Muc2/IL-10DKOmice showed mucosal thickening, increased proliferation, superficial erosions and a diminished Muc4 expression. Furthermore, pro-inflammatory cytokines were significantly upregulated, both in tissue (mRNA) and systemically in Muc2/IL-10DKOmice. In conclusion, Muc2/IL-10DKOmice develop colitis, which is more severe in every aspect compared to Muc2-/-and IL-10-/-mice. These data indicate that (i) in case of Muc2 deficiency, the anti-inflammatory cytokine IL-10 can control epithelial damage, though to a limited extent and (ii) the mucus layer is most likely a key factor determining colitis.

Published

2008

2. Predictors of orphan drug approval in the European Union

Author

Heemstra, H.E. (Harald), Vrueh, R.L.A. (Remco) de, Weely, S. (Sonja) van, Büller, H.A. (Hans), Leufkens, H.G.M. (Hubert), Heemstra, H.E. (Harald), Vrueh, R.L.A. (Remco) de, Weely, S. (Sonja) van, Büller, H.A. (Hans), and Leufkens, H.G.M. (Hubert)

Abstract

Objective: To encourage the development of drugs for rare diseases, orphan drug legislation has been introduced in the USA (1983) and in the EU (2000). Recent literature discusses factors that may influence the development of new orphan medicinal products in the EU. This study aims to identify predictors for successful marketing authorisation of potential orphan drugs in the EU. Methods: A comparison between randomly selected authorised and a matched sample of not-yet-authorised orphan drug designations has been performed. Determinants in the study included characteristics of the indication, of the product and of the sponsor. Data were collected from the public domain only. Results: Orphan drug approval was strongly associated with previous experience of the sponsor in obtaining approval for another orphan drug (OR=17.3, 95% CI=5.6-53.1). Furthermore, existing synthetic entities compared to biotechnology products tended to have a higher likelihood of reaching approval status (OR=3.9, 95% CI=0.9-16.6). Conclusion: This study showed that experience of a company in developing orphan drugs is an important predictor for subsequent authorisation of other orphan drugs. The same applies for existing (synthetic) molecules, for which much knowledge is available. Further research should be directed towards studying the quality of the clinical development program of those designated orphan medicinal products not reaching approval status.

Published

2008

3. Alterations in epithelial and mesenchymal intestinal gene expression during doxorubicin-induced mucositis in mice

Author

Koning, B.A.E. (Barbara) de, Lindenbergh-Kortleve, D.J. (Dicky), Pieters, R. (Rob), Büller, H.A. (Hans), Renes, I.B. (Ingrid), Einerhand, A.W.C. (Sandra), Koning, B.A.E. (Barbara) de, Lindenbergh-Kortleve, D.J. (Dicky), Pieters, R. (Rob), Büller, H.A. (Hans), Renes, I.B. (Ingrid), and Einerhand, A.W.C. (Sandra)

Abstract

In the current study we aimed to gain insight into epithelial-mesenchymal cross-talk and progenitor compartment modulation during doxorubicin (DOX)-induced mucositis in mice. Intestinal segments were collected on various days after DOX treatment. DOX-induced damage at day 1-2 was characterized by increased epithelial proliferation and apoptosis and a decrease in the expression of epithelial differentiation markers. Concurrently, T-cell factor-4 (TCF4) levels increased and the epithelial differentiation enhancing factor, bone morphogenic protein-4 (BMP4), decreased. During severe damage (day 3), BMP4 levels were significantly increased, which inversely correlated with epithelial proliferation. At the same time, the expression of the epithelial differentiation markers was increasing again. At day 7, BMP4 levels were down-regulated, while the levels of the epithelial differentiation markers and TCF4 were normalized again. These data suggest that in response to DOX-induced damage, BMP4 and TCF4 are modulated in such a way that homeostasis of the progenitor compartment is partly preserved.

Published

2007

4. Cyclooxygenase activity is important for efficient replication of mouse hepatitis virus at an early stage of infection

Author

Raaben, M. (Matthijs), Einerhand, A.W.C. (Sandra), Taminiau, L.J.A. (Lucas), Houdt, M. (Michel) van, Bouma, J. (Janneke), Raatgeep, R.H. (Rolien), Büller, H.A. (Hans), Haan, C.A.M. (Cornelis) de, Rossen, J.W. (John), Raaben, M. (Matthijs), Einerhand, A.W.C. (Sandra), Taminiau, L.J.A. (Lucas), Houdt, M. (Michel) van, Bouma, J. (Janneke), Raatgeep, R.H. (Rolien), Büller, H.A. (Hans), Haan, C.A.M. (Cornelis) de, and Rossen, J.W. (John)

Abstract

Cyclooxygenases (COXs) play a significant role in many different viral infections with respect to replication and pathogenesis. Here we investigated the role of COXs in the mouse hepatitis coronavirus (MHV) infection cycle. Blocking COX activity by different inhibitors or by RNA interference affected MHV infection in different cells. The COX inhibitors reduced MHV infection at a post-binding step, but early in the replication cycle. Both viral RNA and viral protein synthesis were affected with subsequent loss of progeny virus production. Thus, COX activity appears to be required for efficient MHV replication, providing a potential target for anti-coronaviral therapy.

Published

2007

5. Adequate feeding and the usefulness of the respiratory quotient in critically ill children

Author

Hulst, J.M. (Jessie), Goudoever, J.B. (Hans) van, Zimmermann, L.J.I. (Luc), Hop, W.C.J. (Wim), Büller, H.A. (Hans), Tibboel, D. (Dick), Joosten, K.F.M. (Koen), Hulst, J.M. (Jessie), Goudoever, J.B. (Hans) van, Zimmermann, L.J.I. (Luc), Hop, W.C.J. (Wim), Büller, H.A. (Hans), Tibboel, D. (Dick), and Joosten, K.F.M. (Koen)

Abstract

Objective: We determined incidences of underfeeding and overfeeding in children who were admitted to a multidisciplinary tertiary pediatric intensive care and evaluated the usefulness of the respiratory quotient (RQ) obtained from indirect calorimetry to assess feeding adequacy. Methods: Children 18 y and younger who fulfilled the criteria for indirect calorimetry entered our prospective, observational study and were studied until day 14. Actual energy intake was recorded, compared with required energy intake (measured energy expenditure plus 10%), and classified as underfeeding (<90% of required), adequate feeding (90% to 110% of required), or

Published

2005

6. Splanchnic bed metabolism of glucose in preterm neonates

Author

Schoor, S.R.D. (Sophie) van der, Stoll, B., Wattimena, J.L.D. (Josias), Büller, H.A. (Hans), Tibboel, D. (Dick), Burrin, D.G. (Douglas), Goudoever, J.B. (Hans) van, Schoor, S.R.D. (Sophie) van der, Stoll, B., Wattimena, J.L.D. (Josias), Büller, H.A. (Hans), Tibboel, D. (Dick), Burrin, D.G. (Douglas), and Goudoever, J.B. (Hans) van

Abstract

BACKGROUND: Glucose is a major oxidative substrate for intestinal energy generation in neonatal animals; however, few data in preterm infants are available. Early administration of enteral nutrition, including glucose, may be an effective strategy to support intestinal adaptation to extrauterine life in preterm neonates. OBJECTIVE: The purpose of the present study was to quantify the first-pass uptake and oxidation of glucose by the splanchnic tissues (intestine and liver) in human neonates. DESIGN: Eight preterm infants [birth weight ( +/- SD): 1.19 +/- 0.22 kg, gestational age: 29 +/- 1 wk] were studied while they received 2 different enteral intakes (A: 40% enteral, 60% parenteral, total glucose intake = 7.5 +/- 0.5 mg. kg(-1). min(-1), and B: 100% enteral, total glucose intake = 7.8 +/- 0.4 mg. kg(-1). min(-1)). Splanchnic and whole-body glucose kinetics were measured by use of dual-tracer techniques. RESULTS: During both feeding periods, approximately one-third of dietary glucose intake was utilized during the first pass by the splanchnic tissues. More than three-quarters of this utilized glucose was oxidized in both periods (79 +/- 36% with A and 84 +/- 45% with B). Whole-body glucose oxidation was substantial under both circumstances: 72 +/- 5% and 77% +/- 6% of the glucose flux was oxidized during partial (A) and full (B) enteral feeding, respectively. CONCLUSIONS: Approximately one-third of dietary glucose is utilized during the first pass by the splanchnic tissues, irrespective of the dietary intake. Most of the utilized glucose is used for energy generation.

Published

2004

7. Lysine kinetics in preterm infants: the importance of enteral feeding

Author

Schoor, S.R.D. (Sophie) van der, Reeds, P.J., Stellaard, F. (Frans), Wattimena, J.L.D. (Josias), Sauer, P.J.J. (Pieter), Büller, H.A. (Hans), Goudoever, J.B. (Hans) van, Schoor, S.R.D. (Sophie) van der, Reeds, P.J., Stellaard, F. (Frans), Wattimena, J.L.D. (Josias), Sauer, P.J.J. (Pieter), Büller, H.A. (Hans), and Goudoever, J.B. (Hans) van

Abstract

INTRODUCTION: Lysine is the first limiting essential amino acid in the diet of newborns. First pass metabolism by the intestine of dietary lysine has a direct effect on systemic availability. We investigated whether first pass lysine metabolism in the intestine is high in preterm infants, particularly at a low enteral intake. PATIENTS AND METHODS: Six preterm infants (birth weight 0.9 (0.1) kg) were studied during two different periods: period A (n = 6): 40% of intake administered enterally, 60% parenterally; lysine intake 92 (6) micromol/(kg x h); and period B (n = 4): 100% enteral feeding; lysine intake 100 (3) micromol/(kg x h). Dual stable isotope tracer techniques were used to assess splanchnic and whole body lysine kinetics. RESULTS: Fractional first pass lysine uptake by the intestine was significantly higher during partial enteral feeding (period A 32 (10)% v period B 18 (7)%; p<0.05). Absolute uptake was not significantly different. Whole body lysine oxidation was significantly decreased during full enteral feeding (period A 44 (9) v period B 17 (3) micromol/(kg x h); p<0.05) so that whole body lysine balance was significantly higher during full enteral feeding (period A 52 (25) v period B 83 (3) micromol/(kg x h); p<0.05). CONCLUSIONS: Fractional first pass lysine uptake was much higher during partial enteral feeding. Preterm infants receiving full enteral feeding have lower whole body lysine oxidation, resulting in a higher net lysine balance, compared with preterm infants receiving partial enteral feeding. Hence parenterally administered lysine is not as effective as dietary lysine in promoting protein deposition in preterm infants.

Published

2004

8. Inhibition of cyclooxygenase activity reduces rotavirus infection at a postbinding step.

Author

Rossen, J.W. (John), Bouma, J. (Janneke), Raatgeep, R.H. (Rolien), Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Rossen, J.W. (John), Bouma, J. (Janneke), Raatgeep, R.H. (Rolien), Büller, H.A. (Hans), and Einerhand, A.W.C. (Sandra)

Abstract

Elevated levels of prostaglandins (PGs), products of cyclooxygenases (COXs), are found in the plasma and stool of rotavirus-infected children. We sought to determine the role of COXs, PGs, and the signal transduction pathways involved in rotavirus infection to elucidate possible new targets for antiviral therapy. Human intestinal Caco-2 cells were infected with human rotavirus Wa or simian rotavirus SA-11. COX-2 mRNA expression and secreted PGE2 levels were determined at different time points postinfection, and the effect of COX inhibitors on rotavirus infection was studied by an immunofluorescence assay (IFA). To reveal the signal transduction pathways involved, the effect of MEK, protein kinase A (PKA), p38 mitogen-activated protein kinase (MAPK), and NF-kappaB inhibitors on rotavirus infection was analyzed. In infected Caco-2 cells, increased COX-2 mRNA expression and secreted PGE2 levels were detected. Indomethacin (inhibiting both COX-1 and COX-2) and specific COX-1 and COX-2 inhibitors reduced rotavirus infection by 85 and 50%, respectively, as measured by an IFA. Indomethacin reduced virus infection at a postbinding step early in the infection cycle, inhibiting virus protein synthesis. Indomethacin did not seem to affect viral RNA synthesis. Inhibitors of MEK, PKA, p38 MAPK, and NF-kappaB decreased rotavirus infection by at least 40%. PGE2 counteracted the effect of the COX and PKA inhibitors but not of the MEK, p38 MAPK, and NF-kappaB inhibitors. Conclusively, COXs and PGE2 are important mediators of rotavirus infection at a postbinding step. The ERK1/2 pathway mediated by PKA is involved in COX induction by rotavirus infection. MAPK and NF-kappaB pathways are involved in rotavirus infection but in a PGE2-independent manner. This report offers new perspectives in the search for therapeutic agents in treatment of severe rotavirus-mediated diarrhea in children.

Published

2004

9. Rotavirus enterotoxin NSP4 binds to the extracellular matrix proteins laminin-beta3 and fibronectin.

Author

Boshuizen, J.A. (Jos), Rossen, J.W. (John), Sitaram, C.K., Kimenai, F.F.P., Simons-Oosterhuis, Y. (Ytje), Laffeber, C., Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Boshuizen, J.A. (Jos), Rossen, J.W. (John), Sitaram, C.K., Kimenai, F.F.P., Simons-Oosterhuis, Y. (Ytje), Laffeber, C., Büller, H.A. (Hans), and Einerhand, A.W.C. (Sandra)

Abstract

Rotavirus is the most important cause of viral gastroenteritis and dehydrating diarrhea in young children. Rotavirus nonstructural protein 4 (NSP4) is an enterotoxin that was identified as an important agent in symptomatic rotavirus infection. To identify cellular proteins that interact with NSP4, a two-hybrid technique with Saccharomyces cerevisiae was used. NSP4 cDNA, derived from the human rotavirus strain Wa, was cloned into the yeast shuttle vector pGBKT7. An intestinal cDNA library derived from Caco-2 cells cloned into the yeast shuttle vector pGAD10 was screened for proteins that interact with NSP4. Protein interactions were confirmed in vivo by coimmunoprecipitation and immunohistochemical colocalization. After two-hybrid library screening, we repeatedly isolated cDNAs encoding the extracellular matrix (ECM) protein laminin-beta3 (amino acids [aa] 274 to 878) and a cDNA encoding the ECM protein fibronectin (aa 1755 to 1884). Using deletion mutants of NSP4, we mapped the region of interaction with the ECM proteins between aa 87 and 145. Deletion analysis of laminin-beta3 indicated that the region comprising aa 726 to 875 of laminin-beta3 interacts with NSP4. Interaction of NSP4 with either laminin-beta3 or fibronectin was confirmed by coimmunoprecipitation. NSP4 was present in infected enterocytes and in the basement membrane (BM) of infected neonatal mice and colocalized with laminin-beta3, indicating a physiological interaction. In conclusion, two-hybrid screening with NSP4 yielded two potential target proteins, laminin-beta3 and fibronectin, interacting with the enterotoxin NSP4. The release of NSP4 from the basal side of infected epithelial cells and the subsequent binding to ECM proteins localized at the BM may signify a new mechanism by which rotavirus disease is established.

Published

2004

10. Changes in small intestinal homeostasis, morphology, and gene expression during rotavirus infection of infant mice

Author

Boshuizen, J.A. (Jos), Reimerink, J.H., Korteland-van Male, A.M. (Anita), Ham, V.J. van, Büller, H.A. (Hans), Dekker, J. (Jan), Einerhand, A.W.C. (Sandra), Koopmans D.V.M., M.P.G. (Marion), Boshuizen, J.A. (Jos), Reimerink, J.H., Korteland-van Male, A.M. (Anita), Ham, V.J. van, Büller, H.A. (Hans), Dekker, J. (Jan), Einerhand, A.W.C. (Sandra), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Rotavirus is the most important cause of infantile gastroenteritis. Since in vivo mucosal responses to a rotavirus infection thus far have not been extensively studied, we related viral replication in the murine small intestine to alterations in mucosal structure, epithelial cell homeostasis, cellular kinetics, and differentiation. Seven-day-old suckling BALB/c mice were inoculated with 2 x 10(4) focus-forming units of murine rotavirus and were compared to mock-infected controls. Diarrheal illness and viral shedding were recorded, and small intestinal tissue was evaluated for rotavirus (NSP4 and structural proteins)- and enterocyte-specific (lactase, SGLT1, and L-FABP) mRNA and protein expression. Morphology, apoptosis, proliferation, and migration were evaluated (immuno)histochemically. Diarrhea was observed from days 1 to 5 postinfection, and viral shedding was observed from days 1 to 10. Two peaks of rotavirus replication were observed at 1 and 4 days postinfection. Histological changes were characterized by the accumulation of vacuolated enterocytes. Strikingly, the number of vacuolated cells exceeded the number of cells in which viral replication was detectable. Apoptosis and proliferation were increased from days 1 to 7, resulting in villous atrophy. Epithelial cell turnover was significantly higher (<4 days) than that observed in controls (7 days). Since epithelial renewal occurred within 4 days, the second peak of viral replication was most likely caused by infection of newly synthesized cells. Expression of enterocyte-specific genes was downregulated in infected cells at mRNA and protein levels starting as early as 6 h after infection. In conclusion, we show for the first time that rotavirus infection induces apoptosis in vivo, an increase in epithelial cell turnover, and a shutoff of gene expression in enterocytes showing viral replication. The shutoff of enterocyte-specific gene expression, together with the loss of mature enterocytes through apoptosis an

Published

2003

11. Specific responses in rat small intestinal epithelial mRNA expression and protein levels during chemotherapeutic damage and regeneration

Author

Verburg, M. (Melissa), Renes, I.B. (Ingrid), Nispen, D.J. van, Ferdinandusse, S., Jorritsma, M., Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Dekker, J. (Jan), Verburg, M. (Melissa), Renes, I.B. (Ingrid), Nispen, D.J. van, Ferdinandusse, S., Jorritsma, M., Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), and Dekker, J. (Jan)

Abstract

The rapidly dividing small intestinal epithelium is very sensitive to the cytostatic drug methotrexate. We investigated the regulation of epithelial gene expression in rat jejunum during methotrexate-induced damage and regeneration. Ten differentiation markers were localized on tissue sections and quantified at mRNA and protein levels relative to control levels. We analyzed correlations in temporal expression patterns between markers. mRNA expression of enterocyte and goblet cell markers decreased significantly during damage for a specific period. Of these, sucrase-isomaltase (-62%) and CPS (-82%) were correlated. Correlations were also found between lactase (-76%) and SGLT1 (-77%) and between I-FABP (-52%) and L-FABP (-45%). Decreases in GLUT5 (-53%), MUC2 (-43%), and TFF3 (-54%) mRNAs occurred independently of any of the other markers. In contrast, lysozyme mRNA present in Paneth cells increased (+76%). At the protein level, qualitative and quantitative changes were in agreement with mRNA expression, except for Muc2 (+115%) and TFF3 (+81%), which increased significantly during damage, following independent patterns. During regeneration, expression of each marker returned to control levels. The enhanced expression of cytoprotective molecules (Muc2, TFF3, lysozyme) during damage represents maintenance of goblet cell and Paneth cell functions, most likely to protect the epithelium. Decreased expression of enterocyte-specific markers represents decreased enterocyte function, of which fatty acid transporters were least affected.

Published

2002

12. Selective sparing of goblet cells and paneth cells in the intestine of methotrexate-treated rats

Author

Verburg, M. (Melissa), Renes, I.B. (Ingrid), Meijer, H.P., Taminiau, J.A., Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), Dekker, J. (Jan), Verburg, M. (Melissa), Renes, I.B. (Ingrid), Meijer, H.P., Taminiau, J.A., Büller, H.A. (Hans), Einerhand, A.W.C. (Sandra), and Dekker, J. (Jan)

Abstract

Proliferation, differentiation, and cell death were studied in small intestinal and colonic epithelia of rats after treatment with methotrexate. Days 1-2 after treatment were characterized by decreased proliferation, increased apoptosis, and decreased numbers and depths of small intestinal crypts in a proximal-to-distal decreasing gradient along the small intestine. The remaining crypt epithelium appeared flattened, except for Paneth cells, in which lysozyme protein and mRNA expression was increased. Regeneration through increased proliferation during days 3-4 coincided with villus atrophy, showing decreased numbers of villus enterocytes and decreased expression of the enterocyte-specific genes sucrase-isomaltase and carbamoyl phosphate synthase I. Remarkably, goblet cells were spared at villus tips and remained functional, displaying Muc2 and trefoil factor 3 expression. On days 8-10, all parameters had returned to normal in the whole small intestine. No methotrexate-induced changes were seen in epithelial morphology, proliferation, apoptosis, Muc2, and TFF3 immunostaining in the colon. The observed small intestinal sparing of Paneth cells and goblet cells following exposure to methotrexate is likely to contribute to epithelial defense during increased vulnerability of the intestinal epithelium.

Published

2000