Search

Your search keyword '"Lenaerts K"' showing total 212 results
Start Over Author "Lenaerts K"
212 results on '"Lenaerts K"'

1. Polyethylene glycol versus dual sugar assay for gastrointestinal permeability analysis: is it time to choose?

Author

van Wijck K, Bessems BAFM, van Eijk HM, Buurman WA, Dejong CH, and Lenaerts K

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Kim van Wijck,1,2 Babs AFM Bessems,2 Hans MH van Eijk,2 Wim A Buurman,2 Cornelis HC Dejong,1,2 Kaatje Lenaerts1,21Top Institute Food and Nutrition, Wageningen, The Netherlands; 2Department of Surgery, NUTRIM School for Nutrition, Toxicology and Metabolism, Maastricht University Medical Center, Maastricht, NetherlandsBackground: Increased intestinal permeability is an important measure of disease activity and prognosis. Currently, many permeability tests are available and no consensus has been reached as to which test is most suitable. The aim of this study was to compare urinary probe excretion and accuracy of a polyethylene glycol (PEG) assay and dual sugar assay in a double-blinded crossover study to evaluate probe excretion and the accuracy of both tests.Methods: Gastrointestinal permeability was measured in nine volunteers using PEG 400, PEG 1500, and PEG 3350 or lactulose-rhamnose. On 4 separate days, permeability was analyzed after oral intake of placebo or indomethacin, a drug known to increase intestinal permeability. Plasma intestinal fatty acid binding protein and calprotectin levels were determined to verify compromised intestinal integrity after indomethacin consumption. Urinary samples were collected at baseline, hourly up to 5 hours after probe intake, and between 5 and 24 hours. Urinary excretion of PEG and sugars was determined using high-pressure liquid chromatography-evaporative light scattering detection and liquid chromatography-mass spectrometry, respectively.Results: Intake of indomethacin increased plasma intestinal fatty acid-binding protein and calprotectin levels, reflecting loss of intestinal integrity and inflammation. In this state of indomethacin-induced gastrointestinal compromise, urinary excretion of the three PEG probes and lactulose increased compared with placebo. Urinary PEG 400 excretion, the PEG 3350/PEG 400 ratio, and the lactulose/rhamnose ratio could accurately detect indomethacin-induced increases in gastrointestinal permeability, especially within 2 hours of probe intake.Conclusion: Hourly urinary excretion and diagnostic accuracy of PEG and sugar probes show high concordance for detection of indomethacin-induced increases in gastrointestinal permeability. This comparative study improves our knowledge of permeability analysis in man by providing a clear overview of both tests and demonstrates equivalent performance in the current setting.Keywords: gastrointestinal permeability, polyethylene glycol, dual sugar

Published
2012

5. Unione Europea: adattarsi ai cambiamenti climatici

Author

Tagliapietra, Simone, Wolff, G., Lenaerts, K., s. tagliapietra, Tagliapietra, Simone, Wolff, G., Lenaerts, K., and s. tagliapietra

Abstract

Adattamento al cambiamento climatico.

Published
2022

6. Potential pathways for the future development and sustainability of the InGRID research infrastructure, Deliverable 7.9

Author

Lenaerts, K., Ramioul, M., Nelson, K., Steinmetz, S., Esteve, A., G��bos, A., Gy��rgy T��th, I., Besamusca, J., Articus, C., M��nnich, R., and Shlomo, N.

Abstract

This document lays out some potential pathways for the future development and sustainability of the InGRID research infrastructure. It is a summary and compilation of key documents prepared under the InGRID-2 project and its work plan, including three strategic notes on data, methods and policy.

Published
2022
Full Text
View/download PDF

7. Clinical management of chronic mesenteric ischemia

Author

Dijk, L.J.D. van, Noord, D. van, Vries, A.C. de, Kolkman, J.J., Geelkerken, R.H., Verhagen, H.J.M., Moelker, A., Bruno, M.J., Balm, R., Borst, G.J. de, Blauw, J.T., Bakker, O.J., Buscher, H.C.J.L., Fioole, B., Hamming, J.F., Harki, J., Heuvel, D.A.F. van den, Hattum, E.S. van, Hinnen, J.W., Laan, M.J. van der, Lenaerts, K., Peppelenbosch, M.P., Petersen, A.S. van, Rijnja, P., Schaar, P.J. van der, Terlouw, L.G., Vries, J.P.P.M. de, Vroegindeweij, D., Dutch Mesenteric Ischemia Study, Gastroenterology & Hepatology, Radiology & Nuclear Medicine, and Surgery

Subjects
Atherosclerotic stenosis, medicine.medical_specialty, Endovascular revascularization, Clinical Decision-Making, UT-Hybrid-D, chemical and pharmacologic phenomena, Review Article, DIAGNOSIS, complex mixtures, STENOSIS, 03 medical and health sciences, 0302 clinical medicine, medicine, Prevalence, Humans, University medical, Erasmus+, Chronic mesenteric ischemia, median arcuate ligament syndrome, ARTERY, Abdominal discomfort, GASTRIC EXERCISE TONOMETRY, endovascular therapy, business.industry, General surgery, MORTALITY, Gastroenterology, Disease Management, medicine.disease, humanities, Treatment Outcome, Oncology, Mesenteric ischemia, 030220 oncology & carcinogenesis, Mesenteric Ischemia, Chronic Disease, 030211 gastroenterology & hepatology, Blood supply, REVASCULARIZATION, Symptom Assessment, atherosclerosis, business, Vascular Surgical Procedures, VISIBLE-LIGHT SPECTROSCOPY, computed tomography angiography
Abstract

This: This Dutch Mesenteric Ischemia Study group consists of: Ron Balm, Academic Medical Center, Amsterdam Gert Jan de Borst, University Medical Center Utrecht, Utrecht Juliette T Blauw, Medisch Spectrum Twente, Enschede Marco J Bruno, Erasmus MC University Medical Center, Rotterdam Olaf J Bakker, St Antonius Hospital, Nieuwegein Louisa JD van Dijk, Erasmus MC University Medical Center, Rotterdam Hessel CJL Buscher, Gelre Hospitals, Apeldoorn Bram Fioole, Maasstad Hospital, Rotterdam Robert H Geelkerken, Medisch Spectrum Twente, Enschede Jaap F Hamming, Leiden University Medical Center, Leiden Jihan Harki, Erasmus MC University Medical Center, Rotterdam Daniel AF van den Heuvel, St Antonius Hospital, Nieuwegein Eline S van Hattum, University Medical Center Utrecht, Utrecht Jan Willem Hinnen, Jeroen Bosch Hospital, ‘s-Hertogenbosch Jeroen J Kolkman, Medisch Spectrum Twente, Enschede Maarten J van der Laan, University Medical Center Groningen, Groningen Kaatje Lenaerts, Maastricht University Medical Center, Maastricht Adriaan Moelker, Erasmus MC University Medical Center, Rotterdam Desirée van Noord, Franciscus Gasthuis & Vlietland, Rotterdam Maikel P Peppelenbosch, Erasmus MC University Medical Center, Rotterdam André S van Petersen, Bernhoven Hospital, Uden Pepijn Rijnja, Medisch Spectrum Twente, Enschede Peter J van der Schaar, St Antonius Hospital, Nieuwegein Luke G Terlouw, Erasmus MC University Medical Center, Rotterdam Hence JM Verhagen, Erasmus MC University Medical Center, Rotterdam Jean Paul PM de Vries, University Medical Center Groningen, Groningen Dammis Vroegindeweij, Maasstad Hospital, Rotterdam review provides an overview on the clinical management of chronic mesenteric ischemia (CMI). CMI is defined as insufficient blood supply to the gastrointestinal tract, most often caused by atherosclerotic stenosis of one or more mesenteric arteries. Patients classically present with postprandial abdominal pain and weight loss. However, patients may present with, atypically, symptoms such as abdominal discomfort, nausea, vomiting, diarrhea or constipation. Early consideration and diagnosis of CMI is important to timely treat, to improve quality of life and to prevent acute-on-chronic mesenteric ischemia. The diagnosis of CMI is based on the triad of clinical symptoms, radiological evaluation of the mesenteric vasculature and if available, functional assessment of mucosal ischemia. Multidisciplinary consensus on the diagnosis of CMI is of paramount importance to adequately select patients for treatment. Patients with a consensus diagnosis of single-vessel or multi-vessel atherosclerotic CMI are preferably treated with endovascular revascularization.

Published
2019

9. Chorioamnionitis induces hepatic inflammation and time-dependent changes of the enterohepatic circulation in the ovine fetus

Author

Heymans, C., den Dulk, M., Lenaerts, K., Heij, L.R., de Lange, I.H., Hadfoune, M., van Heugten, C., Kramer, B.W., Jobe, A.H., Saito, M., Kemp, M.W., Wolfs, T.G.A.M., van Gemert, W.G., Heymans, C., den Dulk, M., Lenaerts, K., Heij, L.R., de Lange, I.H., Hadfoune, M., van Heugten, C., Kramer, B.W., Jobe, A.H., Saito, M., Kemp, M.W., Wolfs, T.G.A.M., and van Gemert, W.G.

Abstract

Chorioamnionitis, inflammation of fetal membranes, is an important cause of preterm birth and a risk factor for the development of adverse neonatal outcomes including sepsis and intestinal pathologies. Intestinal bile acids (BAs) accumulation and hepatic cytokine production are involved in adverse intestinal outcomes. These findings triggered us to study the liver and enterohepatic circulation (EHC) following intra-amniotic (IA) lipopolysaccharide (LPS) exposure. An ovine chorioamnionitis model was used in which circulatory cytokines and outcomes of the liver and EHC of preterm lambs were longitudinally assessed following IA administration of 10 mg LPS at 5, 12 or 24h or 2, 4, 8 or 15d before preterm birth. Hepatic inflammation was observed, characterized by increased hepatic cytokine mRNA levels (5h – 2d post IA LPS exposure) and increased erythropoietic clusters (at 8 and 15 days post IA LPS exposure). Besides, 12h after IA LPS exposure, plasma BA levels were increased, whereas gene expression levels of several hepatic BA transporters were decreased. Initial EHC alterations normalized over time. Concluding, IA LPS exposure induces significant time-dependent changes in the fetal liver and EHC. These chorioamnionitis induced changes have potential postnatal consequences and the duration of IA LPS exposure might be essential herein.

Published
2021

14. Prophylactic Intra-Uterine β-Cyclodextrin Administration during Intra-Uterine Ureaplasma parvum Infection Partly Prevents Liver Inflammation without Interfering with the Enterohepatic Circulation of the Fetal Sheep

Author

Heymans, C., Heij, L.R., Lenaerts, K., den Dulk, M., Hadfoune, M., van Heugten, C., Spiller, O.B., Beeton, M.L., Stock, S.J., Jobe, A.H., Payne, M.S., Kemp, M.W., Kramer, B.W., Plat, J., van Gemert, W.G., Wolfs, T.G.A.M., Heymans, C., Heij, L.R., Lenaerts, K., den Dulk, M., Hadfoune, M., van Heugten, C., Spiller, O.B., Beeton, M.L., Stock, S.J., Jobe, A.H., Payne, M.S., Kemp, M.W., Kramer, B.W., Plat, J., van Gemert, W.G., and Wolfs, T.G.A.M.

Abstract

Chorioamnionitis can lead to inflammation and injury of the liver and gut, thereby predisposing patients to adverse outcomes such as necrotizing enterocolitis (NEC). In addition, intestinal bile acids (BAs) accumulation is causally linked to NEC development. Plant sterols are a promising intervention to prevent NEC development, considering their anti-inflammatory properties in the liver. Therefore, we investigated whether an intra-amniotic (IA) Ureaplasma parvum (UP) infection affected the liver and enterohepatic circulation (EHC) and evaluated whether an IA administered plant sterol mixture dissolved in β-cyclodextrin exerted prophylactic effects. An ovine chorioamnionitis model was used in which liver inflammation and the EHC were assessed following IA UP exposure in the presence or absence of IA prophylactic plant sterols (a mixture of β-sitosterol and campesterol dissolved in β-cyclodextrin (carrier)) or carrier alone. IA UP exposure caused an inflammatory reaction in the liver, histologically seen as clustered and conflated hepatic erythropoiesis in the parenchyma, which was partially prevented by IA administration of sterol + β-cyclodextrin, or β-cyclodextrin alone. In addition, IA administration of β-cyclodextrin prior to UP caused changes in the expression of several hepatic BAs transporters, without causing alterations in other aspects of the EHC. Thereby, the addition of plant sterols to the carrier β-cyclodextrin did not have additional effects.

Published
2020

15. Corrigendum: Chronic Intra-Uterine Ureaplasma parvum infection induces injury of the enteric Nervous System in Ovine Fetuses

Author

Heymans, C., de Lange, I. H., Hütten, M.C., Lenaerts, K., de Ruijter, N.J.E., Kessels, L.C.G.A., Rademakers, G., Melotte, V., Boesmans, W., Saito, M., Usuda, H., Stock, S.J., Spiller, O.B., Beeton, M.L., Payne, M.S., Kramer, B.W., Newnham, J.P., Jobe, A.H., Kemp, M.W., van Gemert, W.G., Wolfs, T.G.A.M., Heymans, C., de Lange, I. H., Hütten, M.C., Lenaerts, K., de Ruijter, N.J.E., Kessels, L.C.G.A., Rademakers, G., Melotte, V., Boesmans, W., Saito, M., Usuda, H., Stock, S.J., Spiller, O.B., Beeton, M.L., Payne, M.S., Kramer, B.W., Newnham, J.P., Jobe, A.H., Kemp, M.W., van Gemert, W.G., and Wolfs, T.G.A.M.

Abstract

Michael L. Beeton was not included as an author in the published article. The corrected Author Contributions Statement appears below.

Published
2020

18. Validation of a score chart to predict the risk of chronic mesenteric ischemia and development of an updated score chart

Author

Dijk, L.J.D. van, Noord, D. van, Geelkerken, R.H., Harki, J., Berendsen, S.A., Vries, A.C. de, Moelker, A., Vergouwe, Y., Verhagen, H.J.M., Kolkman, J.J., Bruno, M.J., Balm, R., Borst, G.J. de, Blauw, J.T., Bakker, O.J., Buscher, H.C.J.L., Fioole, B., Hamming, J.F., Heuvel, D.A.F. van den, Hattum, E.S. van, Hinnen, J.W., Laan, M.J. van der, Lenaerts, K., Peppelenbosch, M.P., Petersen, A.S. van, Rijnja, P., Schaar, P.J. van der, Terlouw, L.G., Vries, J.P.P.M. de, Vroegindeweij, D., Dutch Mesenteric Ischemia Study Gr, Gastroenterology & Hepatology, Radiology & Nuclear Medicine, Public Health, Surgery, ​Robotics and image-guided minimally-invasive surgery (ROBOTICS), RS: NUTRIM - R2 - Liver and digestive health, and Multi-Modality Medical Imaging

Subjects
Male, Vasodilator Agents, Constriction, Pathologic, DUPLEX ULTRASOUND, Cohort Studies, 0302 clinical medicine, Symptom relief, Celiac artery, celiac artery, Prospective Studies, Prospective cohort study, median arcuate ligament syndrome, chronic mesenteric ischemia, Aged, 80 and over, GASTRIC EXERCISE TONOMETRY, Gastroenterology, Angiography, superior mesenteric artery, Middle Aged, Mesenteric Arteries, prediction model, Oncology, Cardiovascular Diseases, 030220 oncology & carcinogenesis, Female, 030211 gastroenterology & hepatology, Median arcuate ligament syndrome, VISIBLE-LIGHT SPECTROSCOPY, CT, Adult, medicine.medical_specialty, computed tomography magnetic resonance angiography, chemical and pharmacologic phenomena, DIAGNOSIS, Risk Assessment, complex mixtures, CHRONIC GASTROINTESTINAL ISCHEMIA, 03 medical and health sciences, Sex Factors, Chart, Mesenteric Artery, Superior, Internal medicine, medicine.artery, Weight Loss, medicine, MANAGEMENT, Humans, Aged, business.industry, Original Articles, medicine.disease, Stenosis, Chronic mesenteric ischemia, Mesenteric Ischemia, Chronic Disease, atherosclerosis, Intermediate risk, business
Abstract

Background and objective: The objective of this article is to externally validate and update a recently published score chart for chronic mesenteric ischemia (CMI). Methods: A multicenter prospective cohort analysis was conducted of 666 CMI-suspected patients referred to two Dutch specialized CMI centers. Multidisciplinary consultation resulted in expert-based consensus diagnosis after which CMI consensus patients were treated. A definitive diagnosis of CMI was established if successful treatment resulted in durable symptom relief. The absolute CMI risk was calculated and discriminative ability of the original chart was assessed by the c-statistic in the validation cohort. Thereafter the original score chart was updated based on the performance in the combined original and validation cohort with inclusion of celiac artery (CA) stenosis cause. Results: In 8% of low-risk patients, 39% of intermediate-risk patients and 94% of high-risk patients of the validation cohort, CMI was diagnosed. Discriminative ability of the original model was acceptable (c-statistic 0.79). The total score of the updated chart ranged from 0 to 28 points (low risk 19% absolute CMI risk, intermediate risk 45%, and high risk 92%). The discriminative ability of the updated chart was slightly better (c-statistic 0.80). Conclusion: The CMI prediction model performs and discriminates well in the validation cohort. The updated score chart has excellent discriminative ability and is useful in clinical decision making.

Published
2019

19. Validation of a score chart to predict the risk of chronic mesenteric ischemia and development of an updated score chart

Author

van Dijk, Louisa, Leemreis - van Noord, Désirée, Geelkerken, RH, Harki, Jihan, Berendsen, Sophie, de Vries, Annemarie, Moelker, Adriaan, Vergouwe, Yvonne, Verhagen, Hence, Kolkman, JJ, Bruno, Marco, Balm, R, de Borst, GJ, Blauw, JTM, Bakker, OJ, Buscher, H, Fioole, B, Hamming, JF, van den Heuvel, DAF, van Hattum, ES, Hinnen, JW, Van der Laan, MJ, Lenaerts, K, Peppelenbosch, Maikel, van Petersen, AS, Rijnja, P, Van der Schaar, PJ, Terlouw, Luke, Vries, JPPM, Vroegindeweij, D, van Dijk, Louisa, Leemreis - van Noord, Désirée, Geelkerken, RH, Harki, Jihan, Berendsen, Sophie, de Vries, Annemarie, Moelker, Adriaan, Vergouwe, Yvonne, Verhagen, Hence, Kolkman, JJ, Bruno, Marco, Balm, R, de Borst, GJ, Blauw, JTM, Bakker, OJ, Buscher, H, Fioole, B, Hamming, JF, van den Heuvel, DAF, van Hattum, ES, Hinnen, JW, Van der Laan, MJ, Lenaerts, K, Peppelenbosch, Maikel, van Petersen, AS, Rijnja, P, Van der Schaar, PJ, Terlouw, Luke, Vries, JPPM, and Vroegindeweij, D

Published
2019

20. Web-based methodology for monitoring new jobs. Updating the occupations observatory

Author

Beblavý, M., Welter-Médée, C., Lenaerts, K., Akgüç, M., Kilhoffer, Z., and Silva, A.

Abstract

The identification of new and emerging occupations has proven to be a challenging task, in which real-time information on labour market developments is key. At present, the most commonly used data sources do not provide up-to-date information, are narrow in scope or limited in size. In this light, online job portals have been suggested as an interesting data source for real-time labour market analysis. This report aims to contribute to the identification of new and emerging occupations by presenting an updated version of the methodology underpinning the Occupations Observatory developed by Beblavý et al. (2016). We use data extracted from online job boards using web scraping techniques, compare newly identified occupations with existing occupational classifications, and present examples of the tasks and skills required. With this update, we set out to further fine-tune the data collection, processing and analysis steps, but also to make the methodology and outputs more user-friendly, while providing more information at the same time. The proposed revised methodology consists of seven stages, and has been tested for the case of Ireland.

Published
2018

23. Enteroendocrine L Cells Sense LPS after Gut Barrier Injury to Enhance GLP-1 Secretion

Author

Lebrun, L.J., Lenaerts, K., Kiers, D., Barros, J.P. Pais de, Guern, N. Le, Plesnik, J., Thomas, C., Bourgeois, T., Dejong, C.H., Kox, M., Hundscheid, I.H.R., Khan, N.A., Mandard, S., Deckert, V., Pickkers, P., Drucker, D.J., Lagrost, L., Grober, J., Lebrun, L.J., Lenaerts, K., Kiers, D., Barros, J.P. Pais de, Guern, N. Le, Plesnik, J., Thomas, C., Bourgeois, T., Dejong, C.H., Kox, M., Hundscheid, I.H.R., Khan, N.A., Mandard, S., Deckert, V., Pickkers, P., Drucker, D.J., Lagrost, L., and Grober, J.

Abstract

Contains fulltext : 182548.pdf (publisher's version ) (Open Access), Glucagon-like peptide 1 (GLP-1) is a hormone released from enteroendocrine L cells. Although first described as a glucoregulatory incretin hormone, GLP-1 also suppresses inflammation and promotes mucosal integrity. Here, we demonstrate that plasma GLP-1 levels are rapidly increased by lipopolysaccharide (LPS) administration in mice via a Toll-like receptor 4 (TLR4)-dependent mechanism. Experimental manipulation of gut barrier integrity after dextran sodium sulfate treatment, or via ischemia/reperfusion experiments in mice, triggered a rapid rise in circulating GLP-1. This phenomenon was detected prior to measurable changes in inflammatory status and plasma cytokine and LPS levels. In human subjects, LPS administration also induced GLP-1 secretion. Furthermore, GLP-1 levels were rapidly increased following the induction of ischemia in the human intestine. These findings expand traditional concepts of enteroendocrine L cell biology to encompass the sensing of inflammatory stimuli and compromised mucosal integrity, linking glucagon-like peptide secretion to gut inflammation.

Published
2017

24. Hepatic Uptake of Rectally Administered Butyrate Prevents an Increase in Systemic Butyrate Concentrations in Humans

Author

van der Beek, C.M., Bloemen, J.G., van den Broek, M.A., Lenaerts, K., Venema, K., Buurman, W.A., Dejong, C.H., RS: NUTRIM - R2 - Gut-liver homeostasis, RS: NUTRIM - R1 - Metabolic Syndrome, RS: NUTRIM - HB/BW section A, Surgery, and Humane Biologie

Abstract

BACKGROUND: Short-chain fatty acids (SCFAs), fermentation products of undigested fibers, are considered beneficial for colonic health. High plasma concentrations are potentially harmful; therefore, information about systemic SCFA clearance is needed before therapeutic use of prebiotics or colonic SCFA administration. OBJECTIVE: The aim of this study was to investigate the effect of rectal butyrate administration on SCFA interorgan exchange. METHODS: Twelve patients (7 men; age: 66.4 +/- 2.0 y; BMI 24.5 +/- 1.4 kg/m(2)) undergoing upper abdominal surgery participated in this randomized placebo-controlled trial. During surgery, 1 group received a butyrate enema (100 mmol sodium butyrate/L; 60 mL; n = 7), and the other group a placebo (140 mmol 0.9% NaCl/L; 60 mL; n = 5). Before and 5, 15, and 30 min after administration, blood samples were taken from the radial artery, hepatic vein, and portal vein. Plasma SCFA concentrations were analyzed, and fluxes from portal-drained viscera, liver, and splanchnic area were calculated and used for the calculation of the incremental area under the curve (iAUC) over a 30-min period. RESULTS: Rectal butyrate administration led to higher portal butyrate concentrations at 5 min compared with placebo (92.2 +/- 27.0 mumol/L vs. 14.3 +/- 3.4 mumol/L, respectively; P < 0.01). In the butyrate-treated group, iAUCs of gut release (282.8 +/- 133.8 mumol/kg BW . 0.5 h) and liver uptake (-293.7 +/- 136.0 mumol/kg BW . 0.5 h) of butyrate were greater than in the placebo group [-16.6 +/- 13.4 mumol/kg BW . 0.5 h (gut release) and 16.0 +/- 13.8 mumol/kg BW . 0.5 h (liver uptake); P = 0.01 and P < 0.05, respectively]. As a result, splanchnic butyrate release did not differ between groups. CONCLUSION: After colonic butyrate administration, splanchnic butyrate release was prevented in patients undergoing upper abdominal surgery. These observations imply that therapeutic colonic SCFA administration at this dose is safe. The trial was registered at clinicaltrials.gov as NCT02271802.

Published
2015

25. Disturbed Intestinal Integrity in Patients With COPD: Effects of Activities of Daily Living

Author

Rutten, E.P.A., Lenaerts, K., Buurman, W.A., Wouters, E.F.M., Pulmonologie, Surgery, RS: CAPHRI School for Public Health and Primary Care, RS: NUTRIM - R3 - Chronic inflammatory disease and wasting, RS: NUTRIM - R2 - Gut-liver homeostasis, and RS: CAPHRI - Asthma and COPD

Subjects
respiratory tract diseases
Abstract

BACKGROUND: COPD is accepted to be a multicomponent disease with various comorbidities. The contribution of the gastrointestinal tract to the systemic manifestation of COPD has never been investigated. This metabolically active organ may experience recurring local oxygen deficits during daily life, leading to disturbed intestinal integrity in COPD patients. METHOD: 18 patients with moderate COPD (mean FEV1: 55+/-3%predicted) and 14 matched healthy controls were tested on two occasions, a baseline measurement at rest and, at another day, during the performance of activities of daily living (ADLs). To assess enterocyte damage, plasma intestinal fatty acid binding protein (IFABP) levels were determined, whereas urinary excretion of orally ingested sugar probes was measured using liquid chromatography and mass spectrometry to assess gastrointestinal permeability. RESULTS: Plasma IFABP concentrations were not different between COPD patients and healthy controls at rest. In contrast, 0-3h urinary lactulose/rhamnose and sucralose/erythritol ratios and 5-24h urinary sucralose/erythritol ratios were significantly higher in COPD patients compared to controls, indicating increased permeability of the small intestine and colon. Furthermore, the performance of ADLs led to significantly increased plasma IFABP concentrations in COPD patients but not in control subjects. In line, the intestinal permeability difference between COPD patients and controls was intensified. CONCLUSION: Besides an altered intestinal permeability in COPD patients at rest, performing ADLs led to enterocyte damage in addition to intestinal hyperpermeability in COPD patients but not in controls, indicating functional alteration in the gastrointestinal tract. Hence, intestinal compromise should be considered as a new component of the multisystem disorder COPD. CLINICAL TRIAL REGISTRATION: ISRCTN33686980.

Published
2014

26. Human splanchnic amino-acid metabolism

Author

Neis, Evelien P. J. G., primary, Sabrkhany, S., additional, Hundscheid, I., additional, Schellekens, D., additional, Lenaerts, K., additional, Olde Damink, S. W., additional, Blaak, E. E., additional, Dejong, C. H. C., additional, and Rensen, Sander S., additional

Published
2016
Full Text
View/download PDF

27. OR05: Human Intestinal Ischemia Reperfusion - Tales from the Crypts

Author

Hundscheid, I.H., primary, Eijssen, L., additional, Soons, Z., additional, Schellekens, D.H., additional, Derikx, J.P., additional, Grootjans, J., additional, van derVries, G., additional, Swertz, M.A., additional, Olde Damink, S.W., additional, Dejong, C.H., additional, and Lenaerts, K., additional

Published
2016
Full Text
View/download PDF

29. The average consumer's degree of attention in trade mark cases -- in Landmark Cases of EU Consumer Law - In honour of Jules Stuyck

Author

Weatherill, Stephen, Puttemans, Andrée, Reich, Norbert, VANNEROM, J., Van Dyck, T., Lenaerts, K., Steennot, Reinhard, Looijestijn-Clearie, A., De Waele, H., Van Schoubroeck, C., Vanistendael, F., Gormley, L.W., Cousy, H., Howells, Geraint, Borghetti, J.-S., Henning-Bodewig, F., Straetmans, G., Colaert, V., Laffineur, J., Van Huffel, M., Keirsbilck, B., Fornage, A.-Ch., Sibony, A.-L., Twigg-Flesner, Ch., Rott, P., Loos, M.B.M., Whittaker, S., Cámara Lapuente, S., Hodges, Christopher, Hondius, E., Micklitz, Hans-W. H., Cafaggi, F., Law, S., Terryn, Evelyne, Stijns, S., Jansen, S., Grundmann, S., and De Coninck, H.

Subjects
Droit des marques - Droit de la consommation, Droits intellectuels, Droit économique
Abstract

Cet article concerne la notion de consommateur moyen en droit des marques, critère d’appréciation-clé en droit des marques comme en droit de la consommation. Le « consommateur moyen » est un être abstrait, une fiction juridique, imaginé par la Cour de Justice de l’Union européenne, dont la jurisprudence n’est pas toujours ni très convaincante, ni très cohérente, comme le montre la présente contribution., info:eu-repo/semantics/published

Published
2013

30. Total parenteral nutrition induces a shift in the firmicutes to bacteroidetes ratio in association with paneth cell activation in rats

Author

Hodin, C.M.I., Visschers, R.G.J., Rensen, S.S.M., Boonen, B., Olde Damink, S., Lenaerts, K., Buurman, W.A., Surgery, Orthopedie, and RS: NUTRIM - R2 - Gut-liver homeostasis

Subjects
digestive system
Abstract

The use of total parenteral nutrition (TPN) in the treatment of critically ill patients has been the subject of debate because it has been associated with disturbances in intestinal homeostasis. Important factors in maintaining the intestinal homeostasis are the intestinal microbiota and Paneth cells, which exist in a mutually amendable relationship. We hypothesized that the disturbed intestinal homeostasis in TPN-fed individuals results from an interplay between a shift in microbiota composition and alterations in Paneth cells. We studied the microbiota composition and expression of Paneth cell antimicrobial proteins in rats receiving TPN or a control diet for 3, 7, or 14 d. qPCR analysis of DNA extracts from small intestinal luminal contents of TPN-fed rats showed a shift in Firmicutes:Bacteroidetes ratio in favor of Bacteroidetes after 14 d (P < 0.05) compared with the control group. This finding coincided with greater staining intensity for lysozyme and significantly greater mRNA expression of Paneth cell antimicrobial proteins lysozyme (P < 0.05), rat alpha-defensin 5 (P < 0.01), and rat alpha-defensin 8 (P < 0.01). Finally, 14 d of TPN resulted in greater circulating ileal lipid-binding protein concentrations (P < 0.05) and greater leakage of horseradish peroxidase (P < 0.01), which is indicative of enterocyte damage and a breached intestinal barrier. Our findings show a shift in intestinal microbiota in TPN-fed rats that correlated with changes in Paneth cell lysozyme expression (r(s) = -0.75, P < 0.01). Further studies that include interventions with microbiota or nutrients that modulate them may yield information on the involvement of microbiota and Paneth cells in TPN-associated intestinal compromise.

Published
2012

31. Reduced Paneth cell antimicrobial protein levels correlate with activation of the unfolded protein response in the gut of obese individuals

Author

Hodin, C.M.I., Verdam, F.J., Grootjans, J., Rensen, S.S.M., Verheyen, F.K., Dejong, C.H.C., Buurman, W.A., Greve, J.W., Lenaerts, K., RS: NUTRIM - R2 - Gut-liver homeostasis, Surgery, Genetica & Celbiologie, and RS: CARIM School for Cardiovascular Diseases

Subjects
digestive system
Abstract

The intestinal microbiota is increasingly acknowledged to play a crucial role in the development of obesity. A shift in intestinal microbiota composition favouring the presence of Firmicutes over Bacteroidetes has been observed in obese subjects. A similar shift has been reported in mice with deficiency of active Paneth cell alpha-defensins. We aimed at investigating changes in Paneth cell antimicrobial levels in the gut of obese subjects. Next, we studied activation of the unfolded protein response (UPR) as a possible mechanism involved in altered Paneth cell function. Paneth cell numbers were counted in jejunal sections of 15 severely obese (BMI > 35) and 15 normal weight subjects. Expression of Paneth cell antimicrobials human alpha-defensin 5 (HD5) and lysozyme were investigated using immunohistochemistry, qPCR, and western blot. Activation of the UPR was assessed with western blot. Severely obese subjects showed decreased protein levels of both HD5 and lysozyme, while Paneth cell numbers were unchanged. Lysozyme protein levels correlated inversely with BMI. Increased expression of HD5 (DEFA5) and lysozyme (LYZ) transcripts in the intestine of obese subjects prompted us to investigate a possible translational block caused by UPR activation. Binding protein (BiP) and activating transcription factor 4 (ATF4) levels were increased, confirming activation of the UPR in the gut of obese subjects. Furthermore, levels of both proteins correlated with BMI. Involvement of the UPR in the lowered antimicrobial protein levels in obese subjects was strongly suggested by a negative correlation between BiP levels and lysozyme levels. Additionally, indications of ER stress were apparent in Paneth cells of obese subjects. Our findings provide the first evidence for altered Paneth cell function in obesity, which may have important implications for the obesity-associated shift in microbiota composition. In addition, we show activation of the UPR in the intestine of obese subjects, which may underlie the observed Paneth cell compromise. Copyright (c) 2011 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2011

33. Human intestinal ischemia-reperfusion-induced inflammation characterized: experiences from a new translational model

Author

Grootjans, J., Lenaerts, K., Derikx, J.P., Matthijsen, R.A., de Bruine, A.P., van Bijnen, A.A., van Dam, R.M., Dejong, C.H.C., Buurman, W.A., RS: NUTRIM - R2 - Gut-liver homeostasis, RS: GROW - School for Oncology and Reproduction, Surgery, and Pathologie

Subjects
DAMAGE, INVOLVEMENT, SYSTEMIC INFLAMMATION, ORGAN DYSFUNCTION, COMPLEMENT PATHWAY, LEUKOCYTE, GUT ISCHEMIA, INHIBITION, RAT, ISCHEMIA/REPERFUSION INJURY
Abstract

Human intestinal ischemia-reperfusion (IR) is a frequent phenomenon carrying high morbidity and mortality. Although intestinal IR-induced inflammation has been studied extensively in animal models, human intestinal IR induced inflammatory responses remain to be characterized. Using a newly developed human intestinal IR model, we show that human small intestinal ischemia results in massive leakage of intracellular components from ischemically damaged cells, as indicated by increased arteriovenous concentration differences of intestinal fatty acid binding protein and soluble cytokeratin 18. IR-induced intestinal barrier integrity loss resulted in free exposure of the gut basal membrane (collagen IV staining) to intraluminal contents, which was accompanied by increased arteriovenous concentration differences of endotoxin. Western blot for complement activation product C3c and immunohistochemistry for activated C3 revealed complement activation after IR. In addition, intestinal IR resulted in enhanced tissue mRNA expression of IL-6, IL-8, and TNF-alpha, which was accompanied by IL-6 and IL-8 release into the circulation. Expression of intercellular adhesion molecule-1 was markedly increased during reperfusion, facilitating influx of neutrophils into IR-damaged villus tips. In conclusion, this study for the first time shows the sequelae of human intestinal IR-induced inflammation, which is characterized by complement activation, production and release of cytokines into the circulation, endothelial activation, and neutrophil influx into IR-damaged tissue.

Published
2010

34. Differentiation stage-dependent preferred uptake of basolateral (systemic) glutamine into Caco-2 cells results in its accumulation in proteins with a role in cell-cell interaction

Author

Lenaerts, K., Mariman, E., Bouwman, F.G., Renes, J., Humane Biologie, and RS: NUTRIM School of Nutrition and Translational Research in Metabolism

Abstract

Glutamine is an essential amino acid for enterocytes, especially in states of critical illness and injury. In several studies it has been speculated that the beneficial effects of glutamine are dependent on the route of supply (luminal or systemic). The aim of this study was to investigate the relevance of both routes of glutamine delivery to in vitro intestinal cells and to explore the molecular basis for proposed beneficial glutamine effects: (a) by determining the relative uptake of radiolabelled glutamine in Caco-2 cells; (b) by assessing the effect of glutamine on the proteome of Caco-2 cells using a 2D gel electrophoresis approach; and (c) by examining glutamine incorporation into cellular proteins using a new mass spectrometry-based method with stable isotope labelled glutamine. Results of this study show that exogenous glutamine is taken up by Caco-2 cells from both the apical and the basolateral side. Basolateral uptake consistently exceeds apical uptake and this phenomenon is more pronounced in 5-day-differentiated cells than in 15-day-differentiated cells. No effect of exogenous glutamine supply on the proteome was detected. However, we demonstrated that exogenous glutamine is incorporated into newly synthesized proteins and this occurred at a faster rate from basolateral glutamine, which is in line with the uptake rates. Interestingly, a large number of rapidly labelled proteins is involved in establishing cell-cell interactions. In this respect, our data may point to a molecular basis for observed beneficial effects of glutamine on intestinal cells and support results from studies with critically ill patients where parenteral glutamine supplementation is preferred over luminal supplementation.

Published
2005

37. Lipid-rich enteral nutrition regulates mucosal mast cell activation via the vagal anti-inflammatory reflex

Author

Haan, J.J. de, Hadfoune, M., Lubbers, T., Hodin, C., Lenaerts, K., Ito, A., Verbaeys, I., Skynner, M.J., Cailotto, C., Vliet, J.A. van der, Jonge, W.J. de, Greve, J.W., Buurman, W.A., Haan, J.J. de, Hadfoune, M., Lubbers, T., Hodin, C., Lenaerts, K., Ito, A., Verbaeys, I., Skynner, M.J., Cailotto, C., Vliet, J.A. van der, Jonge, W.J. de, Greve, J.W., and Buurman, W.A.

Abstract

Item does not contain fulltext, Nutritional stimulation of the cholecystokinin-1 receptor (CCK-1R) and nicotinic acetylcholine receptor (nAChR)-mediated vagal reflex was shown to reduce inflammation and preserve intestinal integrity. Mast cells are important early effectors of the innate immune response; therefore modulation of mucosal mast cells is a potential therapeutic target to control the acute inflammatory response in the intestine. The present study investigates intestinal mast cell responsiveness upon nutritional activation of the vagal anti-inflammatory reflex during acute inflammation. Mucosal mast cell degranulation was induced in C57/Bl6 mice by administration of Salmonella enterica LPS. Lipid-rich enteral feeding prior to LPS significantly decreased circulatory levels of mouse mast cell protease at 30 min post-LPS compared with isocaloric low-lipid nutrition or fasting. CCK-1R blockage reversed the inhibitory effects of lipid-rich feeding, whereas stimulation of the peripheral CCK-1R mimicked nutritional mast cell inhibition. The effects of lipid-rich nutrition were negated by nAChR blockers chlorisondamine and alpha-bungarotoxin and vagal intestinal denervation. Accordingly, release of beta-hexosaminidase by MC/9 mast cells following LPS or IgE-ovalbumin complexes was dose dependently inhibited by acetylcholine and nicotine. Application of GSK1345038A, a specific agonist of the nAChR alpha7, in bone marrow-derived mast cells from nAChR beta2-/- and wild types indicated that cholinergic inhibition of mast cells is mediated by the nAChR alpha7 and is independent of the nAChR beta2. Together, the present study reveals mucosal mast cells as a previously unknown target of the nutritional anti-inflammatory vagal reflex.

Published
2013

38. Ischaemia-induced mucus barrier loss and bacterial penetration are rapidly counteracted by increased goblet cell secretory activity in human and rat colon

Author

Grootjans, J. (Joep), Hundscheid, I.H.R. (Inca H.), Lenaerts, K. (Kaatje), Boonen, B. (Bas), Renes, I.B. (Ingrid), Verheyen, J. (Jens), Dejong, C.H. (Cees), Meyenfeldt, M.F. (Maarten) von, Beets, G.L. (Geerard), Buurman, W.A. (Wim), Grootjans, J. (Joep), Hundscheid, I.H.R. (Inca H.), Lenaerts, K. (Kaatje), Boonen, B. (Bas), Renes, I.B. (Ingrid), Verheyen, J. (Jens), Dejong, C.H. (Cees), Meyenfeldt, M.F. (Maarten) von, Beets, G.L. (Geerard), and Buurman, W.A. (Wim)

Published
2013
Full Text
View/download PDF

41. Exercise-induced splanchnic hypoperfusion results in gut dysfunction in healthy men

Author

Wijck, K. van, Lenaerts, K., Loon, L.J.C. van, Peters, W.H.M., Buurman, W.A., Dejong, C.H., Wijck, K. van, Lenaerts, K., Loon, L.J.C. van, Peters, W.H.M., Buurman, W.A., and Dejong, C.H.

Abstract

Contains fulltext : 96903.pdf (publisher's version ) (Open Access), BACKGROUND: Splanchnic hypoperfusion is common in various pathophysiological conditions and often considered to lead to gut dysfunction. While it is known that physiological situations such as physical exercise also result in splanchnic hypoperfusion, the consequences of flow redistribution at the expense of abdominal organs remained to be determined. This study focuses on the effects of splanchnic hypoperfusion on the gut, and the relationship between hypoperfusion, intestinal injury and permeability during physical exercise in healthy men. METHODS AND FINDINGS: Healthy men cycled for 60 minutes at 70% of maximum workload capacity. Splanchnic hypoperfusion was assessed using gastric tonometry. Blood, sampled every 10 minutes, was analyzed for enterocyte damage parameters (intestinal fatty acid binding protein (I-FABP) and ileal bile acid binding protein (I-BABP)). Changes in intestinal permeability were assessed using sugar probes. Furthermore, liver and renal parameters were assessed. Splanchnic perfusion rapidly decreased during exercise, reflected by increased gap(g-a)pCO(2) from -0.85+/-0.15 to 0.85+/-0.42 kPa (p<0.001). Hypoperfusion increased plasma I-FABP (615+/-118 vs. 309+/-46 pg/ml, p<0.001) and I-BABP (14.30+/-2.20 vs. 5.06+/-1.27 ng/ml, p<0.001), and hypoperfusion correlated significantly with this small intestinal damage (r(S) = 0.59; p<0.001). Last of all, plasma analysis revealed an increase in small intestinal permeability after exercise (p<0.001), which correlated with intestinal injury (r(S) = 0.50; p<0.001). Liver parameters, but not renal parameters were elevated. CONCLUSIONS: Exercise-induced splanchnic hypoperfusion results in quantifiable small intestinal injury. Importantly, the extent of intestinal injury correlates with transiently increased small intestinal permeability, indicating gut barrier dysfunction in healthy individuals. These physiological observations increase our knowledge of splanchnic hypoperfusion sequelae, and may help to u

Published
2011

42. Exercise-induced splanchnic hypoperfusion results in gut dysfunction in healthy men

Author

van Wijck, K., van Wijck, K., Lenaerts, K., van Loon, L.J.C., Peters, W. H., Buurman, W.A., Dejong, C.H.C., van Wijck, K., van Wijck, K., Lenaerts, K., van Loon, L.J.C., Peters, W. H., Buurman, W.A., and Dejong, C.H.C.

Abstract

BACKGROUND: Splanchnic hypoperfusion is common in various pathophysiological conditions and often considered to lead to gut dysfunction. While it is known that physiological situations such as physical exercise also result in splanchnic hypoperfusion, the consequences of flow redistribution at the expense of abdominal organs remained to be determined. This study focuses on the effects of splanchnic hypoperfusion on the gut, and the relationship between hypoperfusion, intestinal injury and permeability during physical exercise in healthy men. METHODS AND FINDINGS: Healthy men cycled for 60 minutes at 70% of maximum workload capacity. Splanchnic hypoperfusion was assessed using gastric tonometry. Blood, sampled every 10 minutes, was analyzed for enterocyte damage parameters (intestinal fatty acid binding protein (I-FABP) and ileal bile acid binding protein (I-BABP)). Changes in intestinal permeability were assessed using sugar probes. Furthermore, liver and renal parameters were assessed. Splanchnic perfusion rapidly decreased during exercise, reflected by increased gap(g-a)pCO(2) from -0.85+/-0.15 to 0.85+/-0.42 kPa (p<0.001). Hypoperfusion increased plasma I-FABP (615+/-118 vs. 309+/-46 pg/ml, p<0.001) and I-BABP (14.30+/-2.20 vs. 5.06+/-1.27 ng/ml, p<0.001), and hypoperfusion correlated significantly with this small intestinal damage (r(S) = 0.59; p<0.001). Last of all, plasma analysis revealed an increase in small intestinal permeability after exercise (p<0.001), which correlated with intestinal injury (r(S) = 0.50; p<0.001). Liver parameters, but not renal parameters were elevated. CONCLUSIONS: Exercise-induced splanchnic hypoperfusion results in quantifiable small intestinal injury. Importantly, the extent of intestinal injury correlates with transiently increased small intestinal permeability, indicating gut barrier dysfunction in healthy individuals. These physiological observations increase our knowledge of splanchnic hypoperfusion sequelae

Published
2011

Catalog

Books, media, physical & digital resources
See catalog results