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1. Lymphatic Invasion of Plakoglobin-Dependent Tumor Cell Clusters Drives Formation of Polyclonal Lung Metastases in Colon Cancer

Author

Küçükköse, Emre, Laoukili, Jamila, Gorelick, Alexander N., Degner, Sebastian, Laclé, Miangela M., van den Bent, Lotte, Peters, Niek A., Verheem, André, Hung, Wei-Ting, Frenkel, Nicola C., Wassenaar, Emma C.E., Lansu, Nico, Lenos, Kristiaan J., Vermeulen, Louis, Koopman, Miriam, Roodhart, Jeanine M.L., Kops, Geert J.P.L., Borel Rinkes, Inne H.M., Hagendoorn, Jeroen, Naxerova, Kamila, and Kranenburg, Onno

Published
2023
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3. KIT promotes tumor stroma formation and counteracts tumor-suppressive TGFβ signaling in colorectal cancer

Author

Emre Küçükköse, Niek A. Peters, Inge Ubink, Veere A. M. van Keulen, Roxanna Daghighian, André Verheem, Jamila Laoukili, and Onno Kranenburg

Subjects
Cytology, QH573-671
Abstract

Abstract Expression profiling has identified four consensus molecular subtypes (CMS1-4) in colorectal cancer (CRC). The receptor tyrosine kinase KIT has been associated with the most aggressive subtype, CMS4. However, it is unclear whether, and how, KIT contributes to the aggressive features of CMS4 CRC. Here, we employed genome-editing technologies in patient-derived organoids (PDOs) to study KIT function in CRC in vitro and in vivo. CRISPR-Cas9-mediated deletion of the KIT gene caused a partial mesenchymal-to-epithelial phenotype switch and a strong reduction of intra-tumor stromal content. Vice versa, overexpression of KIT caused a partial epithelial-to-mesenchymal phenotype switch, a strong increase of intra-tumor stromal content, and high expression of TGFβ1. Surprisingly, the levels of phosphorylated SMAD2 were significantly lower in KIT-expressing versus KIT-deficient tumor cells. In vitro analyses showed that TGFβ signaling in PDOs limits their regenerative capacity. Overexpression of KIT prevented tumor-suppressive TGFβ signaling, while KIT deletion sensitized PDOs to TGFβ-mediated growth inhibition. Mechanistically, we found that KIT expression caused a strong reduction in the expression of SMAD2, a central mediator of canonical TGFβ signaling. We propose that KIT induces a pro-fibrotic tumor microenvironment by stimulating TGFβ expression, and protects the tumor cells from tumor-suppressive TGFβ signaling by inhibiting SMAD2 expression.

Published
2022
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4. Tissue clearing and immunostaining to visualize the spatial organization of vasculature and tumor cells in mouse liver

Author

Nicola Frenkel, Susanna Poghosyan, Jan Willem van Wijnbergen, Lotte van den Bent, Liza Wijler, André Verheem, Inne Borel Rinkes, Onno Kranenburg, and Jeroen Hagendoorn

Subjects
tissue clearing, liver vasculature, CLARITY, 3DISCO, iDISCO, tumor micro environment, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

The liver has a complex and hierarchical segmental organization of arteries, portal veins, hepatic veins and lymphatic vessels. In-depth imaging of liver vasculature and malignancies could improve knowledge on tumor micro-environment, local tumor growth, invasion, as well as metastasis. Non-invasive imaging techniques such as computed tomography (CT), magnetic resonance imaging (MRI) and positron-emission transmission (PET) are routine for clinical imaging, but show inadequate resolution at cellular and subcellular level. In recent years, tissue clearing – a technique rendering tissues optically transparent allowing enhanced microscopy imaging – has made great advances. While mainly used in the neurobiology field, recently more studies have used clearing techniques for imaging other organ systems as well as tumor tissues. In this study, our aim was to develop a reproducible tissue clearing and immunostaining model for visualizing intrahepatic blood microvasculature and tumor cells in murine colorectal liver metastases. CLARITY and 3DISCO/iDISCO+ are two established clearing methods that have been shown to be compatible with immunolabelling, most often in neurobiology research. In this study, CLARITY unfortunately resulted in damaged tissue integrity of the murine liver lobes and no specific immunostaining. Using the 3DISCO/iDISCO+ method, liver samples were successfully rendered optically transparent. After which, successful immunostaining of the intrahepatic microvasculature using panendothelial cell antigen MECA-32 and colorectal cancer cells using epithelial cell adhesion molecule (EpCAM) was established. This approach for tumor micro-environment tissue clearing would be especially valuable for allowing visualization of spatial heterogeneity and complex interactions of tumor cells and their environment in future studies.

Published
2023
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5. Voluntary exercise influences metastatic organotropism in a murine colorectal cancer model

Author

Liza A. Wijler, Danielle A.E. Raats, Andre Verheem, Anna M. denOtter, Helene Rundqvist, Miriam vanDijk, Anne M. May, and Onno Kranenburg

Subjects
Exercise oncology, Running, Colorectal cancer, Metastasis, Organotropism, Inflammation, Internal medicine, RC31-1245
Abstract

Abstract Background Physical activity is associated with a lower risk of colorectal cancer (CRC) and CRC‐specific mortality. However, evidence for a causal relationship between physical activity and disease progression is lacking. Here, we have used CRC organoids to create a novel mouse model for spontaneous metastasis formation to multiple organs. We have used this model to assess the influence of voluntary exercise on disease progression. Methods Collagen‐embedded murine colorectal tumour organoids were transplanted into the livers of immunocompetent C57Bl/6 mice using microsurgery. Voluntary exercise in tumour‐bearing mice was modelled by offering running wheels continuously (n = 12) or 3 h/day (n = 12) versus no wheel access (n = 12). Running wheel revolutions were cumulatively measured every 30 min and physical activity was continuously monitored by infrared cameras. Food intake was monitored throughout the experiment and body composition was assessed with echoMRI. Animals were sacrificed 14 weeks after tumour initiation. Tumour load was quantified by EpCAM immunohistochemistry staining. Systemic inflammation parameters were assessed in blood plasma by a multiplex immunoassay. Results Tumour growth was initiated by implantation of CRC organoids into the livers of immunocompetent mice. The resulting tumours spontaneously formed distant metastases to non‐implanted liver lobes and to the lungs. Mice with access to the running wheels for 3 h/day ran relatively short distances (2.3 ± 0.3 km/night; 221 ± 29 km total distance) with relatively high intensity (wheel revolutions/h). Mice with continuous access to the running wheels ran significantly longer distances (6.6 ± 3.0 km/night; 600 ± 290 km total distance) with a significantly lower intensity. Both exercise groups showed increased lean body mass, and decreased fat mass and body weight compared with tumour‐bearing control mice. Food intake was unaffected by exercise or tumour growth. Primary tumour growth was not significantly affected by exercise. However, mice with continuous wheel access (long distance‐lower intensity group) displayed increased lung metastasis and decreased liver metastasis formation, when compared with the sedentary control group. Short distance‐higher intensity exercise did not affect metastasis formation. Analysis of blood cytokine levels revealed that mice with continuous wheel access displayed signs of systemic inflammation. Conclusions These results suggest that exercise has the potential to influence the patterns and extent of metastasis in CRC, and that the degree and intensity of exercise are likely to be important variables. Confirmation of these results in additional preclinical models with or without systemic treatment is warranted.

Published
2022
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6. Modeling resistance of colorectal peritoneal metastases to immune checkpoint blockade in humanized mice

Author

Onno Kranenburg, Hergen Spits, Julien Villaudy, Madalina Cercel, Miriam Koopman, Cornelis J A Punt, Jamila Laoukili, Andre Verheem, Inne H M Borel Rinkes, Emre Küçükköse, Balthasar A Heesters, Susan van Hal, Sylvia F Boj, and Jeanine M L Roodhart

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Background The immunogenic nature of metastatic colorectal cancer (CRC) with high microsatellite instability (MSI-H) underlies their responsiveness to immune checkpoint blockade (ICB). However, resistance to ICB is commonly observed, and is associated with the presence of peritoneal-metastases and ascites formation. The mechanisms underlying this site-specific benefit of ICB are unknown.Methods We created a novel model for spontaneous multiorgan metastasis in MSI-H CRC tumors by transplanting patient-derived organoids (PDO) into the cecum of humanized mice. Anti-programmed cell death protein-1 (PD-1) and anti-cytotoxic T-lymphocytes-associated protein 4 (CTLA-4) ICB treatment effects were analyzed in relation to the immune context of primary tumors, liver metastases, and peritoneal metastases. Immune profiling was performed by immunohistochemistry, flow cytometry and single-cell RNA sequencing. The role of B cells was assessed by antibody-mediated depletion. Immunosuppressive cytokine levels (interleukin (IL)-10, transforming growth factor (TGF)b1, TGFb2, TGFb3) were determined in ascites and serum samples by ELISA.Results PDO-initiated primary tumors spontaneously metastasized to the liver and the peritoneum. Peritoneal-metastasis formation was accompanied by the accumulation of ascites. ICB completely cleared liver metastases and reduced primary tumor mass but had no effect on peritoneal metastases. This mimics clinical observations. After therapy discontinuation, primary tumor masses progressively decreased, but peritoneal metastases displayed unabated growth. Therapy efficacy correlated with the formation of tertiary lymphoid structures (TLS)—containing B cells and juxtaposed T cells—and with expression of an interferon-γ signature together with the B cell chemoattractant CXCL13. B cell depletion prevented liver-metastasis clearance by anti-CTLA-4 treatment. Peritoneal metastases were devoid of B cells and TLS, while the T cells in these lesions displayed a dysfunctional phenotype. Ascites samples from patients with cancer with peritoneal metastases and from the mouse model contained significantly higher levels of IL-10, TGFb1, TGFb2 and TGFb3 than serum samples.Conclusions By combining organoid and humanized mouse technologies, we present a novel model for spontaneous multiorgan metastasis by MSI-H CRC, in which the clinically observed organ site-dependent benefit of ICB is recapitulated. Moreover, we provide empirical evidence for a critical role for B cells in the generation of site-dependent antitumor immunity following anti-CTLA-4 treatment. High levels of immunosuppressive cytokines in ascites may underlie the observed resistance of peritoneal metastases to ICB.

Published
2022
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7. Liver lymphatic drainage patterns follow segmental anatomy in a murine model

Author

Nicola C. Frenkel, Susanna Poghosyan, André Verheem, Timothy P. Padera, Inne H. M. Borel Rinkes, Onno Kranenburg, and Jeroen Hagendoorn

Subjects
Medicine, Science
Abstract

Abstract The liver’s cellular functions are sustained by a hierarchical, segmentally-organized vascular system. Additionally, liver lymphatic vessels are thought to drain to perihepatic lymph nodes. Surprisingly, while recent findings highlight the importance of organ-specific lymphatics, the functional anatomy of liver lymphatics has not been mapped out. In literature, no segmental or preferential lymphatic drainage patterns are known to exist. We employ a novel murine model of liver lymphangiography and in vivo microscopy to delineate the lymphatic drainage patterns of individual liver lobes. Our data from blue dye liver lymphangiography show preferential lymphatic drainage patterns: Right lobe mainly to hepatoduodenal ligament lymph node 1 (LN1); left lobe to hepatoduodenal ligament LN1 + LN2 concurrently; median lobe showed a more variable LN1/LN2 drainage pattern with increased (sometimes exclusive) mediastinal thoracic lymph node involvement, indicating that part of the liver can drain directly to the mediastinum. Upon ferritin lymphangiography, we observed no functional communication between the lobar lymphatics. Altogether, these results show the existence of preferential lymphatic drainage patterns in the murine liver. Moreover, this drainage can occur directly to mediastinal lymph nodes and there is no interlobar lymphatic flow. Collectively, these data provide the first direct evidence that liver lymphatic drainage patterns follow segmental anatomy.

Published
2020
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9. Onward Spread from Liver Metastases Is a Major Cause of Multi-Organ Metastasis in a Mouse Model of Metastatic Colon Cancer.

Author

Wijler, Liza A., Viergever, Bastiaan J., Strating, Esther, van Schelven, Susanne J., Poghosyan, Susanna, Frenkel, Nicola C., te Rietmole, Hedy, Verheem, Andre, Raats, Danielle A. E., Borel Rinkes, Inne H. M., Hagendoorn, Jeroen, and Kranenburg, Onno

Subjects
LIVER tumors, BIOLOGICAL models, MACROPHAGES, RESEARCH funding, DESCRIPTIVE statistics, COLON tumors, METASTASIS, MICE, LUMINESCENCE spectroscopy, IMMUNOHISTOCHEMISTRY, ANIMAL experimentation, DATA analysis software, DISEASE complications
Abstract

Simple Summary: The prognosis of patients with metastatic colon cancer remains very poor. A minority of patients, mostly those with liver-restricted disease, are eligible for intentionally curative surgery. In most cases, however, the presence of extra-hepatic metastases precludes curative treatment. The aim of this study was to gain insight into the processes governing multi-organ metastasis. We applied the microsurgical transplantation of mouse colon tumor organoids into the caecum or into the liver of syngeneic immunocompetent mice. Colon tumors growing in the liver seeded distant metastases to the lungs and to the peritoneal cavity more efficiently than those growing in the caecum. This was associated with the formation of hotspots of macrophage-surrounded vitronectin-positive blood vessels, specifically in liver tumors. Thus, 'onward spread' from liver metastases plays a major role in multi-organ metastasis, potentially through liver-specific vascular hotspots. The therapeutic targeting of these signals may help achieve the containment of the disease within the liver, thus preventing multi-organ metastasis. Colorectal cancer metastasizes predominantly to the liver but also to the lungs and the peritoneum. The presence of extra-hepatic metastases limits curative (surgical) treatment options and is associated with very poor survival. The mechanisms governing multi-organ metastasis formation are incompletely understood. Here, we tested the hypothesis that the site of tumor growth influences extra-hepatic metastasis formation. To this end, we implanted murine colon cancer organoids into the primary tumor site (i.e., the caecum) and into the primary metastasis site (i.e., the liver) in immunocompetent mice. The organoid-initiated liver tumors were significantly more efficient in seeding distant metastases compared to tumors of the same origin growing in the caecum (intra-hepatic: 51 vs. 40%, p = 0.001; peritoneal cavity: 51% vs. 33%, p = 0.001; lungs: 30% vs. 7%, p = 0.017). The enhanced metastatic capacity of the liver tumors was associated with the formation of 'hotspots' of vitronectin-positive blood vessels surrounded by macrophages. RNA sequencing analysis of clinical samples showed a high expression of vitronectin in liver metastases, along with signatures reflecting hypoxia, angiogenesis, coagulation, and macrophages. We conclude that 'onward spread' from liver metastases is facilitated by liver-specific microenvironmental signals that cause the formation of macrophage-associated vascular hotspots. The therapeutic targeting of these signals may help to contain the disease within the liver and prevent onward spread. [ABSTRACT FROM AUTHOR]

Published
2024
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11. Voluntary exercise influences metastatic organotropism in a murine colorectal cancer model

Author

Andre Verheem, Liza A. Wijler, Miriam van Dijk, Anna M. Otter, Danielle A.E. Raats, Helene Rundqvist, Onno Kranenburg, and Anne M. May

Subjects
Oncology, Inflammation, medicine.medical_specialty, Colorectal cancer, business.industry, Organotropism, medicine.disease, RC31-1245, Running, Metastasis, Internal medicine, medicine, Exercise oncology, business
Abstract

Background Physical activity is associated with a lower risk of colorectal cancer (CRC) and CRC‐specific mortality. However, evidence for a causal relationship between physical activity and disease progression is lacking. Here, we have used CRC organoids to create a novel mouse model for spontaneous metastasis formation to multiple organs. We have used this model to assess the influence of voluntary exercise on disease progression. Methods Collagen‐embedded murine colorectal tumour organoids were transplanted into the livers of immunocompetent C57Bl/6 mice using microsurgery. Voluntary exercise in tumour‐bearing mice was modelled by offering running wheels continuously (n = 12) or 3 h/day (n = 12) versus no wheel access (n = 12). Running wheel revolutions were cumulatively measured every 30 min and physical activity was continuously monitored by infrared cameras. Food intake was monitored throughout the experiment and body composition was assessed with echoMRI. Animals were sacrificed 14 weeks after tumour initiation. Tumour load was quantified by EpCAM immunohistochemistry staining. Systemic inflammation parameters were assessed in blood plasma by a multiplex immunoassay. Results Tumour growth was initiated by implantation of CRC organoids into the livers of immunocompetent mice. The resulting tumours spontaneously formed distant metastases to non‐implanted liver lobes and to the lungs. Mice with access to the running wheels for 3 h/day ran relatively short distances (2.3 ± 0.3 km/night; 221 ± 29 km total distance) with relatively high intensity (wheel revolutions/h). Mice with continuous access to the running wheels ran significantly longer distances (6.6 ± 3.0 km/night; 600 ± 290 km total distance) with a significantly lower intensity. Both exercise groups showed increased lean body mass, and decreased fat mass and body weight compared with tumour‐bearing control mice. Food intake was unaffected by exercise or tumour growth. Primary tumour growth was not significantly affected by exercise. However, mice with continuous wheel access (long distance‐lower intensity group) displayed increased lung metastasis and decreased liver metastasis formation, when compared with the sedentary control group. Short distance‐higher intensity exercise did not affect metastasis formation. Analysis of blood cytokine levels revealed that mice with continuous wheel access displayed signs of systemic inflammation. Conclusions These results suggest that exercise has the potential to influence the patterns and extent of metastasis in CRC, and that the degree and intensity of exercise are likely to be important variables. Confirmation of these results in additional preclinical models with or without systemic treatment is warranted.

Published
2022

12. Modeling resistance of colorectal peritoneal metastases to immune checkpoint blockade in humanized mice

Author

Küçükköse, Emre, Heesters, Balthasar A., Villaudy, Julien, Verheem, André, Cercel, Madalina, Van Hal, Susan, Boj, Sylvia F., Borel Rinkes, Inne H.M., Punt, Cornelis J.A., Roodhart, Jeanine M.L., Laoukili, Jamila, Koopman, Miriam, Spits, Hergen, Kranenburg, Onno, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Oncology, Experimental Immunology, AII - Cancer immunology, and CCA - Cancer biology and immunology

Subjects
Pharmacology, Cancer Research, Liver Neoplasms, Immunology, Ascites, Mice, Transforming Growth Factor beta3, Oncology, Animals, Cytokines, Immunology and Allergy, Molecular Medicine, Peritoneum, Colorectal Neoplasms, Immune Checkpoint Inhibitors, Peritoneal Neoplasms
Abstract

BackgroundThe immunogenic nature of metastatic colorectal cancer (CRC) with high microsatellite instability (MSI-H) underlies their responsiveness to immune checkpoint blockade (ICB). However, resistance to ICB is commonly observed, and is associated with the presence of peritoneal-metastases and ascites formation. The mechanisms underlying this site-specific benefit of ICB are unknown.MethodsWe created a novel model for spontaneous multiorgan metastasis in MSI-H CRC tumors by transplanting patient-derived organoids (PDO) into the cecum of humanized mice. Anti-programmed cell death protein-1 (PD-1) and anti-cytotoxic T-lymphocytes-associated protein 4 (CTLA-4) ICB treatment effects were analyzed in relation to the immune context of primary tumors, liver metastases, and peritoneal metastases. Immune profiling was performed by immunohistochemistry, flow cytometry and single-cell RNA sequencing. The role of B cells was assessed by antibody-mediated depletion. Immunosuppressive cytokine levels (interleukin (IL)-10, transforming growth factor (TGF)b1, TGFb2, TGFb3) were determined in ascites and serum samples by ELISA.ResultsPDO-initiated primary tumors spontaneously metastasized to the liver and the peritoneum. Peritoneal-metastasis formation was accompanied by the accumulation of ascites. ICB completely cleared liver metastases and reduced primary tumor mass but had no effect on peritoneal metastases. This mimics clinical observations. After therapy discontinuation, primary tumor masses progressively decreased, but peritoneal metastases displayed unabated growth. Therapy efficacy correlated with the formation of tertiary lymphoid structures (TLS)—containing B cells and juxtaposed T cells—and with expression of an interferon-γ signature together with the B cell chemoattractant CXCL13. B cell depletion prevented liver-metastasis clearance by anti-CTLA-4 treatment. Peritoneal metastases were devoid of B cells and TLS, while the T cells in these lesions displayed a dysfunctional phenotype. Ascites samples from patients with cancer with peritoneal metastases and from the mouse model contained significantly higher levels of IL-10, TGFb1, TGFb2 and TGFb3 than serum samples.ConclusionsBy combining organoid and humanized mouse technologies, we present a novel model for spontaneous multiorgan metastasis by MSI-H CRC, in which the clinically observed organ site-dependent benefit of ICB is recapitulated. Moreover, we provide empirical evidence for a critical role for B cells in the generation of site-dependent antitumor immunity following anti-CTLA-4 treatment. High levels of immunosuppressive cytokines in ascites may underlie the observed resistance of peritoneal metastases to ICB.

Published
2022

13. Detection of Experimental Colorectal Peritoneal Metastases by a Novel PDGFRβ-Targeting Nanobody

Author

Esther Strating, Sjoerd Elias, Guus van Scharrenburg, Kaisa Luoto, André Verheem, Inne Borel Rinkes, Herman Steen, and Onno Kranenburg

Subjects
Cancer Research, platelet-derived growth factor receptor beta, colorectal cancer, peritoneal metastases, molecular imaging, Oncology
Abstract

Peritoneal metastases in colorectal cancer (CRC) belong to Consensus Molecular Subtype 4 (CMS4) and are associated with poor prognosis. Conventional imaging modalities, such as Computed Tomography (CT) and Fluorodeoxyglucose-Positron Emission Tomography (FDG-PET), perform very poorly in the detection of peritoneal metastases. However, the stroma-rich nature of these lesions provides a basis for developing molecular imaging strategies. In this study, conducted from 2019 to 2021, we aimed to generate a Platelet-Derived Growth Factor Receptor beta (PDGFRB)-binding molecular imaging tracer for the detection of CMS4 CRC, including peritoneal metastases. The expression of PDGFRB mRNA discriminated CMS4 from CMS1-3 (AUROC = 0.86 (95% CI 0.85–0.88)) and was associated with poor relapse-free survival. PDGFRB mRNA and protein levels were very high in all human peritoneal metastases examined (n = 66). Therefore, we generated a PDGFRB-targeting llama nanobody (VHH1E12). Biotin-labelled VHH1E12 bound to immobilized human and mouse PDGFRB with high affinity (EC50 human PDGFRB = 7 nM; EC50 murine PDGFRB = 0.8 nM), and to PDGFRB-expressing HEK293 cells grown in vitro. A pharmacokinetic analysis of IRDye-800CW-conjugated VHH1E12 in mice showed that the plasma half-life was 6 min. IRDye-800CW-conjugated VHH1E12 specifically accumulated in experimentally induced colorectal cancer peritoneal metastases in mice. A tissue analysis subsequently demonstrated co-localization of the nanobody with PDGFRB expression in the tumour stroma. Our results demonstrate the potential value of PDGFRB-targeted molecular imaging as a novel strategy for the non-invasive detection of CMS4 CRC, in particular, peritoneal metastases.

Published
2022
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18. Tissue clearing and immunostaining to visualize the spatial organization of vasculature and tumor cells in mouse liver.

Author

Frenkel, Nicola, Poghosyan, Susanna, van Wijnbergen, Jan Willem, van den Bent, Lotte, Wijler, Liza, Verheem, André, Rinkes, Inne Borel, Kranenburg, Onno, and Hagendoorn, Jeroen

Subjects
LIVER cells, COLORECTAL liver metastasis, CELL adhesion molecules, IMMUNOSTAINING, BLOOD vessels
Abstract

The liver has a complex and hierarchical segmental organization of arteries, portal veins, hepatic veins and lymphatic vessels. In-depth imaging of liver vasculature and malignancies could improve knowledge on tumor microenvironment, local tumor growth, invasion, as well as metastasis. Non-invasive imaging techniques such as computed tomography (CT), magnetic resonance imaging (MRI) and positron-emission transmission (PET) are routine for clinical imaging, but show inadequate resolution at cellular and subcellular level. In recent years, tissue clearing - a technique rendering tissues optically transparent allowing enhanced microscopy imaging - has made great advances. While mainly used in the neurobiology field, recently more studies have used clearing techniques for imaging other organ systems as well as tumor tissues. In this study, our aim was to develop a reproducible tissue clearing and immunostaining model for visualizing intrahepatic blood microvasculature and tumor cells in murine colorectal liver metastases. CLARITY and 3DISCO/iDISCO+ are two established clearing methods that have been shown to be compatible with immunolabelling, most often in neurobiology research. In this study, CLARITY unfortunately resulted in damaged tissue integrity of the murine liver lobes and no specific immunostaining. Using the 3DISCO/iDISCO+ method, liver samples were successfully rendered optically transparent. After which, successful immunostaining of the intrahepatic microvasculature using panendothelial cell antigen MECA-32 and colorectal cancer cells using epithelial cell adhesion molecule (EpCAM) was established. This approach for tumor micro-environment tissue clearing would be especially valuable for allowing visualization of spatial heterogeneity and complex interactions of tumor cells and their environment in future studies. [ABSTRACT FROM AUTHOR]

Published
2023
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20. 25 years of SEA: personal reflections on recent progress, current status and future prospects.

Author

Sadler, Barry and Verheem, Rob

Subjects
*OCEAN waves, *CONSORTIA, *ENVIRONMENTAL sciences
Abstract

2021 marked the 25th anniversary of the publication of our report 'SEA – status, challenges and future directions'. This report was part of an international study of the effectiveness of environmental assessment by a consortium of countries and organisations. In recognition of the anniversary, the NCEA has placed a digital version of the report, making it widely available through the internet for the first time (). The report documents the state of SEA practice at a key stage of process development and provides a benchmark against which subsequent progress can be reviewed. Using the report as a baseline, we take stock of the course of SEA development over the last quarter century and its bearing on the state of practice today. [ABSTRACT FROM AUTHOR]

Published
2023
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21. Impact of global Fxr deficiency on experimental acute pancreatitis and genetic variation in the FXR locus in human acute pancreatitis.

Author

Rian M Nijmeijer, Frank G Schaap, Alexander J J Smits, Andreas E Kremer, Louis M A Akkermans, Alfons B A Kroese, Ger T Rijkers, Marguerite E I Schipper, André Verheem, Cisca Wijmenga, Hein G Gooszen, and Karel J van Erpecum

Subjects
Medicine, Science
Abstract

BackgroundInfectious complications often occur in acute pancreatitis, related to impaired intestinal barrier function, with prolonged disease course and even mortality as a result. The bile salt nuclear receptor farnesoid X receptor (FXR), which is expressed in the ileum, liver and other organs including the pancreas, exhibits anti-inflammatory effects by inhibiting NF-κB activation and is implicated in maintaining intestinal barrier integrity and preventing bacterial overgrowth and translocation. Here we explore, with the aid of complementary animal and human experiments, the potential role of FXR in acute pancreatitis.MethodsExperimental acute pancreatitis was induced using the CCK-analogue cerulein in wild-type and Fxr-/- mice. Severity of acute pancreatitis was assessed using histology and a semi-quantitative scoring system. Ileal permeability was analyzed in vitro by Ussing chambers and an in vivo permeability assay. Gene expression of Fxr and Fxr target genes was studied by quantitative RT-PCR. Serum FGF19 levels were determined by ELISA in acute pancreatitis patients and healthy volunteers. A genetic association study in 387 acute pancreatitis patients and 853 controls was performed using 9 tagging single nucleotide polymorphisms (SNPs) covering the complete FXR gene and two additional functional SNPs.ResultsIn wild-type mice with acute pancreatitis, ileal transepithelial resistance was reduced and ileal mRNA expression of Fxr target genes Fgf15, SHP, and IBABP was decreased. Nevertheless, Fxr-/- mice did not exhibit a more severe acute pancreatitis than wild-type mice. In patients with acute pancreatitis, FGF19 levels were lower than in controls. However, there were no associations of FXR SNPs or haplotypes with susceptibility to acute pancreatitis, or its course, outcome or etiology.ConclusionWe found no evidence for a major role of FXR in acute human or murine pancreatitis. The observed altered Fxr activity during the course of disease may be a secondary phenomenon.

Published
2014
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22. Detection of Experimental Colorectal Peritoneal Metastases by a Novel PDGFRβ-Targeting Nanobody.

Author

Strating, Esther, Elias, Sjoerd, van Scharrenburg, Guus, Luoto, Kaisa, Verheem, André, Borel Rinkes, Inne, Steen, Herman, and Kranenburg, Onno

Subjects
RNA analysis, TISSUE analysis, CONSENSUS (Social sciences), IN vitro studies, IMMUNOGLOBULINS, CONFIDENCE intervals, MOLECULAR diagnosis, ANIMAL experimentation, IMMUNOHISTOCHEMISTRY, METASTASIS, PROGNOSIS, PHARMACOKINETICS, COLORECTAL cancer, PERITONEUM tumors, MOLECULAR biology, DIAGNOSTIC imaging, GENE expression, DESCRIPTIVE statistics, RADIOPHARMACEUTICALS, MESSENGER RNA, BIOTIN, MOLECULAR structure, CELL lines, COMPUTED tomography, DEOXY sugars, PROGRESSION-free survival, HISTOLOGY, PLATELET-derived growth factor, MICE, EMISSION-computed tomography, CHEMICAL inhibitors
Published
2022
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32. A contribution to the conceptualisation of quality in impact assessment

Author

Ben Cave, Peter N. Duinker, R. Verheem, Monica Fundingsland, Alan Bond, Francois Retief, and Alan Brown

Subjects
Quality management, Knowledge management, Ecology, business.industry, Management science, Impact assessment, Geography, Planning and Development, 0211 other engineering and technologies, 021107 urban & regional planning, 02 engineering and technology, 010501 environmental sciences, Management, Monitoring, Policy and Law, 01 natural sciences, Pluralism (political theory), Health care, Transactive memory, Normative, business, Legitimacy, 0105 earth and related environmental sciences, Plural
Abstract

Quality is much sought after in, and a basic foundation for, good impact assessment (IA). However, the term is rarely defined, has an uncertain relationship with IA effectiveness, and it means different things to different stakeholders, which can lead to debates over the legitimacy associated with an IA process. Thus, IA quality needs conceptualising to position research and practice within broader understandings. This paper contributes to this conceptualisation by identifying nine dimensions of quality through a process of literature review drawing on three fields of study in which quality and quality management have already been debated and conceptualised: education; health care; and business. This approach sidesteps the plural views on quality existing within the field of IA itself which might otherwise bias the identification of quality dimensions. We therefore propose that the dimensions of IA quality are: Efficiency; Optimacy; Conformance; Legitimacy; Equity; Capacity Maintenance; Transformative Capacity; and Quality Management. A literature review of IA research and practice confirms the relevance of the identified quality dimensions to IA. We identify, to an extent, the relationship between quality and effectiveness. Quality aligns with procedural and transactive effectiveness, partly aligns with normative effectiveness and is distinct from, but helps to deliver, substantive effectiveness.

Published
2018

33. Liver lymphatic drainage patterns follow segmental anatomy in a murine model.

Author

Frenkel, Nicola C., Poghosyan, Susanna, Verheem, André, Padera, Timothy P., Rinkes, Inne H. M. Borel, Kranenburg, Onno, and Hagendoorn, Jeroen

Subjects
LYMPHATICS, LYMPH nodes, LYMPHANGIOGRAPHY, MEDIASTINUM, FERRITIN, LABORATORY mice
Abstract

The liver's cellular functions are sustained by a hierarchical, segmentally-organized vascular system. Additionally, liver lymphatic vessels are thought to drain to perihepatic lymph nodes. Surprisingly, while recent findings highlight the importance of organ-specific lymphatics, the functional anatomy of liver lymphatics has not been mapped out. In literature, no segmental or preferential lymphatic drainage patterns are known to exist. We employ a novel murine model of liver lymphangiography and in vivo microscopy to delineate the lymphatic drainage patterns of individual liver lobes. Our data from blue dye liver lymphangiography show preferential lymphatic drainage patterns: Right lobe mainly to hepatoduodenal ligament lymph node 1 (LN1); left lobe to hepatoduodenal ligament LN1 + LN2 concurrently; median lobe showed a more variable LN1/LN2 drainage pattern with increased (sometimes exclusive) mediastinal thoracic lymph node involvement, indicating that part of the liver can drain directly to the mediastinum. Upon ferritin lymphangiography, we observed no functional communication between the lobar lymphatics. Altogether, these results show the existence of preferential lymphatic drainage patterns in the murine liver. Moreover, this drainage can occur directly to mediastinal lymph nodes and there is no interlobar lymphatic flow. Collectively, these data provide the first direct evidence that liver lymphatic drainage patterns follow segmental anatomy. [ABSTRACT FROM AUTHOR]

Published
2020
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35. SIRT1/PGC1a-dependent increase in oxidative phosphorylation supports chemotherapy resistance of colon cancer

Author

Susanne J. van Schelven, Kari Trumpi, Inne H.M. Borel Rinkes, Andre Verheem, Benjamin L. Emmink, Vincent C. J. de Boer, Onno Kranenburg, Thomas T. Vellinga, Tijana Borovski, Nikol Snoeren, Szabolcs Fatrai, Jan Koster, Other departments, Laboratory Genetic Metabolic Diseases, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, CCA -Cancer Center Amsterdam, and Oncogenomics

Subjects
Cancer Research, chemotherapy resistance, Colorectal cancer, medicine.medical_treatment, Respiratory chain, oxidative phosphorylation, Gene Expression, Drug resistance, Biology, Downregulation and upregulation, Sirtuin 1, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Gene Regulatory Networks, Gene knockdown, Chemotherapy, Liver Neoplasms, Cancer, medicine.disease, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Mitochondria, Gene Expression Regulation, Neoplastic, Oncology, Mitochondrial biogenesis, colon cancer, Drug Resistance, Neoplasm, Immunology, Colonic Neoplasms, Cancer research, Energy Metabolism, Oxidation-Reduction, Transcription Factors
Abstract

Purpose: Chemotherapy treatment of metastatic colon cancer ultimately fails due to development of drug resistance. Identification of chemotherapy-induced changes in tumor biology may provide insight into drug resistance mechanisms. Experimental Design: We studied gene expression differences between groups of liver metastases that were exposed to preoperative chemotherapy or not. Multiple patient-derived colonosphere cultures were used to assess how chemotherapy alters energy metabolism by measuring mitochondrial biomass, oxygen consumption, and lactate production. Genetically manipulated colonosphere-initiated tumors were used to assess how altered energy metabolism affects chemotherapy efficacy. Results: Gene ontology and pathway enrichment analysis revealed significant upregulation of genes involved in oxidative phosphorylation (OXPHOS) and mitochondrial biogenesis in metastases that were exposed to chemotherapy. This suggested chemotherapy induces a shift in tumor metabolism from glycolysis towards OXPHOS. Indeed, chemotreatment of patient-derived colonosphere cultures resulted in an increase of mitochondrial biomass, increased expression of respiratory chain enzymes, and higher rates of oxygen consumption. This was mediated by the histone deacetylase sirtuin-1 (SIRT1) and its substrate, the transcriptional coactivator PGC1α. Knockdown of SIRT1 or PGC1α prevented chemotherapy-induced OXPHOS and significantly sensitized patient-derived colonospheres as well as tumor xenografts to chemotherapy. Conclusions: Chemotherapy of colorectal tumors induces a SIRT1/PGC1α-dependent increase in OXPHOS that promotes tumor survival during treatment. This phenomenon is also observed in chemotherapy-exposed resected liver metastases, strongly suggesting that chemotherapy induces long-lasting changes in tumor metabolism that potentially interfere with drug efficacy. In conclusion, we propose a novel mechanism of chemotherapy resistance that may be clinically relevant and therapeutically exploitable. Clin Cancer Res; 21(12); 2870–9. ©2015 AACR.

Published
2015

36. Maintenance of Clonogenic KIT(+) Human Colon Tumor Cells Requires Secretion of Stem Cell Factor by Differentiated Tumor Cells

Author

Klaas M. Govaert, Danielle A.E. Raats, Susanne J. van Schelven, Inne H.M. Borel Rinkes, Inge Ubink, Jan Koster, Andre Verheem, Onno Kranenburg, Szabolcs Fatrai, Amsterdam Gastroenterology Endocrinology Metabolism, Cancer Center Amsterdam, and Oncogenomics

Subjects
Epithelial-Mesenchymal Transition, Time Factors, Cellular differentiation, Mice, Nude, Stem cell factor, Tumor initiation, Biology, Research Support, Paracrine signalling, Spheroids, Cellular, Niche, Paracrine Communication, Journal Article, Biomarkers, Tumor, Tumor Cells, Cultured, Animals, Humans, Epithelial–mesenchymal transition, Non-U.S. Gov't, Clonogenic assay, Protein Kinase Inhibitors, Colorectal, Cell Proliferation, Medicine(all), Stem Cell Factor, Hepatology, Research Support, Non-U.S. Gov't, Gastroenterology, Cell Differentiation, Colon Cancer Model, Molecular biology, Cell Hypoxia, Coculture Techniques, Tumor Burden, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-kit, Tumor progression, Colonic Neoplasms, Cancer cell, Tumor Progression, Neoplastic Stem Cells, Cancer research, Signal Transduction
Abstract

Background & Aims Colon tumors contain a fraction of undifferentiated stem cell−like cancer cells with high tumorigenic potential. Little is known about the signals that maintain these stem-like cells. We investigated whether differentiated tumor cells provide support. Methods We established undifferentiated colonosphere cultures from human colon tumors and used them to generate stably differentiated cell lines. Antibody arrays were used to identify secreted factors. Expression of genes involved in stemness, differentiation, and the epithelial to mesenchymal transition was measured using reverse transcription quantitative polymerase chain reaction. Expression of KIT in human tumors was analyzed with gene expression arrays and by immunohistochemistry. Colonospheres were injected into the livers of CBy.Cg-Foxn1nu/J mice. After liver tumors had formed, hypoxia was induced by vascular clamping. Results Differentiated cells from various tumors, or medium conditioned by them, increased the clonogenic capacity of colonospheres. Stem cell factor (SCF) was secreted by differentiated tumor cells and supported the clonogenic capacity of KIT + colonosphere cells. Differentiated tumor cells induced the epithelial to mesenchymal transition in colonosperes; this was prevented by inhibition of KIT or SCF. SCF prevented loss of clonogenic potential under differentiation-inducing conditions. Suppression of SCF or KIT signaling greatly reduced the expression of genes that regulate stemness and the epithelial to mesenchymal transition and inhibited clonogenicity and tumor initiation. Bioinformatic and immunohistochemical analyses revealed a correlation between expression of KIT- and hypoxia-related genes in colon tumors, which was highest in relapse-prone mesenchymal-type tumors. Hypoxia induced expression of KIT in cultured cells and in human colon tumor xenografts and this contributed to the clonogenic capacity of the tumor cells. Conclusions Paracrine signaling from SCF to KIT, between differentiated tumor cells and undifferentiated stem-like tumor cells, helps maintain the stem-like features of tumor cells, predominantly under conditions of hypoxia.

Published
2015

37. Impact of Global Fxr Deficiency on Experimental Acute Pancreatitis and Genetic Variation in the FXR Locus in Human Acute Pancreatitis

Author

Nijmeijer, Rian M, Schaap, Frank G, Smits, Alexander J J, Kremer, Andreas E, Akkermans, Louis M A, Kroese, A.B., Rijkers, Ger T, Schipper, Marguerite E I, Verheem, André, Wijmenga, Cisca, Gooszen, Hein G, van Erpecum, Karel J, Dep IRAS, Sub IRAS Tox CMT/NTX, Risk Assessment of Toxic and Immunomodulatory Agents, IRAS RATIA1, Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Surgery, RS: NUTRIM - R2 - Gut-liver homeostasis, Other departments, Dep IRAS, Sub IRAS Tox CMT/NTX, Risk Assessment of Toxic and Immunomodulatory Agents, and IRAS RATIA1

Subjects
Male, Gene Expression, Receptors, Cytoplasmic and Nuclear, Tumours of the digestive tract Radboud Institute for Health Sciences [Radboudumc 14], Gene Knockout Techniques, Medizinische Fakultät, GROWTH-FACTOR 19, Medicine and Health Sciences, Electric Impedance, Intestinal Mucosa, Receptor, Mice, Knockout, Multidisciplinary, Pancreatitis, Acute Necrotizing, EXOCRINE PANCREAS, Animal Models, NUCLEAR RECEPTOR FXR, INTESTINAL BARRIER DYSFUNCTION, Acute pancreatitis, Medicine, medicine.symptom, Anatomy, ORGAN FAILURE, Research Article, EXPRESSION, medicine.medical_specialty, Science, Inflammation, Endocrine System, Mouse Models, Gastroenterology and Hepatology, Biology, BINDING PROTEIN, Research and Analysis Methods, Polymorphism, Single Nucleotide, Model Organisms, Ileum, Internal medicine, medicine, Genetics, Animals, Humans, ddc:610, Pancreas, Genetic Association Studies, FGF15, Biology and Life Sciences, FGF19, Human Genetics, medicine.disease, Fibroblast Growth Factors, Mice, Inbred C57BL, MICE, Endocrinology, GALLSTONE DISEASE, Nuclear receptor, Pancreatitis, Case-Control Studies, Genetics of Disease, BILE, Farnesoid X receptor, Gene Function
Abstract

Contains fulltext : 170664.PDF (Publisher’s version ) (Open Access) BACKGROUND: Infectious complications often occur in acute pancreatitis, related to impaired intestinal barrier function, with prolonged disease course and even mortality as a result. The bile salt nuclear receptor farnesoid X receptor (FXR), which is expressed in the ileum, liver and other organs including the pancreas, exhibits anti-inflammatory effects by inhibiting NF-kappaB activation and is implicated in maintaining intestinal barrier integrity and preventing bacterial overgrowth and translocation. Here we explore, with the aid of complementary animal and human experiments, the potential role of FXR in acute pancreatitis. METHODS: Experimental acute pancreatitis was induced using the CCK-analogue cerulein in wild-type and Fxr-/- mice. Severity of acute pancreatitis was assessed using histology and a semi-quantitative scoring system. Ileal permeability was analyzed in vitro by Ussing chambers and an in vivo permeability assay. Gene expression of Fxr and Fxr target genes was studied by quantitative RT-PCR. Serum FGF19 levels were determined by ELISA in acute pancreatitis patients and healthy volunteers. A genetic association study in 387 acute pancreatitis patients and 853 controls was performed using 9 tagging single nucleotide polymorphisms (SNPs) covering the complete FXR gene and two additional functional SNPs. RESULTS: In wild-type mice with acute pancreatitis, ileal transepithelial resistance was reduced and ileal mRNA expression of Fxr target genes Fgf15, SHP, and IBABP was decreased. Nevertheless, Fxr-/- mice did not exhibit a more severe acute pancreatitis than wild-type mice. In patients with acute pancreatitis, FGF19 levels were lower than in controls. However, there were no associations of FXR SNPs or haplotypes with susceptibility to acute pancreatitis, or its course, outcome or etiology. CONCLUSION: We found no evidence for a major role of FXR in acute human or murine pancreatitis. The observed altered Fxr activity during the course of disease may be a secondary phenomenon.

Published
2014

38. Planning in tiers? Tiering as a way of linking SEA and EIA

Author

Arts, Jos, Tomlinson, Paul, Voogd, Henk, Sadler, Barry, Dusik, Jiri, Fischer, Thomas, Partidario, Maria, Verheem, Rob, Aschemann, Ralf, and Urban and Regional Studies Institute

Abstract

The idea of tiering can be considered as one of the major drivers for the development of strategic environmental assessment (SEA) (see, for example, Thérivel et al, 1992; UNECE, 1992; Wood and Djeddour, 1992; The rivel and Partidário, 1996; Sadler and Verheem, 1996; Partidário, 1999; Fischer, 2002a; Wood, 2003). Many decisions that have a bearing on environmental quality are taken at a higher level of decision-making than the project level. As Partidário (1999, p60) indicates: ‘The reasons [for SEA] are various but initially related to the timing of project [environmental impact assessment] EIA, i.e. it enters the decision-making process at too late a stage to be able the final decision in a satisfactory way.’ Tiering means that, by preparing a sequence of environmental assessments (EAs) at different planning levels and linking them, foreclosure may be prevented, postponement of detailed issues may be permitted and assessments can be better scoped. A tiered approach minimizes the problem of EIA being only a ‘snapshot in time’. Accordingly, the European SEADirective (2001/42/EC) explicitly assumes tiering of SEAs and EIAs at different planning levels and the SEA and EIA Directives are directly linked.

Published
2012

39. From formulation to implementation: Strengthening SEA through follow-up

Author

Cherp, Aleh, Partidário, Maria R., Arts, Jos, Sadler, Barry, Dusik, Jiri, Fischer, Thomas, Partidario, Maria, Verheem, Rob, Aschemann, Ralf, and Urban and Regional Studies Institute

Abstract

This chapter deals with strategic environmental assessment (SEA) follow-up, which we define as: Monitoring and evaluation of the implementation of a strategic initiative and relevant environmental factors for management of, and communication about, the environmental performance of that strategic initiative.

Published
2012

40. Sea and water management

Author

Huntjens, Patrick, Sadler, Barry, Dusik, Jiri, Fischer, Thomas, Partidario, Maria, Verheem, Rob, Aschemann, Ralf, RS: GSBE MSI, and Maastricht Sustainability Institute

Abstract

Water management is one the world’s most pressing issues. Major regions and subcontinents have serious problems of water shortage, flooding and pollution that present serious risks to people and wetland ecosystems that provide invaluable services. Technical solutions to water management are often difficult to implement cost-effectively for many reasons, including the scale and inter-jurisdictional complexity of water systems and their multiple uses, many of which conflict, impeding cooperation and cost-sharing. In some cases, there is also skewed interdependency, for example, where upstream jurisdictions control the water on which downstream jurisdictions depend or undertake major developments that have adverse downstream impacts.

Published
2010

43. Modification of intestinal flora with multispecies probiotics reduces bacterial translocation and improves clinical course in a rat model of acute pancreatitis

Author

Sergey R. Konstantinov, Louis M. A. Akkermans, Hauke Smidt, L. Paul van Minnen, Wil Harmsen, Hein G. Gooszen, Maarten R. Visser, Femke Lutgendorff, Ger T. Rijkers, Andre Verheem, and Harro M. Timmerman

Subjects
Male, medicine.medical_specialty, Necrosis, Pancreatic disease, complications, Duodenum, medicine.drug_class, Antibiotics, Placebo, Gastroenterology, Microbiology, law.invention, acute necrotizing pancreatitis, necrosis, Rats, Sprague-Dawley, Probiotic, law, Microbiologie, Internal medicine, medicine, Animals, Bifidobacterium, VLAG, biology, Pancreatitis, Acute Necrotizing, business.industry, Probiotics, biology.organism_classification, medicine.disease, mortality, evaluating therapy, infection, Rats, failure, lactobacillus, antibiotic-resistance, Bacterial Translocation, Immunology, Pancreatitis, Acute pancreatitis, Surgery, gastrointestinal-tract, medicine.symptom, business
Abstract

Infection of pancreatic necrosis by gut bacteria is a major cause of morbidity and mortality in patients with severe acute pancreatitis. Use of prophylactic antibiotics remains controversial. The aim of this experiment was assess if modification of intestinal flora with specifically designed multispecies probiotics reduces bacterial translocation or improves outcome in a rat model of acute pancreatitis. METHODS: Male Sprague-Dawley rats were allocated into 3 groups: (1) controls (sham-operated, no treatment), (2) pancreatitis and placebo, and (3) pancreatitis and probiotics. Acute pancreatitis was induced by intraductal glycodeoxycholate and intravenous cerulein infusion. Daily probiotics or placebo was administered intragastrically from 5 days prior until 7 days after induction of pancreatitis. Tissue and fluid samples were collected for microbiologic and quantitative real-time PCR analysis of bacterial translocation. RESULTS: Probiotics reduced duodenal bacterial overgrowth of potential pathogens (Log(10) colony-forming units [CFU]/g 5.0 +/- 0.7 [placebo] vs 3.5 +/- 0.3 CFU/g [probiotics], P

Published
2007

44. Prophylactic probiotics reduce bacterial translocation and improve outcome in experimental pancreatitis

Author

A. Verheem, Ger T. Rijkers, W. Harmsen, Hein G. Gooszen, Hauke Smidt, Lma Akkermans, Sergey R. Konstantinov, Maarten R. Visser, Femke Lutgendorff, Harro M. Timmerman, and L. P. van Minnen

Subjects
Hepatology, Endocrinology, Diabetes and Metabolism, Biology, Bacterial translocation, Bioinformatics, medicine.disease, Microbiology, Endocrinology, Microbiologie, Immunology, Internal Medicine, medicine, Pancreatitis, Life Science, VLAG
Published
2006

47. Bacterial overgrowth and translocation in an experimental pancreatitis model.

Author

van Felius, I., Bosscha, K., Verheem, A., Harmsen, W., Visser, M., van Dijk, J., van de Gaag, I., Gooszen, H., and Akkermans, L.

Subjects
BACTERIAL growth, PANCREATITIS
Abstract

Presents an abstract of the article 'Bacterial Overgrowth and Translocation in an Experimental Pancreatitis Model,' by I. van Felius, K. Bosscha, A. Verheem, W. Harmsen, M. Visser, J. van Dijk, I. van de Gaag, H. Gooszen and L. Akkermans presented to the joint meeting of the Surgical Infection Society of Europe and the European Shock Society held in Nijmegen, Netherlands on May 2000.

Published
2000
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