Your search keyword '"Antwan G Ederveen"' showing total 11 results

1. Correction: Intestinal Tumorigenesis Is Not Affected by Progesterone Signaling in Rodent Models.

Author

Jarom Heijmans, Vanesa Muncan, Rutger J Jacobs, Eveline S M de Jonge-Muller, Laura Graven, Izak Biemond, Antwan G Ederveen, Patrick G Groothuis, Sietse Mosselman, James C Hardwick, Daniel W Hommes, and Gijs R van den Brink

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0022620.].

Published

2013

2. Intestinal tumorigenesis is not affected by progesterone signaling in rodent models.

Author

Jarom Heijmans, Vanesa Muncan, Rutger J Jacobs, Eveline S M de Jonge-Muller, Laura Graven, Izak Biemond, Antwan G Ederveen, Patrick G Groothuis, Sietse Mosselman, James C Hardwick, Daniel W Hommes, and Gijs R van den Brink

Subjects

Medicine, Science

Abstract

Clinical data suggest that progestins have chemopreventive properties in the development of colorectal cancer. We set out to examine a potential protective effect of progestins and progesterone signaling on colon cancer development. In normal and neoplastic intestinal tissue, we found that the progesterone receptor (PR) is not expressed. Expression was confined to sporadic mesenchymal cells. To analyze the influence of systemic progesterone receptor signaling, we crossed mice that lacked the progesterone receptor (PRKO) to the Apc(Min/+) mouse, a model for spontaneous intestinal polyposis. PRKO-Apc(Min/+) mice exhibited no change in polyp number, size or localization compared to Apc(Min/+). To examine effects of progestins on the intestinal epithelium that are independent of the PR, we treated mice with MPA. We found no effects of either progesterone or MPA on gross intestinal morphology or epithelial proliferation. Also, in rats treated with MPA, injection with the carcinogen azoxymethane did not result in a difference in the number or size of aberrant crypt foci, a surrogate end-point for adenoma development. We conclude that expression of the progesterone receptor is limited to cells in the intestinal mesenchyme. We did not observe any effect of progesterone receptor signaling or of progestin treatment in rodent models of intestinal tumorigenesis.

Published

2011

3. Early Clinical Development Planning via Biomarkers, Clinical Endpoints, and Simulation: A Case Study to Optimize for Phase 3 Dose Selection

Author

Ghassan N. Fayad, Bret J. Musser, Yue Shentu, Nitin Patel, Lori A. Mixson, James Bolognese, Antwan G. Ederveen, and Jaydeep Bhattacharyya

Subjects

Dose finding, business.industry, Sample size determination, Public Health, Environmental and Occupational Health, Clinical endpoint, Biomarker (medicine), Medicine, Pharmacology (medical), Bioinformatics, business, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Prior information, Dose selection

Abstract

This study investigated a framework that leverages the relationship between biomarkers and a target clinical endpoint to optimize an early development plan.Different biomarker designs were assessed for proof of concept (PoC) and dose finding (DF) to improve phase 2b (Ph2b) design as well as phase 3 (Ph3) dose choice. A case study using a Bayesian trivariate normal distribution model for 2 biomarkers and a clinically relevant endpoint was utilized with simulation to assess performance characteristics.We found the following: (1) at typical sample sizes for early development trials, biomarkers appear useful for PoC but not for clinical endpoint DF; and (2) even with large amounts of prior information and near perfect correlation between biomarkers and clinical endpoints, Ph2b variability is only overcome by increased Ph2b sample sizes to improve Ph3 dose choice.For highly variable clinical endpoints, the fastest path should be to demonstrate PoC by biomarkers and then go directly to Ph2b to measure the target clinical endpoint.

Published

2018

4. Discovery and Clinical Evaluation of MK‐8150, A Novel Nitric Oxide Donor With a Unique Mechanism of Nitric Oxide Release

Author

David E. Gutstein, Christopher J. Morabito, Anna Mitselos, Kaushik Mitra, Wen Liu, Peggy H. Wong, Doris F. Cully, Karim Azer, Shu Yu Sun, Clayton D. Knox, Antwan G. Ederveen, Pieter‐Jan de Kam, Michael Man-Chu Lo, Tom Reynders, Alan G. Meehan, Daniel Jonathan, Amjad Ali, Jean Francois Denef, and Diane Shevell

Subjects

0301 basic medicine, Adult, Male, lcsh:Diseases of the circulatory (Cardiovascular) system, medicine.medical_specialty, Adolescent, Vasodilation, 030204 cardiovascular system & hematology, Pharmacology, In Vitro Techniques, Nitric oxide, Kidney Tubules, Proximal, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Dogs, Pharmacokinetics, nitrate, nitric oxide, Clinical Studies, medicine, Animals, Humans, Nitric Oxide Donors, vasodilation, Cyclic GMP, Original Research, Aged, Cardiovascular Surgery, CYP3A4, business.industry, Mechanism (biology), blood pressure, Metabolism, Middle Aged, nitrate tolerance, Surgery, 030104 developmental biology, Blood pressure, Drug development, chemistry, lcsh:RC666-701, Hypertension, Triazenes, Cardiology and Cardiovascular Medicine, business

Abstract

Background Nitric oxide donors are widely used to treat cardiovascular disease, but their major limitation is the development of tolerance, a multifactorial process to which the in vivo release of nitric oxide is thought to contribute. Here we describe the preclinical and clinical results of a translational drug development effort to create a next‐generation nitric oxide donor with improved pharmacokinetic properties and a unique mechanism of nitric oxide release through CYP 3A4 metabolism that was designed to circumvent the development of tolerance. Methods and Results Single‐ and multiple‐dose studies in telemetered dogs showed that MK ‐8150 induced robust blood‐pressure lowering that was sustained over 14 days. The molecule was safe and well tolerated in humans, and single doses reduced systolic blood pressure by 5 to 20 mm Hg in hypertensive patients. Multiple‐dose studies in hypertensive patients showed that the blood‐pressure–lowering effect diminished after 10 days, and 28‐day studies showed that the hemodynamic effects were completely lost by day 28, even when the dose of MK ‐8150 was increased during the dosing period. Conclusions The novel nitric oxide donor MK ‐8150 induced significant blood‐pressure lowering in dogs and humans for up to 14 days. However, despite a unique mechanism of nitric oxide release mediated by CYP 3A4 metabolism, tolerance developed over 28 days, suggesting that tolerance to nitric oxide donors is multifactorial and cannot be overcome solely through altered in vivo release of nitric oxide. Clinical Trial Registration URL : http://www.clinicaltrials.gov . Unique identifiers: NCT 01590810 and NCT 01656408.

Published

2016

5. Oestrogens promote tumorigenesis in a mouse model for colitis-associated cancer

Author

Daniel W. Hommes, Patrick G. Groothuis, Mattheus C. B. Wielenga, Eveline S.M. de Jonge-Muller, James C. H. Hardwick, Joris J. T. H. Roelofs, Gijs R. van den Brink, Izak Biemond, Vanesa Muncan, Antwan G. Ederveen, Sanne L. Rosekrans, Jarom Heijmans, Geert D'Haens, Jooske F. van Lidth de Jeude, Tytgat Institute for Liver and Intestinal Research, Graduate School, Gastroenterology and Hepatology, Amsterdam Cardiovascular Sciences, Amsterdam institute for Infection and Immunity, Pathology, Amsterdam Gastroenterology Endocrinology Metabolism, and Cancer Center Amsterdam

Subjects

Medroxyprogesterone, medicine.medical_specialty, Hormone Replacement Therapy, Colorectal cancer, Carcinogenesis, Ovariectomy, Azoxymethane, Biology, medicine.disease_cause, Mice, Internal medicine, IBD Basic Research, medicine, Animals, Medroxyprogesterone acetate, Hormone replacement therapy, Colitis, Cancer, Estradiol, Dextran Sulfate, Gastroenterology, Estrogens, medicine.disease, Immunohistochemistry, Ulcerative colitis, Disease Models, Animal, Endocrinology, Colonic Neoplasms, Cytokines, Female, medicine.drug, Hormone

Abstract

Background Hormone replacement therapy increases the risk of developing ulcerative colitis in postmenopausal women. Chronic intestinal inflammation predisposes to colon cancer development, but effects of female hormones on colitis-associated cancer development have not been examined. Aim To investigate the role of female hormones in the dextran sodium sulfate (DSS)-azoxymethane (AOM) mouse model for colitis-associated cancer. Design We performed ovariectomies, or sham operations, on mice, and supplemented these animals with indicated hormones. Additionally, we used oestrogen receptor α or β ( Erα or Erβ ) mutant mice. To study colitis or colitis-associated cancer, we used DSS only, or DSS and AOM, respectively. Results Ovariectomy protects female mice against colitis-associated tumour development. Hormone replacement in ovariectomised mice with either oestradiol (E2), medroxyprogesterone acetate or a combination of both suggests that oestrogens are the ovary-derived factor that promotes tumour development in the context of inflammatory damage. E2-treated animals showed increased clinical symptoms and Il-6 production upon DSS-induced colitis and enhanced epithelial proliferation. Treatment with E2 markedly increased the numbers of polyps in ovariectomised mice and also strongly promoted tumour progression with all E2-treated animals developing at least one invasive adenocarcinoma, whereas, placebo-treated animals developed adenomas only. Using Er mutant mice, we find that the protumorigenic effect of oestrogen depends on both Erα and Erβ. Conclusions Our results suggest that oestrogens promote inflammation-associated cancer development by impairing the mucosal response to inflammatory damage.

Published

2014

6. Sex disparity in colonic adenomagenesis involves promotion by male hormones, not protection by female hormones

Author

Kathy J. Krentz, William F. Dove, Alexandra Shedlovsky, Antwan G. Ederveen, Jarom Heijmans, Linda Clipson, Elisa Dunkin, Mattheus C. B. Wielenga, Vanesa Muncan, Daniel W. Hommes, Gijs R. van den Brink, Sietse Mosselman, James M. Amos-Landgraf, Patrick G. Groothuis, Tytgat Institute for Liver and Intestinal Research, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, CCA -Cancer Center Amsterdam, Gastroenterology and Hepatology, and AII - Amsterdam institute for Infection and Immunity

Subjects

Male, chemistry.chemical_compound, Mice, Random Allocation, Sex hormone-binding globulin, Animals, Congenic, Orchiectomy, Gonadal Steroid Hormones, Testosterone, Multidisciplinary, biology, Estradiol, Dihydrotestosterone, Postmenopause, Adenomatous Polyposis Coli, Organ Specificity, Receptors, Androgen, Colonic Neoplasms, Female, medicine.drug, Adenoma, medicine.medical_specialty, Genes, APC, Neoplasms, Hormone-Dependent, Hormone Replacement Therapy, Ovariectomy, Azoxymethane, Medroxyprogesterone Acetate, Rats, Mutant Strains, Species Specificity, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Sex Distribution, business.industry, medicine.disease, Rats, Inbred F344, digestive system diseases, Rats, Mice, Inbred C57BL, Disease Models, Animal, Castration, Endocrinology, chemistry, Mutation, biology.protein, Carcinogens, business, Hormone

Abstract

It recently has been recognized that men develop colonic adenomas and carcinomas at an earlier age and at a higher rate than women. In the Apc(Pirc/+) (Pirc) rat model of early colonic cancer, this sex susceptibility was recapitulated, with male Pirc rats developing twice as many adenomas as females. Analysis of large datasets revealed that the Apc(Min/+) mouse also shows enhanced male susceptibility to adenomagenesis, but only in the colon. In addition, WT mice treated with injections of the carcinogen azoxymethane (AOM) showed increased numbers of colonic adenomas in males. The mechanism underlying these observations was investigated by manipulation of hormonal status. The preponderance of colonic adenomas in the Pirc rat model allowed a statistically significant investigation in vivo of the mechanism of sex hormone action on the development of colonic adenomas. Females depleted of endogenous hormones by ovariectomy did not exhibit a change in prevalence of adenomas, nor was any effect observed with replacement of one or a combination of female hormones. In contrast, depletion of male hormones by orchidectomy (castration) markedly protected the Pirc rat from adenoma development, whereas supplementation with testosterone reversed that effect. These observations were recapitulated in the AOM mouse model. Androgen receptor was undetectable in the colon or adenomas, making it likely that testosterone acts indirectly on the tumor lineage. Our findings suggest that indirect tumor-promoting effects of testosterone likely explain the disparity between the sexes in the development of colonic adenomas.

Published

2014

7. Correction: Intestinal Tumorigenesis Is Not Affected by Progesterone Signaling in Rodent Models

Author

Patrick G. Groothuis, Antwan G. Ederveen, Rutger J. Jacobs, Laura Graven, Izak Biemond, Sietse Mosselman, Jarom Heijmans, Eveline S.M. de Jonge-Muller, Gijs R. van den Brink, Daniel W. Hommes, James C. H. Hardwick, Vanesa Muncan, Graduate School, Amsterdam Gastroenterology Endocrinology Metabolism, Gastroenterology and Hepatology, Cancer Center Amsterdam, and Amsterdam institute for Infection and Immunity

Subjects

Multidisciplinary, Rodent, biology, biology.animal, Immunology, lcsh:R, Cancer research, lcsh:Medicine, lcsh:Q, lcsh:Science, Intestinal tumorigenesis

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0022620.].

Published

2013

8. Intestinal Tumorigenesis Is Not Affected by Progesterone Signaling in Rodent Models

Author

Patrick G. Groothuis, Daniel W. Hommes, Rutger J. Jacobs, Gijs R. van den Brink, Sietse Mosselman, Jarom Heijmans, James C. H. Hardwick, Izak Biemond, Vanesa Muncan, Laura Graven, Antwan G. Ederveen, Eveline S.M. de Jonge-Muller, Luk, John, Tytgat Institute for Liver and Intestinal Research, Amsterdam Gastroenterology Endocrinology Metabolism, Cancer Center Amsterdam, Gastroenterology and Hepatology, Amsterdam institute for Infection and Immunity, and Faculteit der Geneeskunde

Subjects

Mouse, estrogen plus progestin colon-cancer medroxyprogesterone acetate colorectal-cancer postmenopausal women tumor progression receptor knockout mammary-gland mouse models mice, lcsh:Medicine, Small, Cell Transformation, chemistry.chemical_compound, Mice, Intestinal mucosa, Receptors, Gastrointestinal Cancers, Basic Cancer Research, Intestine, Small, Intestinal Mucosa, lcsh:Science, Progesterone, Cancer, Multidisciplinary, Intestinal Polyposis, Animal Models, Intestinal epithelium, Immunohistochemistry, Intestine, Colo-Rectal Cancer, medicine.anatomical_structure, Cell Transformation, Neoplastic, Oncology, Medicine, Signal transduction, Receptors, Progesterone, Aberrant crypt foci, Research Article, Signal Transduction, medicine.medical_specialty, General Science & Technology, medicine.drug_class, Colon, Mesenchyme, Gastroenterology and Hepatology, Biology, Model Organisms, Internal medicine, Progesterone receptor, Intestinal Neoplasms, medicine, Animals, Cell Proliferation, Neoplastic, Animal, Azoxymethane, Prevention, lcsh:R, Correction, Rats, Disease Models, Animal, Endocrinology, chemistry, Disease Models, lcsh:Q, Progestins, Digestive Diseases, Progestin

Abstract

Clinical data suggest that progestins have chemopreventive properties in the development of colorectal cancer. We set out to examine a potential protective effect of progestins and progesterone signaling on colon cancer development. In normal and neoplastic intestinal tissue, we found that the progesterone receptor (PR) is not expressed. Expression was confined to sporadic mesenchymal cells. To analyze the influence of systemic progesterone receptor signaling, we crossed mice that lacked the progesterone receptor (PRKO) to the Apc(Min/+) mouse, a model for spontaneous intestinal polyposis. PRKO-Apc(Min/+) mice exhibited no change in polyp number, size or localization compared to Apc(Min/+). To examine effects of progestins on the intestinal epithelium that are independent of the PR, we treated mice with MPA. We found no effects of either progesterone or MPA on gross intestinal morphology or epithelial proliferation. Also, in rats treated with MPA, injection with the carcinogen azoxymethane did not result in a difference in the number or size of aberrant crypt foci, a surrogate end-point for adenoma development. We conclude that expression of the progesterone receptor is limited to cells in the intestinal mesenchyme. We did not observe any effect of progesterone receptor signaling or of progestin treatment in rodent models of intestinal tumorigenesis.

Published

2011

9. Olfactomedin-4 Regulation by Estrogen in the Human Endometrium Requires Epidermal Growth Factor Signaling

Author

Anton F.P.M. de Goeij, Gerard A.J. Dunselman, Patrick G. Groothuis, Antwan G. Ederveen, Andrea Romano, Claudia Marchetti, Cleophas M. Kyama, Jan P. G. Klomp, Rick Kamps, Hellen Dassen, Iris A. Schulkens, Bert Delvoux, Thomas D'Hooghe, Fred Dijcks, Chamindie Punyadeera, Ondersteunend personeel CD, Obstetrie & Gynaecologie, MUMC+: MA Medische Staf Obstetrie Gynaecologie (9), Genetica & Celbiologie, Pathologie, and RS: GROW - School for Oncology and Reproduction

Subjects

Endometriosis, Apoptosis, Vimentin, Endometrium, Epidermal growth factor, Granulocyte Colony-Stimulating Factor, 80 and over, Promoter Regions, Genetic, Adult, Aged, Aged, 80 and over, Cell Adhesion, Cells, Cultured, Endometrial Neoplasms, Epidermal Growth Factor, Estrogens, Female, Humans, Menstrual Cycle, Middle Aged, Receptor, Epidermal Growth Factor, Signal Transduction, Tumor Suppressor Proteins, 2734, Cultured, ErbB Receptors, medicine.anatomical_structure, endometrial cancer, Trefoil Factor-1, Signal transduction, Receptor, medicine.medical_specialty, medicine.drug_class, Cells, Biology, Pathology and Forensic Medicine, Promoter Regions, Genetic, Internal medicine, medicine, Settore MED/06 - ONCOLOGIA MEDICA, Endometrial cancer, Cancer, medicine.disease, Endocrinology, Settore MED/40 - GINECOLOGIA E OSTETRICIA, Estrogen, Cancer research, biology.protein, Regular Articles

Abstract

Olfactomedin-4 (OLFM-4) is an extracellular matrix protein that is highly expressed in human endometrium. We have examined the regulation and function of OLFM-4 in normal endometrium and in cases of endometriosis and endometrial cancer. OLFM-4 expression levels are highest in proliferative-phase endometrium, and 17 beta-estradiol up-regulates OLFM-4 mRNA in endometrial explant cultures. Using the luciferase reporter under control of the OLFM-4 promoter, it was shown that both 17 beta-estradiol and OH-tamoxifen induce luciferase activity, and epidermal growth factor receptor-1 is required for this estrogenic response. In turn, EGF activates the OLFM-4 promoter, and estrogen receptor-alpha is needed for the complete EGF response. The cellular functions of OLFM-4 were examined by its expression in OLFM-4-negative HEK-293 cells, which resulted in decreased vimentin expression and cell adherence as well as increased apoptosis resistance. In cases of endometriosis and endometrial cancer, OLFM-4 expression correlated with the presence of epidermal growth factor receptor-1 and estrogen receptor-alpha (or estrogen signaling). An increase of OLFM-4 mRNA was observed in the endometrium of endometriosis patients. No change in OLFM-4 expression levels were observed in patients with endometrial cancer relative with controts. In conclusion, cross-talk between estrogen and EGF signaling regulates OLFM-4 expression. The role of OLFM-4 in endometrial tissue remodeling before the secretory phase and during the predisposition and early events in endometriosis can be postulated but requires additional investigation. (Am J Pathol 2010, 177:2495-2508: DOI: 10.2353/ajpath.2010.100026

Published

2010

10. Sa1676 Estrogens Promote Development of Colitis-Associated Cancer

Author

Izak Biemond, Sanne L. Rosekrans, Jarom Heijmans, Mattheus C. B. Wielenga, Daniel W. Hommes, Antwan G. Ederveen, Joris J. T. H. Roelofs, James C. H. Hardwick, Vanesa Muncan, Gijs R. van den Brink, Eveline S. de Jonge Muller, Patrick G. Groothuis, and Jooske F. van Lidth de Jeude

Subjects

Hepatology, business.industry, Gastroenterology, Cancer research, Medicine, Colitis associated cancer, business

Published

2013

11. Discovery and Clinical Evaluation of MK‐8150, A Novel Nitric Oxide Donor With a Unique Mechanism of Nitric Oxide Release

Author

Clayton D. Knox, Pieter‐Jan deKam, Karim Azer, Peggy Wong, Antwan G. Ederveen, Diane Shevell, Christopher Morabito, Alan G. Meehan, Wen Liu, Tom Reynders, Jean Francois Denef, Anna Mitselos, Daniel Jonathan, David E. Gutstein, Kaushik Mitra, Shu Yu Sun, Michael Man‐Chu Lo, Doris Cully, and Amjad Ali

Subjects

blood pressure, nitrate, nitrate tolerance, nitric oxide, vasodilation, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background Nitric oxide donors are widely used to treat cardiovascular disease, but their major limitation is the development of tolerance, a multifactorial process to which the in vivo release of nitric oxide is thought to contribute. Here we describe the preclinical and clinical results of a translational drug development effort to create a next‐generation nitric oxide donor with improved pharmacokinetic properties and a unique mechanism of nitric oxide release through CYP3A4 metabolism that was designed to circumvent the development of tolerance. Methods and Results Single‐ and multiple‐dose studies in telemetered dogs showed that MK‐8150 induced robust blood‐pressure lowering that was sustained over 14 days. The molecule was safe and well tolerated in humans, and single doses reduced systolic blood pressure by 5 to 20 mm Hg in hypertensive patients. Multiple‐dose studies in hypertensive patients showed that the blood‐pressure–lowering effect diminished after 10 days, and 28‐day studies showed that the hemodynamic effects were completely lost by day 28, even when the dose of MK‐8150 was increased during the dosing period. Conclusions The novel nitric oxide donor MK‐8150 induced significant blood‐pressure lowering in dogs and humans for up to 14 days. However, despite a unique mechanism of nitric oxide release mediated by CYP3A4 metabolism, tolerance developed over 28 days, suggesting that tolerance to nitric oxide donors is multifactorial and cannot be overcome solely through altered in vivo release of nitric oxide. Clinical Trial Registration URL: http://www.clinicaltrials.gov. Unique identifiers: NCT01590810 and NCT01656408.

Published

2016