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1. The deubiquitinase USP9X suppresses pancreatic ductal adenocarcinoma

Author

Perez-Mancera, P, Rust, AG, van der Weyden, L, Kristiansen, GO, Li, A, Sarver, AL, Silverstein, KAT, Grutzmann, R, Aust, DE, Rummele, P, Knosel, T, Herd, C, Stemple, D, Kettleborough, R, Brosnan, JA, Richard, GM, Knight, S, Yu, J, Stegeman, S, Collier, LS, Ten Hoeve, JJ, De Ridder, J, Klein, A, Goggins, M, Hruban, R, Chang, D, Biankin, AV, Pinese, M, Grimmond, S, Wessels, L, Wood, S, Iacobuzio-donahue, CA, Pilarsky, CP, Largaespada, DA, Adams, DJ, Tuveson, DA, Perez-Mancera, P, Rust, AG, van der Weyden, L, Kristiansen, GO, Li, A, Sarver, AL, Silverstein, KAT, Grutzmann, R, Aust, DE, Rummele, P, Knosel, T, Herd, C, Stemple, D, Kettleborough, R, Brosnan, JA, Richard, GM, Knight, S, Yu, J, Stegeman, S, Collier, LS, Ten Hoeve, JJ, De Ridder, J, Klein, A, Goggins, M, Hruban, R, Chang, D, Biankin, AV, Pinese, M, Grimmond, S, Wessels, L, Wood, S, Iacobuzio-donahue, CA, Pilarsky, CP, Largaespada, DA, Adams, DJ, and Tuveson, DA

Abstract

Pancreatic ductal adenocarcinoma (PDA) remains a lethal malignancy despite much progress concerning its molecular characterization. PDA tumours harbour four signature somatic mutations1, 2, 3, 4 in addition to numerous lower frequency genetic events of uncertain significance5. Here we use Sleeping Beauty (SB) transposon-mediated insertional mutagenesis6, 7 in a mouse model of pancreatic ductal preneoplasia8 to identify genes that cooperate with oncogenic KrasG12D to accelerate tumorigenesis and promote progression. Our screen revealed new candidate genes for PDA and confirmed the importance of many genes and pathways previously implicated in human PDA. The most commonly mutated gene was the X-linked deubiquitinase Usp9x, which was inactivated in over 50% of the tumours. Although previous work had attributed a pro-survival role to USP9X in human neoplasia9, we found instead that loss of Usp9x enhances transformation and protects pancreatic cancer cells from anoikis. Clinically, low USP9X protein and messenger RNA expression in PDA correlates with poor survival after surgery, and USP9X levels are inversely associated with metastatic burden in advanced disease. Furthermore, chromatin modulation with trichostatin A or 5-aza-2Œ-deoxycytidine elevates USP9X expression in human PDA cell lines, indicating a clinical approach for certain patients. The conditional deletion of Usp9x cooperated with KrasG12D to accelerate pancreatic tumorigenesis in mice, validating their genetic interaction. We propose that USP9X is a major tumour suppressor gene with prognostic and therapeutic relevance in PDA.

Published
2012

2. The deubiquitinase USP9X suppresses pancreatic ductal adenocarcinoma

Author

Perez-Mancera, PA, Rust, AG, van der Weyden, L, Kristiansen, G, Li, A, Sarver, AL, Silverstein, KAT, Gruetzmann, R, Aust, D, Ruemmele, P, Knoesel, T, Herd, C, Stemple, DL, Kettleborough, R, Brosnan, JA, Morgan, R, Knight, S, Yu, J, Stegeman, S, Collier, LS, ten Hoeve, JJ, de Ridder, J, Klein, AP, Goggins, M, Hruban, RH, Chang, DK, Biankin, AV, Grimmond, SM, Wessels, LFA, Wood, SA, Iacobuzio-Donahue, CA, Pilarsky, C, Largaespada, DA, Adams, DJ, Tuveson, DA, Perez-Mancera, PA, Rust, AG, van der Weyden, L, Kristiansen, G, Li, A, Sarver, AL, Silverstein, KAT, Gruetzmann, R, Aust, D, Ruemmele, P, Knoesel, T, Herd, C, Stemple, DL, Kettleborough, R, Brosnan, JA, Morgan, R, Knight, S, Yu, J, Stegeman, S, Collier, LS, ten Hoeve, JJ, de Ridder, J, Klein, AP, Goggins, M, Hruban, RH, Chang, DK, Biankin, AV, Grimmond, SM, Wessels, LFA, Wood, SA, Iacobuzio-Donahue, CA, Pilarsky, C, Largaespada, DA, Adams, DJ, and Tuveson, DA

Abstract

Pancreatic ductal adenocarcinoma (PDA) remains a lethal malignancy despite much progress concerning its molecular characterization. PDA tumours harbour four signature somatic mutations in addition to numerous lower frequency genetic events of uncertain significance. Here we use Sleeping Beauty (SB) transposon-mediated insertional mutagenesis in a mouse model of pancreatic ductal preneoplasia to identify genes that cooperate with oncogenic Kras(G12D) to accelerate tumorigenesis and promote progression. Our screen revealed new candidate genes for PDA and confirmed the importance of many genes and pathways previously implicated in human PDA. The most commonly mutated gene was the X-linked deubiquitinase Usp9x, which was inactivated in over 50% of the tumours. Although previous work had attributed a pro-survival role to USP9X in human neoplasia, we found instead that loss of Usp9x enhances transformation and protects pancreatic cancer cells from anoikis. Clinically, low USP9X protein and messenger RNA expression in PDA correlates with poor survival after surgery, and USP9X levels are inversely associated with metastatic burden in advanced disease. Furthermore, chromatin modulation with trichostatin A or 5-aza-2'-deoxycytidine elevates USP9X expression in human PDA cell lines, indicating a clinical approach for certain patients. The conditional deletion of Usp9x cooperated with Kras(G12D) to accelerate pancreatic tumorigenesis in mice, validating their genetic interaction. We propose that USP9X is a major tumour suppressor gene with prognostic and therapeutic relevance in PDA.

Published
2012

3. Het Bataafse kniesoor

Author

Bejczy, I.P., Verheesen-Stegeman, S., and Verweij, M.F.

Subjects
Christelijk cultureel erfgoed
Abstract

Item does not contain fulltext 3 p.

Published
2000

5. Th. Janssonius ab Almeloveen, une source importante pour le Dictionnaire

Author

Stegeman, S.

Subjects
Intellectual relations in Western Europe from the Renaissance to the end of the nineteenth century, Intellectuele betrekkingen binnen West-Europa in de Nieuwe Tijd
Abstract

Item does not contain fulltext Internationaal congres Le Dictionnaire de Pierre Bayle, 24-26 oktober 1996, 24 oktober 1996 Nijmegen : [s.n.]

Published
1996

7. Patronage en dienstverlening: het netwerk van Theodorus Janssonius van Almeloveen (1657-1712) in de Republiek der Letteren

Author

Stegeman, S., Radboud University Nijmegen, Bots, J.A.H., and Vet, J.J.V.M. de

Subjects
Intellectual relations in Western Europe from the Renaissance to the end of the nineteenth century, Intellectuele betrekkingen binnen West-Europa in de Nieuwe Tijd
Abstract

Contains fulltext : mmubn000001_237427826.pdf (Publisher’s version ) (Open Access) Promotores : J. Bots en J. de Vet cum laude XI, 412 p.

Published
1996

17. A genetic variant of MDM4 influences regulation by multiple microRNAs in prostate cancer.

Author

Stegeman S, Moya L, Selth LA, Spurdle AB, Clements JA, and Batra J

Subjects
Cell Cycle Proteins, Cell Line, Tumor, Disease Progression, Female, Humans, Male, MicroRNAs metabolism, Nuclear Proteins metabolism, Ovarian Neoplasms genetics, Polymorphism, Single Nucleotide, Prostate metabolism, Prostatic Neoplasms pathology, Proto-Oncogene Proteins metabolism, MicroRNAs genetics, Nuclear Proteins genetics, Prostatic Neoplasms genetics, Proto-Oncogene Proteins genetics
Abstract

The oncogene MDM4, also known as MDMX or HDMX, contributes to cancer susceptibility and progression through its capacity to negatively regulate a range of genes with tumour-suppressive functions. As part of a recent genome-wide association study it was determined that the A-allele of the rs4245739 SNP (A>C), located in the 3'-UTR of MDM4, is associated with an increased risk of prostate cancer. Computational predictions revealed that the rs4245739 SNP is located within a predicted binding site for three microRNAs (miRNAs): miR-191-5p, miR-887 and miR-3669. Herein, we show using reporter gene assays and endogenous MDM4 expression analyses that miR-191-5p and miR-887 have a specific affinity for the rs4245739 SNP C-allele in prostate cancer. These miRNAs do not affect MDM4 mRNA levels, rather they inhibit its translation in C-allele-containing PC3 cells but not in LNCaP cells homozygous for the A-allele. By analysing gene expression datasets from patient cohorts, we found that MDM4 is associated with metastasis and prostate cancer progression and that targeting this gene with miR-191-5p or miR-887 decreases in PC3 cell viability. This study is the first, to our knowledge, to demonstrate regulation of the MDM4 rs4245739 SNP C-allele by two miRNAs in prostate cancer, and thereby to identify a mechanism by which the MDM4 rs4245739 SNP A-allele may be associated with an increased risk for prostate cancer., (© 2015 Society for Endocrinology.)

Published
2015
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18. A Large-Scale Analysis of Genetic Variants within Putative miRNA Binding Sites in Prostate Cancer.

Author

Stegeman S, Amankwah E, Klein K, O'Mara TA, Kim D, Lin HY, Permuth-Wey J, Sellers TA, Srinivasan S, Eeles R, Easton D, Kote-Jarai Z, Amin Al Olama A, Benlloch S, Muir K, Giles GG, Wiklund F, Gronberg H, Haiman CA, Schleutker J, Nordestgaard BG, Travis RC, Neal D, Pharoah P, Khaw KT, Stanford JL, Blot WJ, Thibodeau S, Maier C, Kibel AS, Cybulski C, Cannon-Albright L, Brenner H, Kaneva R, Teixeira MR, Spurdle AB, Clements JA, Park JY, and Batra J

Subjects
3' Untranslated Regions, Adult, Aged, Alleles, Case-Control Studies, Cluster Analysis, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Genotype, Humans, Kallikreins genetics, Kallikreins metabolism, Male, MicroRNAs chemistry, Middle Aged, Neoplasm Grading, Neoplasm Staging, Polymorphism, Single Nucleotide, Prostate-Specific Antigen genetics, Prostate-Specific Antigen metabolism, Prostatic Neoplasms metabolism, Prostatic Neoplasms pathology, Quantitative Trait Loci, R-SNARE Proteins genetics, R-SNARE Proteins metabolism, RNA, Messenger chemistry, Binding Sites, Genetic Variation, MicroRNAs genetics, Prostatic Neoplasms genetics, RNA, Messenger genetics
Abstract

Unlabelled: Prostate cancer is the second most common malignancy among men worldwide. Genome-wide association studies have identified 100 risk variants for prostate cancer, which can explain approximately 33% of the familial risk of the disease. We hypothesized that a comprehensive analysis of genetic variations found within the 3' untranslated region of genes predicted to affect miRNA binding (miRSNP) can identify additional prostate cancer risk variants. We investigated the association between 2,169 miRSNPs and prostate cancer risk in a large-scale analysis of 22,301 cases and 22,320 controls of European ancestry from 23 participating studies. Twenty-two miRSNPs were associated (P<2.3×10(-5)) with risk of prostate cancer, 10 of which were within 7 genes previously not mapped by GWAS studies. Further, using miRNA mimics and reporter gene assays, we showed that miR-3162-5p has specific affinity for the KLK3 rs1058205 miRSNP T-allele, whereas miR-370 has greater affinity for the VAMP8 rs1010 miRSNP A-allele, validating their functional role., Significance: Findings from this large association study suggest that a focus on miRSNPs, including functional evaluation, can identify candidate risk loci below currently accepted statistical levels of genome-wide significance. Studies of miRNAs and their interactions with SNPs could provide further insights into the mechanisms of prostate cancer risk., (©2015 American Association for Cancer Research.)

Published
2015
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19. Loss of Usp9x disrupts cortical architecture, hippocampal development and TGFβ-mediated axonogenesis.

Author

Stegeman S, Jolly LA, Premarathne S, Gecz J, Richards LJ, Mackay-Sim A, and Wood SA

Subjects
Animals, Astrocytes metabolism, Astrocytes pathology, Axons pathology, Central Nervous System metabolism, Doublecortin Protein, Female, Gene Deletion, Genes, Lethal, Hippocampus pathology, Male, Mice, Mice, Knockout, Neurons metabolism, Neurons pathology, Organ Size, Signal Transduction, Ubiquitin Thiolesterase, Axons metabolism, Cerebellar Cortex metabolism, Cerebellar Cortex pathology, Endopeptidases genetics, Hippocampus metabolism, Neurogenesis genetics, Transforming Growth Factor beta metabolism
Abstract

The deubiquitylating enzyme Usp9x is highly expressed in the developing mouse brain, and increased Usp9x expression enhances the self-renewal of neural progenitors in vitro. USP9X is a candidate gene for human neurodevelopmental disorders, including lissencephaly, epilepsy and X-linked intellectual disability. To determine if Usp9x is critical to mammalian brain development we conditionally deleted the gene from neural progenitors, and their subsequent progeny. Mating Usp9x(loxP/loxP) mice with mice expressing Cre recombinase from the Nestin promoter deleted Usp9x throughout the entire brain, and resulted in early postnatal lethality. Although the overall brain architecture was intact, loss of Usp9x disrupted the cellular organization of the ventricular and sub-ventricular zones, and cortical plate. Usp9x absence also led to dramatic reductions in axonal length, in vivo and in vitro, which could in part be explained by a failure in Tgf-β signaling. Deletion of Usp9x from the dorsal telencephalon only, by mating with Emx1-cre mice, was compatible with survival to adulthood but resulted in reduction or loss of the corpus callosum, a dramatic decrease in hippocampal size, and disorganization of the hippocampal CA3 region. This latter phenotypic aspect resembled that observed in Doublecortin knock-out mice, which is an Usp9x interacting protein. This study establishes that Usp9x is critical for several aspects of CNS development, and suggests that its regulation of Tgf-β signaling extends to neurons.

Published
2013
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20. The deubiquitinase USP9X suppresses pancreatic ductal adenocarcinoma.

Author

Pérez-Mancera PA, Rust AG, van der Weyden L, Kristiansen G, Li A, Sarver AL, Silverstein KA, Grützmann R, Aust D, Rümmele P, Knösel T, Herd C, Stemple DL, Kettleborough R, Brosnan JA, Li A, Morgan R, Knight S, Yu J, Stegeman S, Collier LS, ten Hoeve JJ, de Ridder J, Klein AP, Goggins M, Hruban RH, Chang DK, Biankin AV, Grimmond SM, Wessels LF, Wood SA, Iacobuzio-Donahue CA, Pilarsky C, Largaespada DA, Adams DJ, and Tuveson DA

Subjects
Animals, Anoikis genetics, Carcinoma, Pancreatic Ductal genetics, Carcinoma, Pancreatic Ductal pathology, Cell Line, Tumor, Disease Models, Animal, Endopeptidases, Gene Expression Regulation, Neoplastic, Gene Knockdown Techniques, Humans, Mice, Mice, Inbred C57BL, Pancreatic Neoplasms genetics, Pancreatic Neoplasms pathology, U937 Cells, Carcinoma, Pancreatic Ductal enzymology, Pancreatic Neoplasms enzymology, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism
Abstract

Pancreatic ductal adenocarcinoma (PDA) remains a lethal malignancy despite much progress concerning its molecular characterization. PDA tumours harbour four signature somatic mutations in addition to numerous lower frequency genetic events of uncertain significance. Here we use Sleeping Beauty (SB) transposon-mediated insertional mutagenesis in a mouse model of pancreatic ductal preneoplasia to identify genes that cooperate with oncogenic Kras(G12D) to accelerate tumorigenesis and promote progression. Our screen revealed new candidate genes for PDA and confirmed the importance of many genes and pathways previously implicated in human PDA. The most commonly mutated gene was the X-linked deubiquitinase Usp9x, which was inactivated in over 50% of the tumours. Although previous work had attributed a pro-survival role to USP9X in human neoplasia, we found instead that loss of Usp9x enhances transformation and protects pancreatic cancer cells from anoikis. Clinically, low USP9X protein and messenger RNA expression in PDA correlates with poor survival after surgery, and USP9X levels are inversely associated with metastatic burden in advanced disease. Furthermore, chromatin modulation with trichostatin A or 5-aza-2'-deoxycytidine elevates USP9X expression in human PDA cell lines, indicating a clinical approach for certain patients. The conditional deletion of Usp9x cooperated with Kras(G12D) to accelerate pancreatic tumorigenesis in mice, validating their genetic interaction. We propose that USP9X is a major tumour suppressor gene with prognostic and therapeutic relevance in PDA.

Published
2012
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21. Human endometrial stromal stem cells differentiate into megakaryocytes with the ability to produce functional platelets.

Author

Wang J, Chen S, Zhang C, Stegeman S, Pfaff-Amesse T, Zhang Y, Zhang W, Amesse L, and Chen Y

Subjects
Adult, Animals, Blood Platelets drug effects, Blood Platelets metabolism, Blood Platelets ultrastructure, Cell Shape drug effects, Cells, Cultured, Culture Media, Female, Fibrinogen metabolism, Flow Cytometry, Humans, Immunohistochemistry, Megakaryocytes drug effects, Megakaryocytes metabolism, Mice, Middle Aged, Octamer Transcription Factor-3 metabolism, P-Selectin metabolism, Protein Binding drug effects, SOXB1 Transcription Factors metabolism, Stem Cells drug effects, Stromal Cells cytology, Stromal Cells drug effects, Thrombin pharmacology, Blood Platelets cytology, Cell Differentiation drug effects, Endometrium cytology, Megakaryocytes cytology, Stem Cells cytology
Abstract

Human endometrium is a high dynamic tissue that contains endometrial stromal stem cells (hESSCs). The hESSCs have been differentiated into a number of cell lineages. However, differentiation of hESSCs into megakaryocytes (MKs) has not yet been investigated. The aim of this study was to investigate the feasibility of MK generation from hESSCs and subsequent production of functional platelets (PLTs). In our study, hESSCs were cultured from endometrial stromal cells as confirmed by positive stromal cell specific markers (CD90 and CD29) and negative hematopoietic stem cell markers (CD45 and CD34) expression. Then, hESSCs were differentiated in a medium supplemented with thrombopoietin (TPO) for 18 days. The MK differentiation was analyzed by flow cytometry and confocal microscopy. The differentiation medium was collected for PLT production analysis by flow cytometry, transmission electron microscopy and functional measurements. Our results show: 1) MKs were successfully generated from hESSCs as identified by expression of specific markers (CD41a: 1 ± 0.09% and 39 ± 3.0%; CD42b: 1.2 ± 0.06% and 28 ± 2.0%, control vs. differentiation) accompanied with reduction of pluripotent transcription factors (Oct4 and Sox2) expression; 2) The level of PLTs in the differentiation medium was 16 ± 1 number/µl as determined by size (2-4 µm) and CD41a expression (CD41a: 1 ± 0.4% and 90±2.0%, control vs. differentiation); 3) Generated PLTs were functional as evidenced by the up-regulation of CD62p expression and fibrinogen binding following thrombin stimulation; 4) Released PLTs showed similar ultra-structure characteristics (alpha granules, vacuoles and dense tubular system) as PLTs from peripheral blood determined by electron microscopic analysis. Data demonstrate the feasibility of generating MKs from hESSCs, and that the generated MKs release functional PLTs. Therefore, hESSCs could be a potential new stem cell source for in vitro MK/PLT production.

Published
2012
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22. Subchronic, developmental, and genetic toxicology studies with the ethane sulfonate metabolite of alachlor.

Author

Heydens WF, Siglin JC, Holson JF, and Stegeman SD

Subjects
Acetamides chemistry, Animals, Drinking Behavior drug effects, Female, Herbicides chemistry, Male, Mice, Micronucleus Tests, Pregnancy, Rats, Rats, Inbred F344, Acetamides toxicity, Alkanesulfonates chemistry, Herbicides toxicity, Teratogens toxicity
Abstract

The ethane sulfonate (ESA) metabolite of the herbicide alachlor is formed in soil by microbial action. The present studies were conducted to assess the toxicity of ESA and provide a base set of data for risk assessment. ESA did not induce chromosomal effects in a mouse bone marrow micronucleus assay following acute administration. Administration of ESA to rats in drinking water at concentration of 200, 2000, and 10,000 ppm for 91 days elicited biologically significant indications of toxicity only at the high-dose level (1002 mg/kg/day). The observed responses included decreases in body weights and food consumption as well as effects on clinical chemistry values. Many of the changes appeared to be due to decreased palatability of the drinking water. There were no ESA-induced gross pathology findings, organ weight changes, or microscopic lesions. ESA did not produce any adverse effects in pregnant rats or their offspring even at 1000 mg/kg/day, the highest dose tested. These findings show that the subchronic and developmental toxicity of ESA are low. Furthermore, comparison of results from studies with alachlor and its metabolite shows that the toxicity of ESA is substantially lower. Margins of exposure for ESA range from 133,824 to 2,573,529 even using worst-case estimates of exposure, indicating that the metabolite poses little risk of producing adverse effects at the very low levels occasionally encountered. These results and accompanying analyses support the conclusion that ESA is not of toxicological concern.

Published
1996
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23. Microscopically controlled excision of skin tumors.

Author

Tromovitch TA and Stegeman SJ

Subjects
Acetates, Carcinoma, Basal Cell diagnosis, Carcinoma, Basal Cell pathology, Cheek, Ear Neoplasms surgery, Epinephrine administration & dosage, Eye Neoplasms surgery, Eyelid Neoplasms surgery, Facial Neoplasms surgery, Head and Neck Neoplasms surgery, Hemostasis, Injections, Intradermal, Lidocaine administration & dosage, Lip Neoplasms surgery, Microscopy, Neoplasm Recurrence, Local, Nose Neoplasms surgery, Skin Neoplasms diagnosis, Skin Neoplasms pathology, Trichloroacetic Acid, Carcinoma, Basal Cell surgery, Skin Neoplasms surgery
Published
1974

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