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13 results on '"Westerman, B.A."'

1. Radio-sensitizing effect of MEK inhibition in glioblastoma in vitro and in vivo.

Author

Houweling, M., Abdul, U.K., Brahm, C., Lagerweij, T., Heukelom, S., Koken, P.W., Honeywell, R., Wedekind, L.E., Peters, G.J., Verheul, H.M.W., Sminia, P., Noske, D., Wurdinger, T., Westerman, B.A., Houweling, M., Abdul, U.K., Brahm, C., Lagerweij, T., Heukelom, S., Koken, P.W., Honeywell, R., Wedekind, L.E., Peters, G.J., Verheul, H.M.W., Sminia, P., Noske, D., Wurdinger, T., and Westerman, B.A.

Abstract

01 januari 2023, Item does not contain fulltext, INTRODUCTION: Glioblastoma (GBM) is an incurable cancer type. New therapeutic options are investigated, including targeting the mitogen-activated protein kinase (MAPK) pathway using MEK inhibitors as radio-sensitizers. In this study, we investigated whether MEK inhibition via PD0325901 leads to radio-sensitization in experimental in vitro and in vivo models of GBM. MATERIALS AND METHODS: In vitro, GBM8 multicellular spheroids were irradiated with 3 fractions of 2 Gy, during 5 consecutive days of incubation with either PD0325901 or MEK-162. In vivo, we combined PD0325901 with radiotherapy in the GBM8 orthotopic mouse model, tumor growth was measured weekly by bioluminescence imaging and overall survival and toxicity were assessed. RESULTS: Regrowth and viability of spheroids monitored until day 18, showed that both MEK inhibitors had an in vitro radio-sensitizing effect. In vivo, PD0325901 concentrations were relatively constant throughout multiple brain areas and temporal PD0325901-related adverse events such as dermatitis were observed in 4 out of 14 mice (29%). Mice that were treated with radiation alone or combined with PD0325901 had significantly better survival compared to vehicle (both P < 0.005), however, no significant interaction between PD0325901 MEK inhibition and irradiation was observed. CONCLUSION: The difference between the radiotherapy-enhancing effect of PD0325901 in vitro and in vivo urges further pharmacodynamic/pharmacokinetic investigation of PD0325901 and possibly other candidate MEK inhibitors.

Published
2023

2. CXCR4 expression in glioblastoma tissue and the potential for PET imaging and treatment with [(68)Ga]Ga-Pentixafor /[(177)Lu]Lu-Pentixather

Author

Jacobs, S.M., Wesseling, P., Keizer, B. de, Tolboom, N., Ververs, F.F.T., Krijger, G.C., Westerman, B.A., Snijders, T.J., Robe, P.A.J.T., Kolk, A.G. van der, Jacobs, S.M., Wesseling, P., Keizer, B. de, Tolboom, N., Ververs, F.F.T., Krijger, G.C., Westerman, B.A., Snijders, T.J., Robe, P.A.J.T., and Kolk, A.G. van der

Abstract

Item does not contain fulltext, PURPOSE: CXCR4 (over)expression is found in multiple human cancer types, while expression is low or absent in healthy tissue. In glioblastoma it is associated with a poor prognosis and more extensive infiltrative phenotype. CXCR4 can be targeted by the diagnostic PET agent [(68)Ga]Ga-Pentixafor and its therapeutic counterpart [(177)Lu]Lu-Pentixather. We aimed to investigate the expression of CXCR4 in glioblastoma tissue to further examine the potential of these PET agents. METHODS: CXCR4 mRNA expression was examined using the R2 genomics platform. Glioblastoma tissue cores were stained for CXCR4. CXCR4 staining in tumor cells was scored. Stained tissue components (cytoplasm and/or nuclei of the tumor cells and blood vessels) were documented. Clinical characteristics and information on IDH and MGMT promoter methylation status were collected. Seven pilot patients with recurrent glioblastoma underwent [(68)Ga]Ga-Pentixafor PET; residual resected tissue was stained for CXCR4. RESULTS: Two large mRNA datasets (N = 284; N = 540) were assesed. Of the 191 glioblastomas, 426 cores were analyzed using immunohistochemistry. Seventy-eight cores (23 tumors) were CXCR4 negative, while 18 cores (5 tumors) had both strong and extensive staining. The remaining 330 cores (163 tumors) showed a large inter- and intra-tumor variation for CXCR4 expression; also seen in the resected tissue of the seven pilot patients-not directly translatable to [(68)Ga]Ga-Pentixafor PET results. Both mRNA and immunohistochemical analysis showed CXCR4 negative normal brain tissue and no significant correlation between CXCR4 expression and IDH or MGMT status or survival. CONCLUSION: Using immunohistochemistry, high CXCR4 expression was found in a subset of glioblastomas as well as a large inter- and intra-tumor variation. Caution should be exercised in directly translating ex vivo CXCR4 expression to PET agent uptake. However, when high CXCR4 expression can be identified with [(68)Ga]Ga-Pentixafor, these p

Published
2022

3. p120-catenin-dependent collective brain infiltration by glioma cell networks

Author

Grytsenko, P., Atlasy, N., Dieteren, C.E.J., Navis, A.C., Venhuizen, J.H., Veelken, C.A., Schubert, D., Acker-Palmer, A., Westerman, B.A., Wurdinger, T., Leenders, W.P., Wesseling, P., Stunnenberg, H.G., Friedl, P., Grytsenko, P., Atlasy, N., Dieteren, C.E.J., Navis, A.C., Venhuizen, J.H., Veelken, C.A., Schubert, D., Acker-Palmer, A., Westerman, B.A., Wurdinger, T., Leenders, W.P., Wesseling, P., Stunnenberg, H.G., and Friedl, P.

Abstract

Contains fulltext : 220594.pdf (publisher's version ) (Closed access), Diffuse brain infiltration by glioma cells causes detrimental disease progression, but its multicellular coordination is poorly understood. We show here that glioma cells infiltrate the brain collectively as multicellular networks. Contacts between moving glioma cells are adaptive epithelial-like or filamentous junctions stabilized by N-cadherin, β-catenin and p120-catenin, which undergo kinetic turnover, transmit intercellular calcium transients and mediate directional persistence. Downregulation of p120-catenin compromises cell-cell interaction and communication, disrupts collective networks, and both the cadherin and RhoA binding domains of p120-catenin are required for network formation and migration. Deregulating p120-catenin further prevents diffuse glioma cell infiltration of the mouse brain with marginalized microlesions as the outcome. Transcriptomics analysis has identified p120-catenin as an upstream regulator of neurogenesis and cell cycle pathways and a predictor of poor clinical outcome in glioma patients. Collective glioma networks infiltrating the brain thus depend on adherens junctions dynamics, the targeting of which may offer an unanticipated strategy to halt glioma progression.

Published
2020

4. Data-driven prioritization and preclinical evaluation of therapeutic targets in glioblastoma

Author

Brahm, C.G., Abdul, U.K., Houweling, M., Linde, M.E. van, Lagerweij, T., Verheul, H.M.W., Westerman, B.A., Walenkamp, A.M., Fehrmann, R.S.N., Brahm, C.G., Abdul, U.K., Houweling, M., Linde, M.E. van, Lagerweij, T., Verheul, H.M.W., Westerman, B.A., Walenkamp, A.M., and Fehrmann, R.S.N.

Abstract

Contains fulltext : 229580.pdf (publisher's version ) (Open Access), BACKGROUND: Patients with glioblastoma (GBM) have a dismal prognosis, and there is an unmet need for new therapeutic options. This study aims to identify new therapeutic targets in GBM. METHODS: mRNA expression data of patient-derived GBM (n = 1279) and normal brain tissue (n = 46) samples were collected from Gene Expression Omnibus and The Cancer Genome Atlas. Functional genomic mRNA profiling was applied to capture the downstream effects of genomic alterations on gene expression levels. Next, a class comparison between GBM and normal brain tissue was performed. Significantly upregulated genes in GBM were further prioritized based on (1) known interactions with antineoplastic drugs, (2) current drug development status in humans, and (3) association with biologic pathways known to be involved in GBM. Antineoplastic agents against prioritized targets were validated in vitro and in vivo. RESULTS: We identified 712 significantly upregulated genes in GBM compared to normal brain tissue, of which 27 have a known interaction with antineoplastic agents. Seventeen of the 27 genes, including EGFR and VEGFA, have been clinically evaluated in GBM with limited efficacy. For the remaining 10 genes, RRM2, MAPK9 (JNK2, SAPK1a), and XIAP play a role in GBM development. We demonstrated for the MAPK9 inhibitor RGB-286638 a viability loss in multiple GBM cell culture models. Although no overall survival benefit was observed in vivo, there were indications that RGB-286638 may delay tumor growth. CONCLUSIONS: The MAPK9 inhibitor RGB-286638 showed promising in vitro results. Furthermore, in vivo target engagement studies and combination therapies with this compound warrant further exploration.

Published
2020

5. The TICking clock of EGFR therapy resistance in glioblastoma: Target Independence or target Compensation

Author

Saleem, H., Kulsoom Abdul, U., Küçükosmanoglu, A., Houweling, M., Cornelissen, FMG, Heiland, D.H., Hegi, M.E., Kouwenhoven, MCM, Bailey, D., Würdinger, T., and Westerman, B.A.

Subjects
Brain Neoplasms/drug therapy, Brain Neoplasms/genetics, Brain Neoplasms/pathology, Carcinogenesis/drug effects, Carcinogenesis/genetics, Drug Resistance, Neoplasm, ErbB Receptors/antagonists & inhibitors, ErbB Receptors/genetics, ErbB Receptors/metabolism, Glioblastoma/drug therapy, Glioblastoma/genetics, Glioblastoma/pathology, Humans, Molecular Targeted Therapy/methods, Mutation, Oncogenes/genetics, Protein Kinase Inhibitors/pharmacology, Protein Kinase Inhibitors/therapeutic use, Proto-Oncogene Proteins c-met/metabolism, Proto-Oncogene Proteins c-sis/metabolism, Receptor, IGF Type 1/metabolism, Signal Transduction/drug effects, Signal Transduction/genetics, Treatment Outcome, CMET, EGFR inhibition, Glioblastoma, IGFR1, Target compensation, PDGFR, Target independence, Therapy resistance
Abstract

Targeted therapy against driver mutations responsible for cancer progression has been shown to be effective in many tumor types. For glioblastoma (GBM), the epidermal growth factor receptor (EGFR) gene is the most frequently mutated oncogenic driver and has therefore been considered an attractive target for therapy. However, so far responses to EGFR-pathway inhibitors have been disappointing. We performed an exhaustive analysis of the mechanisms that might account for therapy resistance against EGFR inhibition. We define two major mechanisms of resistance and propose modalities to overcome them. The first resistance mechanism concerns target independence. In this case, cells have lost expression of the EGFR protein and experience no negative impact of EGFR targeting. Loss of extrachromosomally encoded EGFR as present in double minute DNA is a frequent mechanism for this type of drug resistance. The second mechanism concerns target compensation. In this case, cells will counteract EGFR inhibition by activation of compensatory pathways that render them independent of EGFR signaling. Compensatory pathway candidates are platelet-derived growth factor β (PDGFβ), Insulin-like growth factor 1 (IGFR1) and cMET and their downstream targets, all not commonly mutated at the time of diagnosis alongside EGFR mutation. Given that both mechanisms make cells independent of EGFR expression, other means have to be found to eradicate drug resistant cells. To this end we suggest rational strategies which include the use of multi-target therapies that hit truncation mutations (mechanism 1) or multi-target therapies to co-inhibit compensatory proteins (mechanism 2).

Published
2019

6. Cross-Tissue Transcriptomic Analysis of Human Secondary Lymphoid Organ-Residing ILC3s Reveals a Quiescent State in the Absence of Inflammation

Author

Bar-Ephraim, Y.E. (Yotam E.), Cornelissen, F.H.J. (Ferry), Papazian, N. (Natalie), Konijn, T. (Tanja), Hoogenboezem, R.M. (Remco), Sanders, M.A. (Mathijs), Westerman, B.A. (Bart A.), Gönültas, M. (Mehmet), Kwekkeboom, J. (Jaap), den Haan, J.M.M. (Joke M.M.), Reijmers, R.M. (Rogier), Mebius, R.E. (Reina), Cupedo, T. (Tom), Bar-Ephraim, Y.E. (Yotam E.), Cornelissen, F.H.J. (Ferry), Papazian, N. (Natalie), Konijn, T. (Tanja), Hoogenboezem, R.M. (Remco), Sanders, M.A. (Mathijs), Westerman, B.A. (Bart A.), Gönültas, M. (Mehmet), Kwekkeboom, J. (Jaap), den Haan, J.M.M. (Joke M.M.), Reijmers, R.M. (Rogier), Mebius, R.E. (Reina), and Cupedo, T. (Tom)

Abstract

A substantial number of human and mouse group 3 innate lymphoid cells (ILC3s) reside in secondary lymphoid organs, yet the phenotype and function of these ILC3s is incompletely understood. Here, we employed an unbiased cross-tissue transcriptomic approach to compare human ILC3s from non-inflamed lymph nodes and spleen to their phenotypic counterparts in inflamed tonsils and from circulation. These analyses revealed that, in the absence of inflammation, lymphoid organ-residing ILC3s lack transcription of cytokines associated with classical ILC3 functions. This was independent of expression of the natural cytotoxicity receptor NKp44. However, and in contrast to ILC3s from peripheral blood, lymphoid organ-residing ILC3s express activating cytokine receptors and have acquired the ability to be recruited into immune responses by inflammatory cytokines. This comprehensive cross-tissue dataset will allow for identification of functional changes in human lymphoid organ ILC3s associated with human disease. Bar-Ephraim et al. describe a cross-tissue transcriptional comparison of human ILC3s and show that ILC3s in lymph nodes and spleen share a transcriptional profile that is distinct from that of tonsil ILC3s. Lymphoid organ ILC3s are a substantial pool of resting cells that can be recruited into immune responses upon local activation.

Published
2017
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7. Expression of Three Proneural basic Helix-Loop-Helix Transcription Factors in Extravillus Trophoblasts suggests Role in Trophoblast Differentiation and Invasion

Author

Oudejans, C.B.M., Westerman, B.A., Poutsma, A., and van Wijk, I.J.

Subjects
Human genetics -- Research, Gene expression -- Research, Trophoblast -- Genetic aspects, Uterus -- Physiological aspects, Human reproduction -- Research, Cell research -- Analysis, Sex differentiation disorders -- Genetic aspects, Biological sciences
Published
2001

8. RNA-Seq of Tumor-Educated Platelets Enables Blood-Based Pan-Cancer, Multiclass, and Molecular Pathway Cancer Diagnostics

Author

Best, M.G., Sol, N., Kooi, I., Tannous, J., Westerman, B.A., Rustenburg, F., Schellen, P., Verschueren, H., Post, E., Koster, J., Ylstra, B., Ameziane, N., Dorsman, J., Smit, E.F., Verheul, H.M., Noske, D.P., Reijneveld, J.C., Nilsson, R.J., Tannous, B.A., Wesseling, P., Wurdinger, T., Best, M.G., Sol, N., Kooi, I., Tannous, J., Westerman, B.A., Rustenburg, F., Schellen, P., Verschueren, H., Post, E., Koster, J., Ylstra, B., Ameziane, N., Dorsman, J., Smit, E.F., Verheul, H.M., Noske, D.P., Reijneveld, J.C., Nilsson, R.J., Tannous, B.A., Wesseling, P., and Wurdinger, T.

Abstract

Contains fulltext : 152642.pdf (Publisher’s version ) (Open Access), Tumor-educated blood platelets (TEPs) are implicated as central players in the systemic and local responses to tumor growth, thereby altering their RNA profile. We determined the diagnostic potential of TEPs by mRNA sequencing of 283 platelet samples. We distinguished 228 patients with localized and metastasized tumors from 55 healthy individuals with 96% accuracy. Across six different tumor types, the location of the primary tumor was correctly identified with 71% accuracy. Also, MET or HER2-positive, and mutant KRAS, EGFR, or PIK3CA tumors were accurately distinguished using surrogate TEP mRNA profiles. Our results indicate that blood platelets provide a valuable platform for pan-cancer, multiclass cancer, and companion diagnostics, possibly enabling clinical advances in blood-based "liquid biopsies".

Published
2015

10. Sequencing of neuroblastoma identifies chromothripsis and defects in neuritogenesis genes

Author

Molenaar, J. (Jan), Koster, J. (Jan), Zwijnenburg, D. (Danny), Sluis, P. (Peter) van, Valentijn, L.J. (Linda), Ploeg, I. (Ida) van der, Hamdi, M. (Mohamed), Nes, J. (Johan) van, Westerman, B.A. (Bart), Arkel, J. (Jennemiek) van, Ebus, M.E., Haneveld, F. (Franciska), Lakeman, A. (Arjan), Schild, L. (Linda), Molenaar, P. (Piet), Stroeken, P. (Peter), Noesel, M.M. (Max) van, Øra, I. (Ingrid), Santo, J.P. (James) di, Caron, H.N. (Huib), Westerhout, E.M. (Ellen), Versteeg, R. (Rogier), Molenaar, J. (Jan), Koster, J. (Jan), Zwijnenburg, D. (Danny), Sluis, P. (Peter) van, Valentijn, L.J. (Linda), Ploeg, I. (Ida) van der, Hamdi, M. (Mohamed), Nes, J. (Johan) van, Westerman, B.A. (Bart), Arkel, J. (Jennemiek) van, Ebus, M.E., Haneveld, F. (Franciska), Lakeman, A. (Arjan), Schild, L. (Linda), Molenaar, P. (Piet), Stroeken, P. (Peter), Noesel, M.M. (Max) van, Øra, I. (Ingrid), Santo, J.P. (James) di, Caron, H.N. (Huib), Westerhout, E.M. (Ellen), and Versteeg, R. (Rogier)

Abstract

Neuroblastoma is a childhood tumour of the peripheral sympathetic nervous system. The pathogenesis has for a long time been quite enigmatic, as only very few gene defects were identified in this often lethal tumour. Frequently detected gene alterations are limited to MYCN amplification (20%) and ALK activations (7%). Here we present a whole-genome sequence analysis of 87 neuroblastoma of all stages. Few recurrent amino-acid-changing mutations were found. In contrast, analysis of structural defects identified a local shredding of chromosomes, known as chromothripsis, in 18% of high-stage neuroblastoma. These tumours are associated with a poor outcome. Structural alterations recurrently affected ODZ3, PTPRD and CSMD1, which are involved in neuronal growth cone stabilization. In addition, ATRX, TIAM1 and a series of regulators of the Rac/Rho pathway were mutated, further implicating defects in neuritogenesis in neuroblastoma. Most tumours with defects in these genes were aggressive high-stage neuroblastomas, but did not carry MYCN amplifications. The genomic landscape of neuroblastoma therefore reveals two novel molecular defects, chromothripsis and neuritogenesis gene alterations, which frequently occur in high-risk tumours.

Published
2012
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