Search

Your search keyword '"Hoeben A"' showing total 2,206 results
Start Over Author "Hoeben A" Search Limiters Full Text
2,206 results on '"Hoeben A"'

4. Forest value chain resilience from a local perspective in five European countries: analysis of predictors and co-drivers

Author

Sandra P. García-Jácome, Martin Jankovský, Annechien Dirkje Hoeben, Marcus Lindner, Sara Uzquiano, Tobias Stern, Ondrej Nuhlíček, Dijana Vuletić, Hrvoje Marjanović, Juan Picos, Mikko Peltoniemi, Lukas Baumbach, and Francisco Lloret

Subjects
disturbances, timber supply, social-ecological systems, forest management, thresholds, wood production, Forestry, SD1-669.5, Environmental sciences, GE1-350
Abstract

Climate change-associated disturbances such as storms, wildfires, and pest outbreaks increasingly destabilize forest systems, threatening their ecological, economic, and social functions. These disruptions impact the forest value chain (FVC) by causing fluctuations in timber supply, from a quantity and quality perspective. This study employed the operational resilience framework (ORF) to assess FVC resilience in five European case studies (CZ, HR, DE, FIN, and ESP), focusing on timber supply as a key system variable. A resilience assessment was conducted using resilience thresholds, considering sustainability from both ecological and economic perspectives. Principal component analysis (PCA) identified three predictor groups that influenced FVC resilience: wood production (WP), harvesting systems (HS), and management and silviculture (MS). Findings revealed that regions with proactive management and sufficient processing capacities (CZ, HR, and ESP) maintained relative stability despite natural disturbances, while others (DE and FIN) experienced prolonged instability due to market-driven logging practices and limited adaptive measures. The study highlighted the frequent breaching of resilience thresholds, particularly during high-volume salvage logging following disturbances such as bark beetle outbreaks, windstorms, and wildfires. The results emphasized the importance of integrating adaptive and proactive strategies to mitigate these impacts. The ORF demonstrated potential for operationalizing FVC resilience and provided guidance for improving preparedness against future disturbances.

Published
2025
Full Text
View/download PDF

5. Antibody-epitope conjugates deliver immunogenic T-cell epitopes more efficiently when close to cell surfaces

Author

W. van der Wulp, W. Luu, M. E. Ressing, J. Schuurman, S. I. van Kasteren, L. Guelen, R. C. Hoeben, B. Bleijlevens, and M. H. M. Heemskerk

Subjects
antibody-epitope conjugates (AECs), virus-specific T-cells, immunotherapy, redirecting T-cells, bispecific-antibodies, Therapeutics. Pharmacology, RM1-950, Immunologic diseases. Allergy, RC581-607
Abstract

Antibody-mediated delivery of immunogenic viral CD8+ T-cell epitopes to redirect virus-specific T cells toward cancer cells is a promising new therapeutic avenue to increase the immunogenicity of tumors. Multiple strategies for viral epitope delivery have been shown to be effective. So far, most of these have relied on a free C-terminus of the immunogenic epitope for extracellular delivery. Here, we demonstrate that antibody-epitope conjugates (AECs) with genetically fused epitopes to the N-terminus of the antibody can also sensitize tumors for attack by virus-specific CD8+ T cells. AECs carrying epitopes genetically fused at the N-terminus of the light chains of cetuximab and trastuzumab demonstrate an even more efficient delivery of the T-cell epitopes compared to AECs with the epitope fused to the C-terminus of the heavy chain. We demonstrate that this increased efficiency is not caused by the shift in location of the cleavage site from the N- to the C-terminus, but by its increased proximity to the cell surface. We hypothesize that this facilitates more efficient epitope delivery. These findings not only provide additional insights into the mechanism of action of AECs but also broaden the possibilities for genetically fused AECs as an avenue for the redirection of multiple virus-specific T cells toward tumors.

Published
2024
Full Text
View/download PDF

6. Preclinical evaluation of the gorilla‐derived HAdV‐B AdV‐lumc007 oncolytic adenovirus ‘GoraVir’ for the treatment of pancreatic ductal adenocarcinoma

Author

Selas T. F. Bots, Tom J. Harryvan, Christianne Groeneveldt, Priscilla Kinderman, Vera Kemp, Nadine vanMontfoort, and Rob C. Hoeben

Subjects
CD46, non‐human primate oncolytic adenovirus, pancreatic ductal adenocarcinoma, tumour‐stroma, xenograft model, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive malignancy which shows unparalleled therapeutic resistance due to its genetic and cellular heterogeneity, dense stromal tissue, and immune‐suppressive tumour microenvironment. Oncolytic virotherapy has emerged as a new treatment modality which uses tumour‐specific viruses to eliminate cancerous cells. Non‐human primate adenoviruses of the human adenovirus B (HAdV‐B) species have demonstrated considerable lytic potential in human cancer cells as well as limited preexisting neutralizing immunity in humans. Previously, we have generated a new oncolytic derivative of the gorilla‐derived HAdV‐B AdV‐lumc007 named ‘GoraVir’. Here, we show that GoraVir displays oncolytic efficacy in pancreatic cancer cells and pancreatic‐cancer‐associated fibroblasts. Moreover, it retains its lytic potential in monoculture and co‐culture spheroids. In addition, we established the ubiquitously expressed complement receptor CD46 as the main entry receptor for GoraVir. Finally, a single intratumoural dose of GoraVir was shown to delay tumour growth in a BxPC‐3 xenograft model at 10 days post‐treatment. Collectively, these data demonstrate that the new gorilla‐derived oncolytic adenovirus is a potent oncolytic vector candidate that targets both pancreatic cancer cells and tumour‐adjacent stroma.

Published
2024
Full Text
View/download PDF

10. Biomarker screen for efficacy of oncolytic virotherapy in patient-derived pancreatic cancer culturesResearch in context

Author

Theresa E. Schäfer, Lisanne I. Knol, Ferdinand V. Haas, Anna Hartley, Sophie C.S. Pernickel, Attila Jády, Maximiliane S.C. Finkbeiner, Johannes Achberger, Stella Arelaki, Živa Modic, Katrin Schröer, Wenli Zhang, Barbara Schmidt, Philipp Schuster, Sebastian Haferkamp, Johannes Doerner, Florian Gebauer, Maximilian Ackermann, Hans-Michael Kvasnicka, Amit Kulkarni, Selas T.F. Bots, Vera Kemp, Lukas J.A.C. Hawinkels, Anna R. Poetsch, Rob C. Hoeben, Anja Ehrhardt, Antonio Marchini, Guy Ungerechts, Claudia R. Ball, and Christine E. Engeland

Subjects
Pancreatic cancer, Oncolytic virotherapy, Cancer immunotherapy, Viral vectors, Medicine, Medicine (General), R5-920
Abstract

Summary: Background: Pancreatic ductal adenocarcinoma (PDAC) is a tumour entity with unmet medical need. To assess the therapeutic potential of oncolytic virotherapy (OVT) against PDAC, different oncolytic viruses (OVs) are currently investigated in clinical trials. However, systematic comparisons of these different OVs in terms of efficacy against PDAC and biomarkers predicting therapeutic response are lacking. Methods: We screened fourteen patient-derived PDAC cultures which reflect the intra- and intertumoural heterogeneity of PDAC for their sensitivity to five clinically relevant OVs, namely serotype 5 adenovirus Ad5-hTERT, herpes virus T-VEC, measles vaccine strain MV-NIS, reovirus jin-3, and protoparvovirus H-1PV. Live cell analysis, quantification of viral genome/gene expression, cell viability as well as cytotoxicity assays and titration of viral progeny were conducted. Transcriptome profiling was employed to identify potential predictive biomarkers for response to OV treatment. Findings: Patient-derived PDAC cultures showed individual response patterns to OV treatment. Twelve of fourteen cultures were responsive to at least one OV, with no single OV proving superior or inferior across all cultures. Known host factors for distinct viruses were retrieved as potential biomarkers. Compared to the classical molecular subtype, the quasi-mesenchymal or basal-like subtype of PDAC was found to be more sensitive to H-1PV, jin-3, and T-VEC. Generally, expression of viral entry receptors did not correlate with sensitivity to OV treatment, with one exception: Expression of Galectin-1 (LGALS1), a factor involved in H-1PV entry, positively correlated with H-1PV induced cell killing. Rather, cellular pathways controlling immunological, metabolic and proliferative signaling appeared to determine outcome. For instance, high baseline expression of interferon-stimulated genes (ISGs) correlated with relative resistance to oncolytic measles virus, whereas low cyclic GMP-AMP synthase (cGAS) expression was associated with exceptional response. Combination treatment of MV-NIS with a cGAS inhibitor improved tumour cell killing in several PDAC cultures and cells overexpressing cGAS were found to be less sensitive to MV oncolysis. Interpretation: Considering the heterogeneity of PDAC and the complexity of biological therapies such as OVs, no single biomarker can explain the spectrum of response patterns. For selection of a particular OV, PDAC molecular subtype, ISG expression as well as activation of distinct signaling and metabolic pathways should be considered. Combination therapies can overcome resistance in specific constellations. Overall, oncolytic virotherapy is a viable treatment option for PDAC, which warrants further development. This study highlights the need for personalised treatment in OVT. By providing all primary data, this study provides a rich source and guidance for ongoing developments. Funding: German National Science Foundation (Deutsche Forschungsgemeinschaft, DFG), German Cancer Aid (Deutsche Krebshilfe), German National Academic Scholarship Foundation (Studienstiftung des deutschen Volkes), Survival with Pancreatic Cancer Foundation.

Published
2024
Full Text
View/download PDF

11. The heterogeneous sensitivity of pediatric brain tumors to different oncolytic viruses is predicted by unique gene expression profiles

Author

Konstantinos Vazaios, Εftychia Stavrakaki, Lisette B. Vogelezang, Jie Ju, Piotr Waranecki, Dennis S. Metselaar, Michaël H. Meel, Vera Kemp, Bernadette G. van den Hoogen, Rob C. Hoeben, E. Antonio Chiocca, William F. Goins, Andrew Stubbs, Yunlei Li, Marta M. Alonso, Friso G. Calkoen, Esther Hulleman, Jasper van der Lugt, and Martine L.M. Lamfers

Subjects
MT: Regular Issue, pediatric brain tumors, oncolytic viruses, sensitivity, resistance, Gene Ontology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Despite decades of research, the prognosis of high-grade pediatric brain tumors (PBTs) remains dismal; however, recent cases of favorable clinical responses were documented in clinical trials using oncolytic viruses (OVs). In the current study, we employed four different species of OVs: adenovirus Delta24-RGD, herpes simplex virus rQNestin34.5v1, reovirus R124, and the non-virulent Newcastle disease virus rNDV-F0-GFP against three entities of PBTs (high-grade gliomas, atypical teratoid/rhabdoid tumors, and ependymomas) to determine their in vitro efficacy. These four OVs were screened on 14 patient-derived PBT cell cultures and the degree of oncolysis was assessed using an ATP-based assay. Subsequently, the observed viral efficacies were correlated to whole transcriptome data and Gene Ontology analysis was performed. Although no significant tumor type-specific OV efficacy was observed, the analysis revealed the intrinsic biological processes that associated with OV efficacy. The predictive power of the identified expression profiles was further validated in vitro by screening additional PBTs. In summary, our results demonstrate OV susceptibility of multiple patient-derived PBT entities and the ability to predict in vitro responses to OVs using unique expression profiles. Such profiles may hold promise for future OV preselection with effective oncolytic potency in a specific tumor, therewith potentially improving OV responses.

Published
2024
Full Text
View/download PDF

12. Pulsed processing by cold plasma, applied to industrial emission control

Author

E. J. M. Van Heesch, T. Huiskamp, K. Yan, F. J. C. M. Beckers, H. W. M. Smulders, G. J. J. Winands, R. H. P. Lemmens, P. P. M. Blom, S. Davalos Segura, W. F. L. M. Hoeben, S. V. B. Van Paasen, J. J. Van Oorschot, A. G. A. Bonkestoter, M. L. J. Van Den Brand, M. Hennink, R. W. J. Smulders, A. J. M. Pemen, and P. C. T. Van Der Laan

Subjects
cold plasma, nanosecond pulses, pulsed processing, plasma processing, VOC, emission control, Chemistry, QD1-999
Abstract

A promising pollution control technology is cold plasma driven chemical processing. The plasma is a pulsed electric gas discharge inside a near atmospheric-pressure-temperature reactor. The system is energized by a continuous stream of very short high-voltage pulses. The exhaust gas to be treated flows through the reactor. The methods applied involve the development of robust cold plasma systems, industrial applications and measuring technologies. Tests of the systems were performed at many industrial sites and involved control of airborne VOC (volatile organic compound) and odor. Electrical, chemical and odor measuring data were collected with state-of-the-art methods. To explain the test data an approximate solution of global reaction kinetics of pulsed plasma chemistry was developed. It involves the Lambert function and, for convenience, a simple approximation of it. The latter shows that the amount of removal, in good approximation, is a function of a single variable. This variable is electric plasma power divided by gas flow divided by input concentration. In the results sections we show that in some cases up to 99% of volatile pollution can be removed at an acceptable energy requirement. In the final sections we look into future efficiency enhancements by implementation of (sub)nanosecond pulsed plasma and solid state high-voltage technology and by integration with catalyst technology.

Published
2024
Full Text
View/download PDF

15. Treatment robustness of total body irradiation with volumetric modulated arc therapy

Author

Enrica Seravalli, Mirjam Willemsen-Bosman, Annelies Zoetelief, Sanne Roosenboom, Tessa Harderwijk, Lean Krikke, Gijsbert Bol, Alexis Kotte, Eline Huijboom, Karel van Loon, and Bianca Hoeben

Subjects
Total body irradiation, TBI, VMAT, Conformal radiotherapy techniques, Patient position verification, Junction, Medical physics. Medical radiology. Nuclear medicine, R895-920, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

This study evaluated the robustness of multi-isocenter Volumetric Modulated Arc Therapy Total Body Irradiation dose distribution in the overlapping region between the head-first and feet-first computed tomography scans, considering the longitudinal isocenter shifts recorded during treatment delivery. For 15 out of 22 patients, the dose distribution in the overlapping region fulfilled all three the robustness criteria. The overlapping region dose distribution of the remaining 7 cases fulfilled two robustness criteria. The dose distribution was found to be robust against daily recorded longitudinal isocenter shifts, as a consequence of the patient position verification procedure, of up to 16 mm.

Published
2024
Full Text
View/download PDF

17. The predictive and prognostic value of weight loss and body composition prior to and during immune checkpoint inhibition in recurrent or metastatic head and neck cancer patients

Author

Anna C. H. Willemsen, Nina De Moor, Jeroen Van Dessel, Laura W. J. Baijens, Michel Bila, Esther Hauben, Mari F. C. M. van denHout, Vincent Vander Poorten, Ann Hoeben, Paul M. Clement, and Annemie M. W. J. Schols

Subjects
body composition, cachexia, head and neck cancer, immune checkpoint inhibitors, weight loss, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background Response rates of immune checkpoint inhibitor (ICI) therapy for recurrent and/or metastatic head and neck squamous cell carcinoma (R/M HNSCC) are low. Patients and Methods This retrospective multicentre cohort study evaluates the predictive and prognostic value of weight loss and changes in body composition prior and during therapy. Patient, tumor, and treatment characteristics of 98 patients were retrieved, including neutrophil and platelet‐lymphocyte‐ratio (NLR and PLR). Programmed death‐ligand 1 (PD‐L1) expression was determined on residual material. Cachexia was defined according to Fearon et al. (2011). Skeletal muscle (SM), visceral adipose tissue (VAT), and subcutaneous adipose tissue (SAT) were evaluated on computed tomography scans at the third lumbar vertebrae level. Univariable and multivariable regression analyses were performed for 6 months progression free survival (PFS6m) and overall survival (OS). Results Significant early weight loss (>2%) during the first 6 weeks of therapy was shown in 34 patients (35%). This patient subgroup had a significantly higher NLR and PLR at baseline. NLR and PLR were inversely correlated with SM and VAT index. Independent predictors of PFS6m were lower World Health Organization performance status (HR 0.16 [0.04–0.54] p = 0.003), higher baseline SAT index (HR 1.045 [1.02–1.08] p = 0.003), and weight loss 2% early weight loss remained a predictor of OS, independent of PD‐L1 expression (HR 2.09 [1.11–3.92] p = 0.02, HR 2.18 [1.13–4.21] p = 0.02). Conclusion We conclude that the combination of cachexia at baseline and weight loss during ICI therapy is associated with worse OS in R/M HNSCC patients, independent of PD‐L1 expression.

Published
2023
Full Text
View/download PDF

18. Efficacy, safety and biomarker analysis of durvalumab in patients with mismatch-repair deficient or microsatellite instability-high solid tumours

Author

Birgit S. Geurts, Thomas W. Battaglia, J. Maxime van Berge Henegouwen, Laurien J. Zeverijn, Gijs F. de Wit, Louisa R. Hoes, Hanneke van der Wijngaart, Vincent van der Noort, Paul Roepman, Wendy W. J. de Leng, Anne M. L. Jansen, Frans L. Opdam, Maja J. A. de Jonge, Geert A. Cirkel, Mariette Labots, Ann Hoeben, Emile D. Kerver, Adriaan D. Bins, Frans G.L. Erdkamp, Johan M. van Rooijen, Danny Houtsma, Mathijs P. Hendriks, Jan-Willem B. de Groot, Henk M. W. Verheul, Hans Gelderblom, and Emile E. Voest

Subjects
Durvalumab, Immunotherapy, Microsatellite instability, Mismatch repair deficiency, Precision medicine, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background In this study we aimed to evaluate the efficacy and safety of the PD-L1 inhibitor durvalumab across various mismatch repair deficient (dMMR) or microsatellite instability-high (MSI-H) tumours in the Drug Rediscovery Protocol (DRUP). This is a clinical study in which patients are treated with drugs outside their labeled indication, based on their tumour molecular profile. Patients and methods Patients with dMMR/MSI-H solid tumours who had exhausted all standard of care options were eligible. Patients were treated with durvalumab. The primary endpoints were clinical benefit ((CB): objective response (OR) or stable disease ≥16 weeks) and safety. Patients were enrolled using a Simon like 2-stage model, with 8 patients in stage 1, up to 24 patients in stage 2 if at least 1/8 patients had CB in stage 1. At baseline, fresh frozen biopsies were obtained for biomarker analyses. Results Twenty-six patients with 10 different cancer types were included. Two patients (2/26, 8%) were considered as non-evaluable for the primary endpoint. CB was observed in 13 patients (13/26, 50%) with an OR in 7 patients (7/26, 27%). The remaining 11 patients (11/26, 42%) had progressive disease. Median progression-free survival and median overall survival were 5 months (95% CI, 2-not reached) and 14 months (95% CI, 5-not reached), respectively. No unexpected toxicity was observed. We found a significantly higher structural variant (SV) burden in patients without CB. Additionally, we observed a significant enrichment of JAK1 frameshift mutations and a significantly lower IFN-γ expression in patients without CB. Conclusion Durvalumab was generally well-tolerated and provided durable responses in pre-treated patients with dMMR/MSI-H solid tumours. High SV burden, JAK1 frameshift mutations and low IFN-γ expression were associated with a lack of CB; this provides a rationale for larger studies to validate these findings. Trial registration Clinical trial registration: NCT02925234. First registration date: 05/10/2016.

Published
2023
Full Text
View/download PDF

19. Transcriptome analysis reveals tumor microenvironment changes in glioblastoma

Author

Hoogstrate, Youri, Draaisma, Kaspar, Ghisai, Santoesha A., van Hijfte, Levi, Barin, Nastaran, de Heer, Iris, Coppieters, Wouter, van den Bosch, Thierry P.P., Bolleboom, Anne, Gao, Zhenyu, Vincent, Arnaud J.P.E., Karim, Latifa, Deckers, Manon, Taphoorn, Martin J.B., Kerkhof, Melissa, Weyerbrock, Astrid, Sanson, Marc, Hoeben, Ann, Lukacova, Slávka, Lombardi, Giuseppe, Leenstra, Sieger, Hanse, Monique, Fleischeuer, Ruth E.M., Watts, Colin, Angelopoulos, Nicos, Gorlia, Thierry, Golfinopoulos, Vassilis, Bours, Vincent, van den Bent, Martin J., Robe, Pierre A., and French, Pim J.

Published
2023
Full Text
View/download PDF

20. Study protocol of the GLOW study: maximising treatment options for recurrent glioblastoma patients by whole genome sequencing-based diagnostics—a prospective multicenter cohort study

Author

Mark P. van Opijnen, Marike L. D. Broekman, Filip Y. F. de Vos, Edwin Cuppen, Jacobus J. M. van der Hoeven, Myra E. van Linde, Annette Compter, Laurens V. Beerepoot, Martin J. van den Bent, Maaike J. Vos, Helle-Brit Fiebrich, Johan A. F. Koekkoek, Ann Hoeben, Kuan H. Kho, Chantal M. L. Driessen, Hanne-Rinck Jeltema, Pierre A. J. T. Robe, and Sybren L. N. Maas

Subjects
Glioblastoma, Whole genome sequencing, Treatment options, Diagnostics, Recurrence, Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Glioblastoma (GBM), the most common glial primary brain tumour, is without exception lethal. Every year approximately 600 patients are diagnosed with this heterogeneous disease in The Netherlands. Despite neurosurgery, chemo -and radiation therapy, these tumours inevitably recur. Currently, there is no gold standard at time of recurrence and treatment options are limited. Unfortunately, the results of dedicated trials with new drugs have been very disappointing. The goal of the project is to obtain the evidence for changing standard of care (SOC) procedures to include whole genome sequencing (WGS) and consequently adapt care guidelines for this specific patient group with very poor prognosis by offering optimal and timely benefit from novel therapies, even in the absence of traditional registration trials for this small volume cancer indication. Methods The GLOW study is a prospective diagnostic cohort study executed through collaboration of the Hartwig Medical Foundation (Hartwig, a non-profit organisation) and twelve Dutch centers that perform neurosurgery and/or treat GBM patients. A total of 200 patients with a first recurrence of a glioblastoma will be included. Dual primary endpoint is the percentage of patients who receive targeted therapy based on the WGS report and overall survival. Secondary endpoints include WGS report success rate and number of targeted treatments available based on WGS reports and number of patients starting a treatment in presence of an actionable variant. At recurrence, study participants will undergo SOC neurosurgical resection. Tumour material will then, together with a blood sample, be sent to Hartwig where it will be analysed by WGS. A diagnostic report with therapy guidance, including potential matching off-label drugs and available clinical trials will then be sent back to the treating physician for discussing of the results in molecular tumour boards and targeted treatment decision making. Discussion The GLOW study aims to provide the scientific evidence for changing the SOC diagnostics for patients with a recurrent glioblastoma by investigating complete genome diagnostics to maximize treatment options for this patient group. Trial registration: ClinicalTrials.gov Identifier: NCT05186064.

Published
2022
Full Text
View/download PDF

21. Comparison of methods generating antibody-epitope conjugates for targeting cancer with virus-specific T cells

Author

Willemijn van der Wulp, Anna M. Gram, Boris Bleijlevens, Renate S. Hagedoorn, Can Araman, Robbert Q. Kim, Jan Wouter Drijfhout, Paul W. H. I. Parren, Richard G. Hibbert, Rob C. Hoeben, Sander I. van Kasteren, Janine Schuurman, Maaike E. Ressing, and Mirjam H. M. Heemskerk

Subjects
antibody-epitope conjugates (AECs), redirecting virus-specific T-cells, immunotherapy, targeted therapy, conjugation strategies, Immunologic diseases. Allergy, RC581-607
Abstract

Therapeutic antibody-epitope conjugates (AECs) are promising new modalities to deliver immunogenic epitopes and redirect virus-specific T-cell activity to cancer cells. Nevertheless, many aspects of these antibody conjugates require optimization to increase their efficacy. Here we evaluated different strategies to conjugate an EBV epitope (YVL/A2) preceded by a protease cleavage site to the antibodies cetuximab and trastuzumab. Three approaches were taken: chemical conjugation (i.e. a thiol-maleimide reaction) to reduced cysteine side chains, heavy chain C-terminal enzymatic conjugation using sortase A, and genetic fusions, to the heavy chain (HC) C-terminus. All three conjugates were capable of T-cell activation and target-cell killing via proteolytic release of the EBV epitope and expression of the antibody target was a requirement for T-cell activation. Moreover, AECs generated with a second immunogenic epitope derived from CMV (NLV/A2) were able to deliver and redirect CMV specific T-cells, in which the amino sequence of the attached peptide appeared to influence the efficiency of epitope delivery. Therefore, screening of multiple protease cleavage sites and epitopes attached to the antibody is necessary. Taken together, our data demonstrated that multiple AECs could sensitize cancer cells to virus-specific T cells.

Published
2023
Full Text
View/download PDF

22. Detection and localization of early- and late-stage cancers using platelet RNA

Author

In ’t Veld, Sjors G.J.G., Arkani, Mohammad, Post, Edward, Antunes-Ferreira, Mafalda, D’Ambrosi, Silvia, Vessies, Daan C.L., Vermunt, Lisa, Vancura, Adrienne, Muller, Mirte, Niemeijer, Anna-Larissa N., Tannous, Jihane, Meijer, Laura L., Le Large, Tessa Y.S., Mantini, Giulia, Wondergem, Niels E., Heinhuis, Kimberley M., van Wilpe, Sandra, Smits, A. Josien, Drees, Esther E.E., Roos, Eva, Leurs, Cyra E., Tjon Kon Fat, Lee-Ann, van der Lelij, Ewoud J., Dwarshuis, Govert, Kamphuis, Maarten J., Visser, Lisanne E., Harting, Romee, Gregory, Annemijn, Schweiger, Markus W., Wedekind, Laurine E., Ramaker, Jip, Zwaan, Kenn, Verschueren, Heleen, Bahce, Idris, de Langen, Adrianus J., Smit, Egbert F., van den Heuvel, Michel M., Hartemink, Koen J., Kuijpers, Marijke J.E., oude Egbrink, Mirjam G.A., Griffioen, Arjan W., Rossel, Rafael, Hiltermann, T. Jeroen N., Lee-Lewandrowski, Elizabeth, Lewandrowski, Kent B., De Witt Hamer, Philip C., Kouwenhoven, Mathilde, Reijneveld, Jaap C., Leenders, William P.J., Hoeben, Ann, Verdonck-de Leeuw, Irma M., Leemans, C. René, Baatenburg de Jong, Robert J., Terhaard, Chris H.J., Takes, Robert P., Langendijk, Johannes A., de Jager, Saskia C., Kraaijeveld, Adriaan O., Pasterkamp, Gerard, Smits, Minke, Schalken, Jack A., Łapińska-Szumczyk, Sylwia, Łojkowska, Anna, Żaczek, Anna J., Lokhorst, Henk, van de Donk, Niels W.C.J., Nijhof, Inger, Prins, Henk-Jan, Zijlstra, Josée M., Idema, Sander, Baayen, Johannes C., Teunissen, Charlotte E., Killestein, Joep, Besselink, Marc G., Brammen, Lindsay, Bachleitner-Hofmann, Thomas, Mateen, Farrah, Plukker, John T.M., Heger, Michal, de Mast, Quirijn, Lisman, Ton, Pegtel, D. Michiel, Bogaard, Harm-Jan, Jassem, Jacek, Supernat, Anna, Mehra, Niven, Gerritsen, Winald, de Kroon, Cornelis D., Lok, Christianne A.R., Piek, Jurgen M.J., Steeghs, Neeltje, van Houdt, Winan J., Brakenhoff, Ruud H., Sonke, Gabe S., Verheul, Henk M., Giovannetti, Elisa, Kazemier, Geert, Sabrkhany, Siamack, Schuuring, Ed, Sistermans, Erik A., Wolthuis, Rob, Meijers-Heijboer, Hanne, Dorsman, Josephine, Oudejans, Cees, Ylstra, Bauke, Westerman, Bart A., van den Broek, Daan, Koppers-Lalic, Danijela, Wesseling, Pieter, Nilsson, R. Jonas A., Vandertop, W. Peter, Noske, David P., Tannous, Bakhos A., Sol, Nik, Best, Myron G., and Wurdinger, Thomas

Published
2022
Full Text
View/download PDF

25. CTP Synthase 1 Is a Novel Therapeutic Target in Lymphoma

Author

Hélène Asnagli, Norbert Minet, Christina Pfeiffer, Eef Hoeben, Rebecca Lane, David Laughton, Louise Birch, Geraint Jones, Andrew Novak, Andrew E. Parker, Heinz Ludwig, Alain Fischer, Sylvain Latour, and Philip A. Beer

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

Lymphoma is the most common hematological malignancy and is among the 10 most prevalent cancers worldwide. Although survival has been improved by modern immunochemotherapeutic regimens, there remains a significant need for novel targeted agents to treat both B-cell and T-cell malignancies. Cytidine triphosphate synthase 1 (CTPS1), which catalyzes the rate-limiting step in pyrimidine synthesis, plays an essential and nonredundant role in B-cell and T-cell proliferation but is complemented by the homologous CTPS2 isoform outside the hemopoietic system. This report describes the identification and characterization of CTPS1 as a novel target in B- and T-cell cancers. A series of small molecules have been developed which show potent and highly selective inhibition of CTPS1. Site-directed mutagenesis studies identified the adenosine triphosphate pocket of CTPS1 as the binding site for this small molecule series. In preclinical studies, a potent and highly selective small molecule inhibitor of CTPS1 blocked the in vitro proliferation of human neoplastic cells, showing the highest potency against lymphoid neoplasms. Importantly, pharmacological CTPS1 inhibition induced cell death by apoptosis in the majority of lymphoid cell lines tested, thus demonstrating a cytotoxic mechanism of action. Selective CTPS1 inhibition also inhibited the growth of neoplastic human B- and T- cells in vivo. These findings identify CTPS1 as a novel therapeutic target in lymphoid malignancy. A compound from this series is in phase 1/2 clinical studies for the treatment of relapsed/refractory B- and T-cell lymphoma (NCT05463263).

Published
2023
Full Text
View/download PDF

26. Heterogeneity of Network Structures and Water Dynamics in κ-Carrageenan Gels Probed by Nanoparticle Diffusometry.

Author

de Kort, Daan, Schuster, Erich, Hoeben, Freek, Barnes, Ryan, Emondts, Meike, Janssen, Henk, Lorén, Niklas, Han, Songi, Van As, Henk, and van Duynhoven, John

Abstract

A set of functionalized nanoparticles (PEGylated dendrimers, d = 2.8-11 nm) was used to probe the structural heterogeneity in Na+/K+ induced κ-carrageenan gels. The self-diffusion behavior of these nanoparticles as observed by 1H pulsed-field gradient NMR, fluorescence recovery after photobleaching, and raster image correlation spectroscopy revealed a fast and a slow component, pointing toward microstructural heterogeneity in the gel network. The self-diffusion behavior of the faster nanoparticles could be modeled with obstruction by a coarse network (average mesh size

Published
2018

27. Pulsed processing by cold plasma, applied to industrial emission control

Author

Van Heesch, E. J. M., primary, Huiskamp, T., additional, Yan, K., additional, Beckers, F. J. C. M., additional, Smulders, H. W. M., additional, Winands, G. J. J., additional, Lemmens, R. H. P., additional, Blom, P. P. M., additional, Segura, S. Davalos, additional, Hoeben, W. F. L. M., additional, Van Paasen, S. V. B., additional, Van Oorschot, J. J., additional, Bonkestoter, A. G. A., additional, Van Den Brand, M. L. J., additional, Hennink, M., additional, Smulders, R. W. J., additional, Pemen, A. J. M., additional, and Van Der Laan, P. C. T., additional

Published
2024
Full Text
View/download PDF

28. Influence of eye movement on lens dose and optic nerve target coverage during craniospinal irradiation

Author

Bianca A.W. Hoeben, Enrica Seravalli, Amber M.L. Wood, Mirjam Bosman, Witold P. Matysiak, John H. Maduro, Astrid L.H.M.W. van Lier, Matteo Maspero, Gijsbert H. Bol, and Geert O. Janssens

Subjects
Craniospinal irradiation, VMAT, 3D-conventional, Proton, Lens, Optic nerve, Medical physics. Medical radiology. Nuclear medicine, R895-920, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Purpose: Optic nerves are part of the craniospinal irradiation (CSI) target volume. Modern radiotherapy techniques achieve highly conformal target doses while avoiding organs-at-risk such as the lens. The magnitude of eye movement and its influence on CSI target- and avoidance volumes are unclear. We aimed to evaluate the movement-range of lenses and optic nerves and its influence on dose distribution of several planning techniques. Methods: Ten volunteers underwent MRI scans in various gaze directions (neutral, left, right, cranial, caudal). Lenses, orbital optic nerves, optic discs and CSI target volumes were delineated. 36-Gy cranial irradiation plans were constructed on synthetic CT images in neutral gaze, with Volumetric Modulated Arc Therapy, pencil-beam scanning proton therapy, and 3D-conventional photons. Movement-amplitudes of lenses and optic discs were analyzed, and influence of gaze direction on lens and orbital optic nerve dose distribution. Results: Mean eye structures’ shift from neutral position was greatest in caudal gaze; −5.8±1.2 mm (±SD) for lenses and 7.0±2.0 mm for optic discs. In 3D-conventional plans, caudal gaze decreased Mean Lens Dose (MLD). In VMAT and proton plans, eye movements mainly increased MLD and diminished D98 orbital optic nerve (D98OON) coverage; mean MLD increased up to 5.5 Gy [total ΔMLD range −8.1 to 10.0 Gy], and mean D98OON decreased up to 3.3 Gy [total ΔD98OON range −13.6 to 1.2 Gy]. VMAT plans optimized for optic disc Internal Target Volume and lens Planning organ-at-Risk Volume resulted in higher MLD over gaze directions. D98OON became ≥95% of prescribed dose over 95/100 evaluated gaze directions, while all-gaze bilateral D98OON significantly changed in 1 of 10 volunteers. Conclusion: With modern CSI techniques, eye movements result in higher lens doses and a mean detriment for orbital optic nerve dose coverage of

Published
2021
Full Text
View/download PDF

29. Collaborating to Improve Neonatal Care: ParentAl Participation on the NEonatal Ward—Study Protocol of the neoPARTNER Study

Author

Hannah Hoeben, Milène T. Alferink, Anne A. M. W. van Kempen, Johannes B. van Goudoever, Nicole R. van Veenendaal, Sophie R. D. van der Schoor, and on behalf of the neoPARTNER Study Group

Subjects
family-integrated care, family-centred rounds, neonatology, parental participation, parental stress, shared decision-making, Pediatrics, RJ1-570
Abstract

Parents are often appointed a passive role in the care for their hospitalised child. In the family-integrated care (FICare) model, parental involvement in neonatal care is emulated. Parental participation in medical rounds, or family-centred rounds (FCR), forms a key element. A paucity remains of randomised trials assessing the outcomes of FCR (embedded in FICare) in families and neonates, and outcomes on an organisational level are relatively unexplored. Likewise, biological mechanisms through which a potential effect may be exerted are lacking robust evidence. Ten level two Dutch neonatal wards are involved in this stepped-wedge cluster-randomised trial FCR (embedded in FICare) by one common implementation strategy. Parents of infants hospitalised for at least 7 days are eligible for inclusion. The primary outcome is parental stress (PSS:NICU) at discharge. Secondary outcomes include parental, neonatal, healthcare professional and organisational outcomes. Biomarkers of stress will be analysed in parent–infant dyads. With a practical approach and broad outcome set, this study aims to obtain evidence on the possible (mechanistic) effect of FCR (as part of FICare) on parents, infants, healthcare professionals and organisations. The practical approach provides (experiences of) FICare material adjusted to the Dutch setting, available for other hospitals after the study.

Published
2023
Full Text
View/download PDF

31. Inter-clinician delineation variation for a new highly-conformal flank target volume in children with renal tumors: A SIOP-Renal Tumor Study Group international multicenter exercise

Author

Mul, Joeri, Melchior, Patrick, Seravalli, Enrica, Saunders, Daniel, Bolle, Stephanie, Cameron, Alison L., Gurtner, Kristin, Harrabi, Semi, Lassen-Ramshad, Yasmin, Lavan, Naomi, Magelssen, Henriette, Mandeville, Henry, Boterberg, Tom, Kroon, Petra S., Kotte, Alexis N.T.J., Hoeben, Bianca A.W., van Rossum, Peter S.N., van Grotel, Martine, Graf, Norbert, van den Heuvel-Eibrink, Marry M., Rübe, Christian, and Janssens, Geert O.

Published
2021
Full Text
View/download PDF

33. Opportunities and Challenges of Small Molecule Inhibitors in Glioblastoma Treatment: Lessons Learned from Clinical Trials.

Author

Hoosemans, Linde, Vooijs, Marc, and Hoeben, Ann

Subjects
THERAPEUTIC use of antineoplastic agents, COMBINATION drug therapy, GLIOMAS, DRUG resistance in cancer cells, CLINICAL trials, ANTINEOPLASTIC agents, SMALL molecules, CANCER chemotherapy, TUMOR suppressor genes, ONCOGENES, TREATMENT failure, CARCINOGENESIS, DRUG discovery, EVALUATION, PHARMACODYNAMICS
Abstract

Simple Summary: Glioblastoma is the most common brain tumour, with a poor prognosis of about 15 months despite intensive treatment. Many trials have tested new drugs targeting specific genes, but none have succeeded, and treatments have not changed since 2005. This review explores why clinical trials with these drugs failed. It highlights the potential of combining different drugs to overcome resistance and suggests ways to improve future trials. The goal is to understand treatment failures and find new drug combinations to improve survival for GBM patients. Glioblastoma (GBM) is the most prevalent central nervous system tumour (CNS). Patients with GBM have a dismal prognosis of 15 months, despite an intensive treatment schedule consisting of surgery, chemoradiation and concurrent chemotherapy. In the last decades, many trials have been performed investigating small molecule inhibitors, which target specific genes involved in tumorigenesis. So far, these trials have been unsuccessful, and standard of care for GBM patients has remained the same since 2005. This review gives an overview of trials investigating small molecule inhibitors on their own, combined with chemotherapy or other small molecule inhibitors. We discuss possible resistance mechanisms in GBM, focussing on intra- and intertumoral heterogeneity, bypass mechanisms and the influence of the tumour microenvironment. Moreover, we emphasise how combining inhibitors can help overcome these resistance mechanisms. We also address strategies for improving trial outcomes through modifications to their design. In summary, this review aims to elucidate different resistance mechanisms against small molecule inhibitors, highlighting their significance in the search for novel therapeutic combinations to improve the overall survival of GBM patients. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

34. Preinduced reovirus-specific T-cell immunity enhances the anticancer efficacy of reovirus therapy

Author

Rob C Hoeben, Sjoerd H van der Burg, Marjolein Sluijter, Thorbald van Hall, Joke M M Den Haan, Camilla Labrie, Christianne Groeneveldt, Priscilla Kinderman, Diana J M van den Wollenberg, Nadine van Montfoort, Lisa Griffioen, and Jordi J C van Stigt Thans

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

Background Many solid tumors do not respond to immunotherapy due to their immunologically cold tumor microenvironment (TME). We and others found that oncolytic viruses (OVs), including reovirus type 3 Dearing, can enhance the efficacy of immunotherapy by recruiting CD8+ T cells to the TME. A significant part of the incoming CD8+ T cells is directed toward reovirus itself, which may be detrimental to the efficacy of OVs. However, here we aim to exploit these incoming virus-specific T cells as anticancer effector cells.Methods We performed an in-depth characterization of the reovirus-induced T-cell response in immune-competent mice bearing pancreatic KPC3 tumors. The immunodominant CD8+ T-cell epitope of reovirus was identified using epitope prediction algorithms and peptide arrays, and the quantity and quality of reovirus-specific T cells after reovirus administration were assessed using high-dimensional flow cytometry. A synthetic long peptide (SLP)-based vaccination strategy was designed to enhance the intratumoral frequency of reovirus-specific CD8+ T cells.Results Reovirus administration did not induce tumor-specific T cells but rather induced high frequencies of reovirus-specific CD8+ T cells directed to the immunodominant epitope. Priming of reovirus-specific T cells required a low-frequent population of cross-presenting dendritic cells which was absent in Batf3-/- mice. While intratumoral and intravenous reovirus administration induced equal systemic frequencies of reovirus-specific T cells, reovirus-specific T cells were highly enriched in the TME exclusively after intratumoral administration. Here, they displayed characteristics of potent effector cells with high expression of KLRG1, suggesting they may be responsive against local reovirus-infected cells. To exploit these reovirus-specific T cells as anticancer effector cells, we designed an SLP-based vaccination strategy to induce a strong T-cell response before virotherapy. These high frequencies of circulating reovirus-specific T cells were reactivated on intratumoral reovirus administration and significantly delayed tumor growth.Conclusions These findings provide proof of concept that OV-specific T cells, despite not being tumor-specific, can be exploited as potent effector cells for anticancer treatment when primed before virotherapy. This is an attractive strategy for low-immunogenic tumors lacking tumor-specific T cells.

Published
2022
Full Text
View/download PDF

35. Neurological Symptom Improvement After Re-Irradiation in Patients With Diffuse Intrinsic Pontine Glioma: A Retrospective Analysis of the SIOP-E-HGG/DIPG Project

Author

Lara Chavaz, Geert O. Janssens, Stephanie Bolle, Henry Mandeville, Monica Ramos-Albiac, Karen Van Beek, Helen Benghiat, Bianca Hoeben, Andres Morales La Madrid, Clemens Seidel, Rolf-Dieter Kortmann, Darren Hargrave, Lorenza Gandola, Emilia Pecori, Dannis G. van Vuurden, Veronica Biassoni, Maura Massimino, Christof M. Kramm, and Andre O. von Bueren

Subjects
diffuse intrinsic pontine glioma (DIPG), radiotherapy, re-irradiation (re-RT), child, adolescent, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

PurposeThe aim of this study is to investigate the spectrum of neurological triad improvement in patients with diffuse intrinsic pontine glioma (DIPG) treated by re-irradiation (re-RT) at first progression.MethodsWe carried out a re-analysis of the SIOP-E retrospective DIPG cohort by investigating the clinical benefits after re-RT with a focus on the neurological triad (cranial nerve deficits, ataxia, and long tract signs). Patients were categorized as “responding” or “non-responding” to re-RT. To assess the interdependence between patients’ characteristics and clinical benefits, we used a chi-square or Fisher’s exact test. Survival according to clinical response to re-RT was calculated by the Kaplan–Meier method.ResultsAs earlier reported, 77% (n = 24/31) of patients had any clinical benefit after re-RT. Among 25/31 well-documented patients, 44% (n = 11/25) had improvement in cranial nerve palsies, 40% (n = 10/25) had improvement in long-tract signs, and 44% (11/25) had improvement in cerebellar signs. Clinical benefits were observed in at least 1, 2, or 3 out of 3 symptoms of the DIPG triad, in 64%, 40%, and 24%, respectively. Patients irradiated with a dose ≥20 Gy versus

Published
2022
Full Text
View/download PDF

36. Tumor-Educated Platelet RNA for the Detection and (Pseudo)progression Monitoring of Glioblastoma

Author

Sol, Nik, in ‘t Veld, Sjors G.J.G., Vancura, Adrienne, Tjerkstra, Maud, Leurs, Cyra, Rustenburg, François, Schellen, Pepijn, Verschueren, Heleen, Post, Edward, Zwaan, Kenn, Ramaker, Jip, Wedekind, Laurine E., Tannous, Jihane, Ylstra, Bauke, Killestein, Joep, Mateen, Farrah, Idema, Sander, de Witt Hamer, Philip C., Navis, Anna C., Leenders, William P.J., Hoeben, Ann, Moraal, Bastiaan, Noske, David P., Vandertop, W. Peter, Nilsson, R. Jonas A., Tannous, Bakhos A., Wesseling, Pieter, Reijneveld, Jaap C., Best, Myron G., and Wurdinger, Thomas

Published
2020
Full Text
View/download PDF

41. Disease‐induced and treatment‐induced alterations in body composition in locally advanced head and neck squamous cell carcinoma

Author

Anna C.H. Willemsen, Ann Hoeben, Roy I. Lalisang, Ardy Van Helvoort, Frederik W.R. Wesseling, Frank Hoebers, Laura W.J. Baijens, and Annemie M.W.J. Schols

Subjects
Muscle wasting, Cancer cachexia, Head and neck, Chemoradiation, Bioradiation, Tube feeding, Diseases of the musculoskeletal system, RC925-935, Human anatomy, QM1-695
Abstract

Abstract Background Chemoradiation or bioradiation treatment (CRT/BRT) of locally advanced head and neck squamous cell carcinoma (LAHNSCC) comes with high toxicity rates, often leading to temporary tube feeding (TF) dependency. Cachexia is a common problem in LAHNSCC. Yet changes in body composition and muscle weakness during CRT/BRT are underexplored. Strong evidence on the effect of TF on body composition during treatment is lacking. The aim of this cohort study was to assess (i) the relationship of fat‐free mass index (FFMI) and handgrip strength (HGS) with CRT/BRT toxicity and outcome, (ii) body composition in patients treated with chemoradiation (cisplatin) vs. bioradiation (cetuximab), and (iii) the effect of the current TF regime on body composition and muscle strength. Methods Locally advanced head and neck squamous cell carcinoma patients treated with CRT/BRT between January 2013 and December 2016 were included (n = 137). Baseline measurements of body composition (bioelectrical impedance analysis) and HGS were performed. Toxicity grades (Common Terminology Criteria for Adverse Events) were scored. In a subset of 69 patients, weight loss, body composition, and HGS were additionally assessed during and after CRT/BRT. TF was initiated according to the Dutch guidelines for malnutrition. Results In this cohort (68% male, mean age 59 ± 8 years), the incidence of baseline muscle wasting, defined as FFMI < P10, was 29%. Muscle wasting was present in 23 of 100 (23%) chemoradiation patients and 17 of 37 (46%) bioradiation patients (P = 0.009). Muscle‐wasted patients required more unplanned hospitalizations during CRT (P = 0.035). In the chemoradiation subset, dose‐limiting toxicity was significantly higher in wasted vs. non‐wasted patients (57% vs. 25%, P = 0.004). Median follow‐up was 32 months. Multivariate Cox regression analysis identified muscle wasting as independent unfavourable prognostic factor for overall survival [hazard ratio 2.1 (95% CI 1.1–4.1), P = 0.022] and cisplatin as favourable prognostic factor [hazard ratio 0.3 (95% CI 0.2–0.6), P = 0.001]. Weight and HGS significantly decreased during CRT/BRT, −3.7 ± 3.5 kg (P < 0.001) and −3.1 ± 6.0 kg (P < 0.001), respectively. Sixty‐four per cent of the patients required TF 21 days (range 0–59) after CRT/BRT initiation. Total weight loss during CRT/BRT was significantly (P = 0.007) higher in the total oral diet group (5.5 ± 3.7 kg) compared with the TF group (3.0 ± 3.2 kg). Loss of FFM and HGS was similar in both groups. Conclusions In LAHNSCC patients undergoing CRT/BRT, FFMI < P10 is an unfavourable prognostic factor for overall survival, treatment toxicity, and tolerance. Patients experience significant weight and FFM loss during treatment. Current TF regime attenuates weight loss but does not overcome loss of muscle mass and function during therapy. Future interventions should consider nutritional intake and additional strategies specifically targeting metabolism, loss of muscle mass, and function.

Published
2020
Full Text
View/download PDF

42. Technical recommendations for implementation of Volumetric Modulated Arc Therapy and Helical Tomotherapy Total Body Irradiation

Author

Klinische Fysica RT, Cancer, MS Radiotherapie, Seravalli, Enrica, Bosman, Mirjam E, Han, Chunhui, Losert, Christoph, Pazos, Montserrat, Engström, Per E, Engellau, Jacob, Fulcheri, Christian P L, Zucchetti, Claudio, Saldi, Simonetta, Ferrer, Carlos, Ocanto, Abrahams, Hiniker, Susan M, Clark, Catharine H, Hussein, Mohammad, Misson-Yates, Sarah, Kobyzeva, Daria A, Loginova, Anna A, Hoeben, Bianca A W, Klinische Fysica RT, Cancer, MS Radiotherapie, Seravalli, Enrica, Bosman, Mirjam E, Han, Chunhui, Losert, Christoph, Pazos, Montserrat, Engström, Per E, Engellau, Jacob, Fulcheri, Christian P L, Zucchetti, Claudio, Saldi, Simonetta, Ferrer, Carlos, Ocanto, Abrahams, Hiniker, Susan M, Clark, Catharine H, Hussein, Mohammad, Misson-Yates, Sarah, Kobyzeva, Daria A, Loginova, Anna A, and Hoeben, Bianca A W

Published
2024

43. Air- & spacepower: back to the basics!

Author

Hoeben, B.A. ; Benning, R.C.I.P. and Hoeben, B.A. ; Benning, R.C.I.P.

Abstract

De oorlog in Oekraïne heeft de afgelopen twee jaar veel stof tot nadenken opgeleverd. Allereerst natuurlijk humanitair en geopolitiek. Maar daarnaast is de oorlog voor de NAVO en haar lidstaten een flinke wake-up call: de militaire dreiging die uitging en -gaat van de Russische Federatie (RF) is op het Europese continent tot realiteit geworden. Daarmee ontstaat onoverkomelijk de discussie hoe deze veiligheidsdreiging de kop te bieden. De gruwelijke strijd op het slagveld in en boven Oekraïne, veelal vergeleken met de Eerste Wereldoorlog (WO I), is daarmee ook studieobject geworden: welke lessen moeten wij leren uit deze oorlog om ons te wapenen tegen een mogelijke Russische aanval op een NAVO-bondgenoot?

Published
2024

44. Tobacco smoking is associated with sex- and plaque-type specific upregulation of CRLF1 in atherosclerotic lesions

Author

CDL Onderzoek Pasterkamp, Experimental Cardiology Laboratory, Experimentele Afd. Cardiologie 1, Circulatory Health, Zorgeenheid Vaatchirurgie Medisch, Onderzoek Vrouw Hart & Vaatziekten, Centraal Diagnostisch Laboratorium, Child Health, Lan, Tian, Palm, Kaylin C.A., Hoeben, Luka, Diez Benavente, Ernest, Perry, R. Noah, Civelek, Mete, de Kleijn, Dominique P.V., den Ruijter, Hester M., Pasterkamp, Gerard, Mokry, Michal, CDL Onderzoek Pasterkamp, Experimental Cardiology Laboratory, Experimentele Afd. Cardiologie 1, Circulatory Health, Zorgeenheid Vaatchirurgie Medisch, Onderzoek Vrouw Hart & Vaatziekten, Centraal Diagnostisch Laboratorium, Child Health, Lan, Tian, Palm, Kaylin C.A., Hoeben, Luka, Diez Benavente, Ernest, Perry, R. Noah, Civelek, Mete, de Kleijn, Dominique P.V., den Ruijter, Hester M., Pasterkamp, Gerard, and Mokry, Michal

Published
2024

46. Efficacy of pembrolizumab and biomarker analysis in patients with WGS-based intermediate to high tumor mutational load: results from the Drug Rediscovery Protocol

Author

Palliatieve Zorg, Pathologie Moleculair, Pathologie Pathologen staf, Cancer, Externen Med. Onco, Geurts, Birgit S, Zeverijn, Laurien J, Leek, Lindsay V M, van Berge Henegouwen, Jade M, Hoes, Louisa R, van der Wijngaart, Hanneke, van der Noort, Vincent, van de Haar, Joris, van Ommen-Nijhof, Annemiek, Kok, Marleen, Roepman, Paul, Jansen, Anne M L, de Leng, Wendy W J, de Jonge, Maja J A, Hoeben, Ann, van Herpen, Carla M L, Westgeest, Hans M, Wessels, Lodewyk F A, Verheul, Henk M W, Gelderblom, Hans, Voest, Emile E, Palliatieve Zorg, Pathologie Moleculair, Pathologie Pathologen staf, Cancer, Externen Med. Onco, Geurts, Birgit S, Zeverijn, Laurien J, Leek, Lindsay V M, van Berge Henegouwen, Jade M, Hoes, Louisa R, van der Wijngaart, Hanneke, van der Noort, Vincent, van de Haar, Joris, van Ommen-Nijhof, Annemiek, Kok, Marleen, Roepman, Paul, Jansen, Anne M L, de Leng, Wendy W J, de Jonge, Maja J A, Hoeben, Ann, van Herpen, Carla M L, Westgeest, Hans M, Wessels, Lodewyk F A, Verheul, Henk M W, Gelderblom, Hans, and Voest, Emile E

Published
2024

47. What Adolescents Do or Say to Actively Influence Peers:Compliance-Gaining Tactics and Adolescent Deviance

Author

Hoeben, Evelien M., Ten Cate, Maartje A., Weerman, Frank M., McGloin, Jean Marie, Hoeben, Evelien M., Ten Cate, Maartje A., Weerman, Frank M., and McGloin, Jean Marie

Abstract

Objectives: Despite abundant evidence of deviant peer influence, it remains unclear precisely how adolescents try to exert such influence. What do adolescents do or say to actively encourage or discourage deviance among their peers? The aim of the current study is to explore the different ways in which adolescents talk each other into—or out of—such behaviors. Methods: We analyzed narratives about delinquency (N = 37), substance use (N = 131), and other deviance (N = 107), which were written by adolescents (ages 14–18) in secondary schools. The study combines criminological perspectives on situational group processes (i.e., instigation, reinforcement, and provocation) with insights on compliance-gaining from other disciplines to inform a qualitative investigation of key influence tactics. Results: Our results demonstrate that adolescents use a number of tactics to encourage and discourage deviance. Many of these same tactics are used to promote prosocial behavior, though provocation-like tactics are largely used to encourage deviance. Conclusions: The range of reported compliance tactics extends well beyond what is captured in typical studies of peer influence, largely revolving around the broader themes of instigation and attempts to impact the anticipated risks, costs, and rewards of behavior. Ultimately, this study underscores the multi-faceted, socially interactive nature of peer influence.

Published
2024

48. Characterization of a hyperbolic vortex plasma reactor for the removal of aqueous phase micropollutants

Author

Klymenko, Roman, de Kroon, Esther, Agosthinho, Luewton, Fuchs, Elmar, Woisetschläger, Jakob, Hoeben, Wilfred F.L.M., Klymenko, Roman, de Kroon, Esther, Agosthinho, Luewton, Fuchs, Elmar, Woisetschläger, Jakob, and Hoeben, Wilfred F.L.M.

Abstract

The present study focuses on the characterization of a hyperbolic vortex plasma reactor through the comparison of various plasma-atmospheric regimes for the production efficiency of reactive nitrogen (RNS) and reactive oxygen (ROS) species. The research also explores effectiveness in the removal of micropollutants, including pharmaceuticals and per- and polyfluoroalkyl substances (PFAS). The technology includes several degradation mechanisms, such as advanced oxidation, ultraviolet photolysis, ozonation, electrolysis, and shockwave water purification, without the need for additional chemicals. Our results indicate that the plasma of bipolar or ‘flashover’ mode is notably more effective and efficient than both positive or negative polarity. Through the testing of various energy levels, it has been demonstrated that higher energy plasma yields lower efficiency but necessitates shorter treatment times compared to lower energy treatment. When plasma is produced under ambient atmosphere, water chemical properties change significantly in comparison to treatment under argon (Ar) or nitrogen (N2) due to the presence of both oxygen and N2 molecules. In a N2 atmosphere, the predominant formation is of RNS due to the chemical reactivity of N2 exited states, whereas under Ar atmosphere, predominantly ROS are generated. Notable advantages of this technology are its scalability and its low energy requirements. The scalability of the technology involves increasing the size of the reactor, the power and electrode count.

Published
2024

49. Efficacy and Safety of Panitumumab in Patients With RAF/RAS-Wild-Type Glioblastoma:Results From the Drug Rediscovery Protocol

Author

Spiekman, Ilse A. C., Geurts, Birgit S., Zeverijn, Laurien J., de Wit, Gijs F., van der Noort, Vincent, Roepman, Paul, de Leng, Wendy W. J., Jansen, Anne M. L., Kusters, Benno, Beerepoot, Laurens, de Vos, Filip Y. F. L., de Groot, Derk-Jan A., de Groot, Jan Willem B., Hoeben, Ann, Buter, Jan, Gelderblom, Hans A. J., Voest, Emile E., Verheul, Henk M. W., Spiekman, Ilse A. C., Geurts, Birgit S., Zeverijn, Laurien J., de Wit, Gijs F., van der Noort, Vincent, Roepman, Paul, de Leng, Wendy W. J., Jansen, Anne M. L., Kusters, Benno, Beerepoot, Laurens, de Vos, Filip Y. F. L., de Groot, Derk-Jan A., de Groot, Jan Willem B., Hoeben, Ann, Buter, Jan, Gelderblom, Hans A. J., Voest, Emile E., and Verheul, Henk M. W.

Abstract

BACKGROUND: The prognosis of malignant primary high-grade brain tumors, predominantly glioblastomas, is poor despite intensive multimodality treatment options. In more than 50% of patients with glioblastomas, potentially targetable mutations are present, including rearrangements, altered splicing, and/or focal amplifications of epidermal growth factor receptor (EGFR) by signaling through the RAF/RAS pathway. We studied whether treatment with the clinically available anti-EGFR monoclonal antibody panitumumab provides clinical benefit for patients with RAF/RAS-wild-type (wt) glioblastomas in the Drug Rediscovery Protocol (DRUP). METHODS: Patients with progression of treatment refractory RAF/RASwt glioblastoma were included for treatment with panitumumab in DRUP when measurable according to RANO criteria. The primary endpoints of this study are clinical benefit (CB: defined as confirmed objective response [OR] or stable disease [SD] ≥ 16 weeks) and safety. Patients were enrolled using a Simon-like 2-stage model, with 8 patients in stage 1 and up to 24 patients in stage 2 if at least 1 in 8 patients had CB in stage 1. RESULTS: Between 03-2018 and 02-2022, 24 evaluable patients were treated. CB was observed in 5 patients (21%), including 2 patients with partial response (8.3%) and 3 patients with SD ≥ 16 weeks (12.5%). After median follow-up of 15 months, median progression-free survival and overall survival were 1.7 months (95% CI 1.6-2.1 months) and 4.5 months (95% CI 2.9-8.6 months), respectively. No unexpected toxicities were observed. CONCLUSIONS: Panitumumab treatment provides limited CB in patients with recurrent RAF/RASwt glioblastoma precluding further development of this therapeutic strategy.

Published
2024

50. Efficacy and Safety of Panitumumab in Patients With RAF/RAS-Wild-Type Glioblastoma: Results From the Drug Rediscovery Protocol

Author

Pathologie Pathologen staf, Cancer, Pathologie Moleculair, MS Medische Oncologie, Brain, Spiekman, Ilse A C, Geurts, Birgit S, Zeverijn, Laurien J, de Wit, Gijs F, van der Noort, Vincent, Roepman, Paul, de Leng, Wendy W J, Jansen, Anne M L, Kusters, Benno, Beerepoot, Laurens V, de Vos, Filip Y F L, de Groot, Derk-Jan A, de Groot, Jan Willem B, Hoeben, Ann, Buter, Jan, Gelderblom, Hans A J, Voest, Emile E, Verheul, Henk M W, Pathologie Pathologen staf, Cancer, Pathologie Moleculair, MS Medische Oncologie, Brain, Spiekman, Ilse A C, Geurts, Birgit S, Zeverijn, Laurien J, de Wit, Gijs F, van der Noort, Vincent, Roepman, Paul, de Leng, Wendy W J, Jansen, Anne M L, Kusters, Benno, Beerepoot, Laurens V, de Vos, Filip Y F L, de Groot, Derk-Jan A, de Groot, Jan Willem B, Hoeben, Ann, Buter, Jan, Gelderblom, Hans A J, Voest, Emile E, and Verheul, Henk M W

Published
2024

Catalog

Books, media, physical & digital resources
See catalog results