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2. Real-world data on the management of pazopanib-induced liver toxicity in routine care of renal cell cancer and soft tissue sarcoma patients

Author

Westerdijk, K., Krens, S. D., Steeghs, N., van der Graaf, W. T. A., Tjwa, E. T. T. L., Westdorp, H., Desar, I. M. E., van Erp, N. P., Westerdijk, K., Krens, S. D., Steeghs, N., van der Graaf, W. T. A., Tjwa, E. T. T. L., Westdorp, H., Desar, I. M. E., and van Erp, N. P.

Abstract

PurposePazopanib is known to cause liver toxicity. A relationship between pazopanib exposure and alanine transaminase elevations has been described in clinical trials. This study investigated the relation between pazopanib exposure and liver toxicity in real-world patients and evaluated the management of pazopanib-induced liver toxicity in routine care.MethodsA retrospective observational cohort study was performed in patients treated with pazopanib in whom pazopanib exposure was measured. The percentage of patients with and without liver toxicity during treatment with pazopanib was calculated as well as the average pazopanib exposure in both groups. Furthermore, the management of patients with liver toxicity was evaluated.ResultsLiver toxicity was observed in 25 out of the 133 patients included (19%). Pazopanib exposure was comparable in patients with or without liver toxicity (27.7 mg/L versus 28.1 mg/L). Seven patients permanently discontinued pazopanib after the occurrence of liver toxicity. Of the remaining 18 patients, continuation or restart of pazopanib after liver toxicity was successful in 16 patients and half of these patients were able to safely continue pazopanib at the same dose as prior to liver toxicity for the remaining duration of treatment.ConclusionOur study did not demonstrate a clear relationship between pazopanib exposure and the occurrence of pazopanib-induced liver toxicity. Half of the patients were able to safely continue or restart pazopanib treatment after liver toxicity and received the same dose as prior to drug withdrawal. Successful interventions to address pazopanib-induced toxicity in the clinic led to an algorithm for the management of pazopanib-induced liver toxicity.

Published
2024

4. Kidney absorbed radiation doses for [ 177 Lu]Lu-PSMA-617 and [ 177 Lu]Lu-PSMA-I&T determined by 3D clinical dosimetry.

Author

Uijen, M.J.M., Privé, B.M., Herpen, C.M.L. van, Westdorp, H., Gemert, W.A.M. van, Bakker, Maarten de, Gotthardt, M., Konijnenberg, M.W., Peters, S.M.B., Nagarajah, J., Uijen, M.J.M., Privé, B.M., Herpen, C.M.L. van, Westdorp, H., Gemert, W.A.M. van, Bakker, Maarten de, Gotthardt, M., Konijnenberg, M.W., Peters, S.M.B., and Nagarajah, J.

Abstract

Item does not contain fulltext, PURPOSE: For prostate-specific membrane antigen-directed radioligand therapy (PSMA-RLT), [ 177 Lu]Lu-PSMA-617 and [ 177 Lu]Lu-PSMA-I&T are the currently preferred compounds. Recent preclinical studies suggested ~30x higher kidney absorbed dose for [ 177 Lu]Lu-PSMA-I&T compared to [ 177 Lu]Lu-PSMA-617, which may lead to an increased risk of kidney toxicity. We performed two single-centre, prospective dosimetry studies with either [ 177 Lu]Lu-PSMA-617 or [ 177 Lu]Lu-PSMA-I&T, using an identical dosimetry protocol. We evaluated the absorbed doses of both 177 Lu-labelled radioligands in human kidneys. METHODS: 3D SPECT/computed tomography (CT) imaging of the kidneys was performed after PSMA-RLT in cancer patients with PSMA-positive disease and an adequate glomerular filtration rate (≥50 mL/min). Ten metastatic hormone-sensitive prostate cancer patients (mHSPC) were treated with [ 177 Lu]Lu-PSMA-617 and 10 advanced salivary gland cancer (SGC) patients were treated with [ 177 Lu]Lu-PSMA-I&T. SPECT/CT imaging was performed at five timepoints (1 h, 24 h, 48 h, 72 h, and 168 h post-injection). In mHSPC patients, SPECT/CT imaging was performed after cycles 1 and 2 (cumulative activity: 9 GBq) and in SGC patients only after cycle 1 (activity: 7.4 GBq). Kidney absorbed dose was calculated using organ-based dosimetry. RESULTS: The median kidney absorbed dose was 0.49 Gy/GBq (range: 0.34-0.66) and 0.73 Gy/GBq (range: 0.42-1.31) for [ 177 Lu]Lu-PSMA-617 and [ 177 Lu]Lu-PSMA-I&T, respectively (independent samples t test; P = 0.010). CONCLUSION: This study shows that the kidney absorbed dose for [ 177 Lu]Lu-PSMA-617 and [ 177 Lu]Lu-PSMA-I&T differs, with a ~1.5x higher median kidney absorbed dose for [ 177 Lu]Lu-PSMA-I&T. This difference in the clinical setting is considerably smaller than observed in preclinical studies and may not hamper treatments with [ 177 Lu]Lu-PSMA-I&T.

Published
2023

5. PSMA-RLT in Patients with Metastatic Hormone-Sensitive Prostate Cancer: A Retrospective Study

Author

Banda, A., Privé, B.M., Allach, Youssra, Uijen, M.J.M., Peters, S.M.B., Loeff, Cato C., Gotthardt, M., Muselaers, C.H.J., Witjes, J.A., Oort, I.M. van, Sedelaar, J.P.M., Westdorp, H., Mehra, N., Janssen, M.J.R., Gemert, W.A.M. van, Nagarajah, J., Banda, A., Privé, B.M., Allach, Youssra, Uijen, M.J.M., Peters, S.M.B., Loeff, Cato C., Gotthardt, M., Muselaers, C.H.J., Witjes, J.A., Oort, I.M. van, Sedelaar, J.P.M., Westdorp, H., Mehra, N., Janssen, M.J.R., Gemert, W.A.M. van, and Nagarajah, J.

Abstract

Item does not contain fulltext

Published
2023

6. Fibroblast activation protein-targeted radionuclide therapy: background, opportunities, and challenges of first (pre)clinical studies.

Author

Privé, B.M., Boussihmad, Mohamed A., Timmermans, Bart, Gemert, W.A.M. van, Peters, S.M.B., Derks, Y.H.W., Lith, S.A.M. van, Mehra, N., Nagarajah, J., Heskamp, S., Westdorp, H., Privé, B.M., Boussihmad, Mohamed A., Timmermans, Bart, Gemert, W.A.M. van, Peters, S.M.B., Derks, Y.H.W., Lith, S.A.M. van, Mehra, N., Nagarajah, J., Heskamp, S., and Westdorp, H.

Abstract

01 juni 2023, Item does not contain fulltext, INTRODUCTION: Fibroblast activation protein (FAP) is highly overexpressed in stromal tissue of various cancers. While FAP has been recognized as a potential diagnostic or therapeutic cancer target for decades, the surge of radiolabeled FAP-targeting molecules has the potential to revolutionize its perspective. It is presently hypothesized that FAP targeted radioligand therapy (TRT) may become a novel treatment for various types of cancer. To date, several preclinical and case series have been reported on FAP TRT using varying compounds and showing effective and tolerant results in advanced cancer patients. Here, we review the current (pre)clinical data on FAP TRT and discuss its perspective towards broader clinical implementation. METHODS: A PubMed search was performed to identify all FAP tracers used for TRT. Both preclinical and clinical studies were included if they reported on dosimetry, treatment response or adverse events. The last search was performed on July 22 2022. In addition, a database search was performed on clinical trial registries (date 15(th) of July 2022) to search for prospective trials on FAP TRT. RESULTS: In total, 35 papers were identified that were related to FAP TRT. This resulted in the inclusion of the following tracers for review: FAPI-04, FAPI-46, FAP-2286, SA.FAP, ND-bisFAPI, PNT6555, TEFAPI-06/07, FAPI-C12/C16, and FSDD. CONCLUSION: To date, data was reported on more than 100 patients that were treated with different FAP targeted radionuclide therapies such as [(177)Lu]Lu-FAPI-04, [(90)Y]Y-FAPI-46, [(177)Lu]Lu-FAP-2286, [(177)Lu]Lu-DOTA.SA.FAPI and [(177)Lu]Lu-DOTAGA.(SA.FAPi)(2). In these studies, FAP targeted radionuclide therapy has resulted in objective responses in difficult to treat end stage cancer patients with manageable adverse events. Although no prospective data is yet available, these early data encourages further research.

Published
2023

7. Case Report: Imaging immune checkpoint inhibitor-induced yin-yang effects in the brain.

Author

Bol, K.F., Peeters, E., Herpen, C.M.L. van, Westdorp, H., Aarntzen, E.H.J.G., Bol, K.F., Peeters, E., Herpen, C.M.L. van, Westdorp, H., and Aarntzen, E.H.J.G.

Abstract

Contains fulltext : 293889.pdf (Publisher’s version ) (Open Access), BACKGROUND: Treatment with immune checkpoint inhibitors (ICI) can induce durable responses in cancer patients, but it is commonly associated with serious immune-related side effects. Both effects are suggested to be mediated by CD8+ T-cell infiltration. Whole body CD8+ T-cell distribution can be visualized by PET imaging of a 89Zr-labeled anti-humanCD8a minibody, currently investigated in a phase 2b trial. MAIN BODY: An adult patient diagnosed with metastatic melanoma developed ICI-related hypophysitis after two courses of combined immunotherapy (ipilimumab (3 mg/kg) and nivolumab (1 mg/kg) at 3 weeks interval). On a [(89)Zr]Zr-crefmirlimab berdoxam PET/CT scan, made 8 days before clinical symptoms occurred, increased CD8+ T-cell infiltration in the pituitary gland was detected. Simultaneously, tracer uptake in a cerebral metastasis was increased, indicating ICI-induced tumor infiltration by CD8+ T-cells. CONCLUSIONS: The observations in this case report underscore the role of CD8+ T-cell in non-tumor tissues in ICI-related toxicity. In addition, it illustrates a potential role for molecular imaging by PET/CT for investigation and monitoring of ICI-induced effects.

Published
2023

8. Case Report: A severe case of immunosuppressant-refractory immune checkpoint inhibitor-mediated colitis rescued by tofacitinib.

Author

Sweep, M.W.D., Tjan, Martijn J.H., Gorris, M.A.J., Bol, K.F., Westdorp, H., Sweep, M.W.D., Tjan, Martijn J.H., Gorris, M.A.J., Bol, K.F., and Westdorp, H.

Abstract

Contains fulltext : 294755.pdf (Publisher’s version ) (Open Access), Immune checkpoint inhibitor therapy for cancer treatment can give rise to a variety of adverse events. Here we report a male patient with metastatic melanoma who experienced life-threatening colitis and duodenitis following treatment with ipilimumab and nivolumab. The patient did not respond to the first three lines of immunosuppressive therapy (corticosteroids, infliximab, and vedolizumab), but recovered well after administration of tofacitinib, a JAK inhibitor. Cellular and transcriptional data on colon and duodenum biopsies shows significant inflammation in the tissue, characterized by a large number of CD8 T cells and high expression of PD-L1. While cellular numbers do decrease during three lines of immunosuppressive therapy, CD8 T cells remain relatively high in the epithelium, along with PD-L1 expression in the involved tissue and expression of colitis-associated genes, indicating an ongoing colitis at that moment. Despite all immunosuppressive treatments, the patient has an ongoing tumor response with no evidence of disease. Tofacitinib might be a good candidate to consider more often for ipilimumab/nivolumab-induced colitis.

Published
2023

9. Tumoral Ki67 and PSMA Expression in Fresh Pre-PSMA-RLT Biopsies and Its Relation With PSMA-PET Imaging and Outcomes of PSMA-RLT in Patients With mCRPC

Author

Laarhuis, B.I., Janssen, M.J.R., Simons, M., Kalmthout, L.W.M. van, Doelen, M.J. van der, Peters, S.M.B., Westdorp, H., Oort, I.M. van, Litjens, G.J., Gotthardt, M., Nagarajah, J., Mehra, N., Privé, B.M., Laarhuis, B.I., Janssen, M.J.R., Simons, M., Kalmthout, L.W.M. van, Doelen, M.J. van der, Peters, S.M.B., Westdorp, H., Oort, I.M. van, Litjens, G.J., Gotthardt, M., Nagarajah, J., Mehra, N., and Privé, B.M.

Abstract

Contains fulltext : 297327.pdf (Publisher’s version ) (Open Access), INTRODUCTION: Prostate specific membrane antigen (PSMA) directed radioligand therapy (RLT) is a novel therapy for metastatic castration-resistant prostate cancer (mCRPC) patients. However, it is still poorly understood why approximately 40% of the patients does not respond to PSMA-RLT. The aims of this study were to evaluate the pretreatment PSMA expression on immunohistochemistry (IHC) and PSMA uptake on PET/CT imaging in mCRPC patients who underwent PSMA-RLT. We correlated these parameters and a cell proliferation marker (Ki67) to the therapeutic efficacy of PSMA-RLT. PATIENTS AND METHODS: In this retrospective study, mCRPC patients who underwent PSMA-RLT were analyzed. Patients biopsies were scored for immunohistochemical Ki67 expression, PSMA staining intensity and percentage of cells with PSMA expression. Moreover, the PSMA tracer uptake of the tumor lesion(s) and healthy organs on PET/CT imaging was assessed. The primary outcome was to evaluate the association between histological PSMA protein expression of tumor in pre-PSMA-RLT biopsies and the PSMA uptake on PSMA PET/CT imaging of the biopsied lesion. Secondary outcomes were to assess the relationship between PSMA expression and Ki67 on IHC and the progression free survival (PFS) and overall survival (OS) following PSMA-RLT. RESULTS: In total, 22 mCRPC patients were included in this study. Nineteen (86%) patients showed a high and homogenous PSMA expression of >80% on IHC. Three (14%) patients had low PSMA expression on IHC. Although there was limited PSMA uptake on PET/CT imaging, these 3 patients had lower PSMA uptake on PET/CT imaging compared to the patients with high PSMA expression on IHC. Yet, no correlation was found between PSMA uptake on PET/CT imaging and PSMA expression on IHC (SUVmax: R(2) = 0.046 and SUVavg: R(2) = 0.036). The 3 patients had a shorter PFS compared to the patients with high PSMA expression on IHC (HR: 4.76, 95% CI: 1.14-19.99; P = .033). Patients with low Ki67 expression had a l

Published
2023

10. 1388P Interim safety analysis of nivolumab 3mg/kg and ipilimumab 1mg/kg (nivo3/ipi1) in molecular-selected patients (pts) with metastastic castration-resistant prostate cancer (mCRPC)

Author

van Wilpe, S., primary, Westdorp, H., additional, Kloots, I.S.H., additional, Slootbeek, P., additional, den Brok, M., additional, Adema, G., additional, Kerkmeijer, L., additional, Smeenk, R.J., additional, Coskunturk, M., additional, Bloemendal, H., additional, Schalken, J., additional, Erp, N.V., additional, Gerritsen, W.R., additional, and Mehra, N., additional

Published
2022
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14. 642TiP Phase II CA184-585 (INSPIRE) trial of ipilimumab with nivolumab for molecular-selected patients with castration-resistant prostate cancer

Author

Mehra, N., primary, Kloots, I., additional, Slootbeek, P., additional, Brok, M. den, additional, Adema, G., additional, Kerkmeijer, L., additional, Smeenk, R.J., additional, Westdorp, H., additional, Bloemendal, H., additional, Schalken, J., additional, van Erp, N.P., additional, Binder, M., additional, De Vries, J., additional, and Gerritsen, W., additional

Published
2021
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15. Update to a randomized controlled trial of lutetium-177-PSMA in Oligo-metastatic hormone-sensitive prostate cancer: the BULLSEYE trial

Author

Privé, B.M., Janssen, M.J.R., Oort, I.M. van, Muselaers, C.H.J., Jonker, M.A., Gemert, W.A. van, Groot, M. de, Westdorp, H., Mehra, N., Verzijlbergen, J.F., Scheenen, T.W.J., Zámecnik, P., Barentsz, J.O., Gotthardt, M., Noordzij, W., Vogel, W.V., Bergman, A.M., Poel, H.G. van der, Vis, Andre N., Oprea-Lager, D.E., Gerritsen, W.R., Witjes, J.A., Nagarajah, J., Privé, B.M., Janssen, M.J.R., Oort, I.M. van, Muselaers, C.H.J., Jonker, M.A., Gemert, W.A. van, Groot, M. de, Westdorp, H., Mehra, N., Verzijlbergen, J.F., Scheenen, T.W.J., Zámecnik, P., Barentsz, J.O., Gotthardt, M., Noordzij, W., Vogel, W.V., Bergman, A.M., Poel, H.G. van der, Vis, Andre N., Oprea-Lager, D.E., Gerritsen, W.R., Witjes, J.A., and Nagarajah, J.

Abstract

Contains fulltext : 244316.pdf (Publisher’s version ) (Open Access), BACKGROUND: The BULLSEYE trial is a multicenter, open-label, randomized controlled trial to test the hypothesis if (177)Lu-PSMA is an effective treatment in oligometastatic hormone-sensitive prostate cancer (oHSPC) to prolong the progression-free survival (PFS) and postpone the need for androgen deprivation therapy (ADT). The original study protocol was published in 2020. Here, we report amendments that have been made to the study protocol since the commencement of the trial. CHANGES IN METHODS AND MATERIALS: Two important changes were made to the original protocol: (1) the study will now use (177)Lu-PSMA-617 instead of (177)Lu-PSMA-I&T and (2) responding patients with residual disease on (18)F-PSMA PET after the first two cycles are eligible to receive additional two cycles of 7.4 GBq (177)Lu-PSMA in weeks 12 and 18, summing up to a maximum of 4 cycles if indicated. Therefore, patients receiving (177)Lu-PSMA-617 will also receive an interim (18)F-PSMA PET scan in week 4 after cycle 2. The title of this study was modified to; "Lutetium-177-PSMA in Oligo-metastatic Hormone Sensitive Prostate Cancer" and is now partly supported by Advanced Accelerator Applications, a Novartis Company. CONCLUSIONS: We present an update of the original study protocol prior to the completion of the study. Treatment arm patients that were included and received (177)Lu-PSMA-I&T under the previous protocol will be replaced. TRIAL REGISTRATION: ClinicalTrials.gov NCT04443062 . First posted: June 23, 2020.

Published
2021

16. Immunophenotyping Reveals Longitudinal Changes in Circulating Immune Cells During Radium-223 Therapy in Patients With Metastatic Castration-Resistant Prostate Cancer

Author

Creemers, J.H.A., Doelen, M.J. van der, Wilpe, S. van, Hermsen, Rick, Duiveman-de Boer, T., Somford, Diederik M., Janssen, M.J.R., Mehra, N., Textor, J.C., Westdorp, H., Creemers, J.H.A., Doelen, M.J. van der, Wilpe, S. van, Hermsen, Rick, Duiveman-de Boer, T., Somford, Diederik M., Janssen, M.J.R., Mehra, N., Textor, J.C., and Westdorp, H.

Abstract

Contains fulltext : 233864.pdf (Publisher’s version ) (Open Access)

Published
2021

17. Immune Checkpoint Inhibitor-related Guillain-Barré Syndrome: A Case Series and Review of the Literature

Author

Janssen, J.B.E., Leow, T.Y., Herbschleb, K.H., Gijtenbeek, J.M.M., Boers-Sonderen, M.J., Gerritsen, W.R., Westdorp, H., Janssen, J.B.E., Leow, T.Y., Herbschleb, K.H., Gijtenbeek, J.M.M., Boers-Sonderen, M.J., Gerritsen, W.R., and Westdorp, H.

Abstract

Item does not contain fulltext, Immune checkpoint inhibitors (ICIs) have been approved for the treatment of various malignancies with promising clinical outcomes. Treatment can, however, be accompanied by serious immune-related adverse events. Neurological adverse events like Guillain-Barré syndrome (GBS) are rare but potentially life-threatening. We present 3 cases of ICI-related GBS; review cases described in current literature, and discuss treatment strategies. Three patients developed GBS after ICI treatment. The first case with pembrolizumab had a fatal outcome despite treatment with multiple regimens, including steroids and intravenous immunoglobulin (IVIg). The other 2 cases with nivolumab-induced and pembrolizumab-induced GBS, respectively, responded well to treatment with IVIg and steroids. In the current literature, a total of 31 other cases were found. Treatment for ICI-related GBS mostly consisted of concurrent IVIg and steroids (44%), which led to clinical improvement in 73%. Most patients recovered with remaining symptoms (68%), while 10 patients developed respiratory failure (29%) and 6 patients (18%) died. ICI-related GBS should be suspected in patients on ICI treatment who develop subacute progressive weakness of the limbs, sensory loss, and areflexia. On the basis of the guidelines recommendations and our review of the literature, we advise first-line therapy with concurrent IVIg 0.4 g/kg/d for 5 days and prednisolone 1-2 mg/kg/d. Discontinuation of immunotherapy after ICI-related GBS is advised.

Published
2021

18. Mechanisms of Immune Checkpoint Inhibitor-Mediated Colitis

Author

Westdorp, H., Sweep, M.W.D., Gorris, M.A.J., Hoentjen, F., Boers-Sonderen, M.J., Post, R.S. van der, Heuvel, M.M. van den, Piet, B., Boleij, A., Bloemendal, H.J., Vries, I.J.M. de, Westdorp, H., Sweep, M.W.D., Gorris, M.A.J., Hoentjen, F., Boers-Sonderen, M.J., Post, R.S. van der, Heuvel, M.M. van den, Piet, B., Boleij, A., Bloemendal, H.J., and Vries, I.J.M. de

Abstract

Contains fulltext : 242610.pdf (Publisher’s version ) (Open Access), Immune checkpoint inhibitors (ICIs) have provided tremendous clinical benefit in several cancer types. However, systemic activation of the immune system also leads to several immune-related adverse events. Of these, ICI-mediated colitis (IMC) occurs frequently and is the one with the highest absolute fatality. To improve current treatment strategies, it is important to understand the cellular mechanisms that induce this form of colitis. In this review, we discuss important pathways that are altered in IMC in mouse models and in human colon biopsy samples. This reveals a complex interplay between several types of immune cells and the gut microbiome. In addition to a mechanistic understanding, patients at risk should be identifiable before ICI therapy. Here we propose to focus on T-cell subsets that interact with bacteria after inducing epithelial damage. Especially, intestinal resident immune cells are of interest. This may lead to a better understanding of IMC and provides opportunities for prevention and management.

Published
2021

19. Reinforcing the immune system against cancer

Author

Westdorp, H., Vries, I.J.M. de, Schreibelt, G., Oort, I.M. van, and Radboud University Nijmegen

Subjects
Radboud Institute for Molecular Life Sciences, Cancer development and immune defence [Radboudumc 2], Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2]
Abstract

Contains fulltext : 217496.pdf (Publisher’s version ) (Open Access) Radboud University, 20 augustus 2020 Promotor : Vries, I.J.M. de Co-promotores : Schreibelt, G., Oort, I.M. van

Published
2020

20. High Health-Related Quality of Life During Dendritic Cell Vaccination Therapy in Patients With Castration-Resistant Prostate Cancer

Author

Westdorp, H., Creemers, J.H.A., Oort, I.M. van, Mehra, N., Hins-de Bree, S.M., Figdor, C.G., Witjes, J.A., Schreibelt, G., Vries, I.J.M. de, Gerritsen, W.R., Ottevanger, P.B., Westdorp, H., Creemers, J.H.A., Oort, I.M. van, Mehra, N., Hins-de Bree, S.M., Figdor, C.G., Witjes, J.A., Schreibelt, G., Vries, I.J.M. de, Gerritsen, W.R., and Ottevanger, P.B.

Abstract

Contains fulltext : 229158.pdf (publisher's version ) (Open Access), BACKGROUND: Maintaining health-related quality of life (HRQoL) is highly desirable during systemic therapies for patients with castration-resistant prostate cancer (CRPC). Patient-reported outcome measures (PROs) were studied in our phase IIa trial on cellular-based immunotherapy with dendritic cells (DC). METHODS: We treated 21 chemo-naive asymptomatic or minimally symptomatic patients with CRPC with maximally three cycles of DC vaccinations (ClinicalTrials.gov, NCT02692976). Here, we report the impact of DC vaccination on HRQoL. PROs were assessed using the EORTC-QLQ-C30, the EORTC-QLQ-PR25, Checklist Individual Strength (CIS20-R), and Beck Depression Inventory Primary Care questionnaires. Short-term and long-term vaccine-related effects on HRQoL were studied. RESULTS: Questionnaires were collected at baseline (n=20), week 6 (n=19), week 12 (n=18), week 24 (n=13), week 50 (n=8) and week 100 (n=2). No clinically relevant differences in symptom-related outcome, functioning-related outcome, and Global Health Status were observed directly after the first cycle of DC vaccinations (week 6) and at follow-up (week 12) compared to baseline. HRQoL remained high throughout the vaccination cycle and six weeks afterward. In radiographic non-progressive patients, who continued DC vaccination, high HRQoL scores were observed up to one and two years after study enrolment. CONCLUSIONS: Patients with asymptomatic or minimally symptomatic CRPC show high HRQoL throughout DC-based immunotherapy. This is a clinically relevant finding in this older-aged patient population with advanced prostate cancer.

Published
2020

21. Reinforcing the immune system against cancer

Author

Vries, I.J.M. de, Schreibelt, G., Oort, I.M. van, Westdorp, H., Vries, I.J.M. de, Schreibelt, G., Oort, I.M. van, and Westdorp, H.

Abstract

Radboud University, 20 augustus 2020, Promotor : Vries, I.J.M. de Co-promotores : Schreibelt, G., Oort, I.M. van, Contains fulltext : 217496.pdf (publisher's version ) (Open Access)

Published
2020

22. Autologous monocyte-derived DC vaccination combined with cisplatin in stage III and IV melanoma patients: a prospective, randomized phase 2 trial

Author

Boudewijns, S, Bloemendal, M., Haas, N. de, Westdorp, H., Bol, K.F., Schreibelt, G., Aarntzen, E.H.J.G., Lesterhuis, W.J., Gorris, M.A.J., Croockewit, A.J., Woude, L.L. van der, Rossum, M.M. van, Welzen, M.E., Goede, A.L. de, Hato, S.V., Graaf, W.T.A. van der, Punt, C.J.A., Koornstra, R.H., Gerritsen, W.R., Figdor, C.G., Vries, I.J.M. de, Boudewijns, S, Bloemendal, M., Haas, N. de, Westdorp, H., Bol, K.F., Schreibelt, G., Aarntzen, E.H.J.G., Lesterhuis, W.J., Gorris, M.A.J., Croockewit, A.J., Woude, L.L. van der, Rossum, M.M. van, Welzen, M.E., Goede, A.L. de, Hato, S.V., Graaf, W.T.A. van der, Punt, C.J.A., Koornstra, R.H., Gerritsen, W.R., Figdor, C.G., and Vries, I.J.M. de

Abstract

Contains fulltext : 219652.pdf (Publisher’s version ) (Open Access), BACKGROUND: Autologous dendritic cell (DC) vaccines can induce tumor-specific T cells, but their effect can be counteracted by immunosuppressive mechanisms. Cisplatin has shown immunomodulatory effects in vivo which may enhance efficacy of DC vaccination. METHODS: This is a prospective, randomized, open-label phase 2 study (NCT02285413) including stage III and IV melanoma patients receiving 3 biweekly vaccinations of gp100 and tyrosinase mRNA-loaded monocyte-derived DCs with or without cisplatin. Primary objectives were to study immunogenicity and feasibility, and secondary objectives were to assess toxicity and survival. RESULTS: Twenty-two stage III and 32 stage IV melanoma patients were analyzed. Antigen-specific CD8(+) T cells were found in 44% versus 67% and functional T cell responses in 28% versus 19% of skin-test infiltrating lymphocytes in patients receiving DC vaccination with and without cisplatin, respectively. Four patients stopped cisplatin because of toxicity and continued DC monotherapy. No therapy-related grade 3 or 4 adverse events occurred due to DC monotherapy. During combination therapy, one therapy-related grade 3 adverse event, decompensated heart failure due to fluid overload, occurred. The clinical outcome parameters did not clearly suggest significant differences. CONCLUSIONS: Combination of DC vaccination and cisplatin in melanoma patients is feasible and safe, but does not seem to result in more tumor-specific T cell responses or improved clinical outcome, when compared to DC vaccination monotherapy.

Published
2020

23. Blood-derived dendritic cell vaccinations induce immune responses that correlate with clinical outcome in patients with chemo-naive castration-resistant prostate cancer

Author

Westdorp, H., Creemers, J.H.A., Oort, I.M. van, Schreibelt, G., Gorris, M.A.J., Mehra, N., Simons, M., Goede, A.L. de, Rossum, M.M. van, Croockewit, A.J., Figdor, C.G., Witjes, J.A., Aarntzen, E.H.J.G., Mus, R.D.M., Bruning, M., Petry, K., Gotthardt, M., Barentsz, J.O., Vries, I.J.M. de, Gerritsen, W.R., Westdorp, H., Creemers, J.H.A., Oort, I.M. van, Schreibelt, G., Gorris, M.A.J., Mehra, N., Simons, M., Goede, A.L. de, Rossum, M.M. van, Croockewit, A.J., Figdor, C.G., Witjes, J.A., Aarntzen, E.H.J.G., Mus, R.D.M., Bruning, M., Petry, K., Gotthardt, M., Barentsz, J.O., Vries, I.J.M. de, and Gerritsen, W.R.

Abstract

Contains fulltext : 215390.pdf (publisher's version ) (Open Access), BACKGROUND: Clinical benefit of cellular immunotherapy has been shown in patients with castration-resistant prostate cancer (CRPC). We investigated the immunological response and clinical outcome of vaccination with blood-derived CD1c(+) myeloid dendritic cells (mDCs; cDC2) and plasmacytoid DCs (pDCs). METHODS: In this randomized phase IIa trial, 21 chemo-naive CRPC patients received maximally 9 vaccinations with mature mDCs, pDCs or a combination of mDCs plus pDCs. DCs were stimulated with protamine/mRNA and loaded with tumor-associated antigens NY-ESO-1, MAGE-C2 and MUC1. Primary endpoint was the immunological response after DC vaccination, which was monitored in peripheral blood and in T cell cultures of biopsies of post-treatment delayed-type hypersensitivity-skin tests. Main secondary endpoints were safety, feasibility, radiological PFS (rPFS) and overall survival. Radiological responses were assessed by MRIs and contrast-enhanced (68)Ga-prostate-specific membrane antigen PET/CT, according to RECIST 1.1, PCWG2 criteria and immune-related response criteria. RESULTS: Both tetramer/dextramer-positive (dm(+)) and IFN-gamma-producing (IFN-gamma(+)) antigen specific T cells were detected more frequently in skin biopsies of patients with radiological non-progressive disease (5/13 patients; 38%) compared to patients with progressive disease (0/8 patients; 0%). In these patients with vaccination enhanced dm(+) and IFN-gamma(+) antigen-specific T cells median rPFS was 18.8 months (n = 5) vs. 5.1 months (n = 16) in patients without IFN-gamma-producing antigen-specific T cells (p = 0.02). The overall median rPFS was 9.5 months. All DC vaccines were well tolerated with grade 1-2 toxicity. CONCLUSIONS: Immunotherapy with blood-derived DC subsets was feasible and safe and induced functional antigen-specific T cells. The presence of functional antigen-specific T cells correlated with an improved clinical outcome. TRIAL REGISTRATION: ClinicalTrials.gov identifier NCT02692976, r

Published
2019

24. Health-related quality of life analysis in stage III melanoma patients treated with adjuvant dendritic cell therapy

Author

Bloemendal, M., Rietveld, M.J.A., Willigen, W.W. van, Gerritsen, W.R., Figdor, C.G., Bonenkamp, J.J., Westdorp, H., Boudewijns, S, Koornstra, R.H., Adang, E.M.M., Schreibelt, G., Ottevanger, P.B., Vries, I.J.M. de, Bol, K.F., Bloemendal, M., Rietveld, M.J.A., Willigen, W.W. van, Gerritsen, W.R., Figdor, C.G., Bonenkamp, J.J., Westdorp, H., Boudewijns, S, Koornstra, R.H., Adang, E.M.M., Schreibelt, G., Ottevanger, P.B., Vries, I.J.M. de, and Bol, K.F.

Abstract

Contains fulltext : 203875.pdf (Publisher’s version ) (Open Access)

Published
2019

25. Natural dendritic cell vaccinations generate immune responses that correlate with clinical outcome in patients with chemo-naive castration-resistant prostate cancer

Author

Creemers, J., primary, Westdorp, H., additional, van Oort, I., additional, Schreibelt, G., additional, Gorris, M., additional, Mehra, N., additional, Simons, M., additional, de Goede, A., additional, van Rossum, M., additional, Croockewit, S., additional, Figdor, C., additional, Witjes, J.A., additional, Aarntzen, E., additional, Mus, R., additional, Gotthardt, M., additional, Barentsz, J., additional, de Vries, J., additional, and Gerritsen, W.R., additional

Published
2019
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26. In-depth assessment of metastatic prostate cancer with high tumour mutational burden

Author

Mehra, N. (N.), Riet, J. (Job) van, Smits, M. (M.), Westdorp, H. (Harm), Gorris, M. (M.), van Ee, T. (T.), van der Doelen, M. (M.), Oort, I.M. (Inge) van, Sedelaar, M. (M.), Textor, J. (J.), Cuppen, E. (Edwin), Grunberg, K. (K.), Ligtenberg, M.J. (Marjolijn), Zwart, W. (Wilbert), Bergman, A.M. (Andries), Werken, H.J.G. (Harmen) van de, Schalken, J.A. (Jack), Vries, I.J.M. (Jolanda) de, Lolkema, M.P. (Martijn), Gerritsen, W.R. (Winald), Mehra, N. (N.), Riet, J. (Job) van, Smits, M. (M.), Westdorp, H. (Harm), Gorris, M. (M.), van Ee, T. (T.), van der Doelen, M. (M.), Oort, I.M. (Inge) van, Sedelaar, M. (M.), Textor, J. (J.), Cuppen, E. (Edwin), Grunberg, K. (K.), Ligtenberg, M.J. (Marjolijn), Zwart, W. (Wilbert), Bergman, A.M. (Andries), Werken, H.J.G. (Harmen) van de, Schalken, J.A. (Jack), Vries, I.J.M. (Jolanda) de, Lolkema, M.P. (Martijn), and Gerritsen, W.R. (Winald)

Published
2018
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27. PTEN Hamartoma Tumor Syndrome and Immune Dysregulation

Author

Eissing, M.L.L.G., Ripken, L.S., Schreibelt, G., Westdorp, H., Ligtenberg, M.J., Netea-Maier, R.T., Netea, M.G., Vries, I.J.M. de, Hoogerbrugge, N., Eissing, M.L.L.G., Ripken, L.S., Schreibelt, G., Westdorp, H., Ligtenberg, M.J., Netea-Maier, R.T., Netea, M.G., Vries, I.J.M. de, and Hoogerbrugge, N.

Abstract

Contains fulltext : 200303.pdf (publisher's version ) (Open Access), Carriers of a pathogenic germline mutations in the PTEN gene, a well-known tumor suppressor gene, are at increased risk of multiple benign and malignant tumors, e.g. breast, thyroid, endometrial and colon cancer. This is called PTEN Hamartomous Tumor Syndrome (PHTS). PHTS patients may also have an increased risk of immunological dysregulation, such as autoimmunity and immune deficiencies. The effects of PTEN on the immune system have been studied in murine knockout models demonstrating that loss of PTEN function leads to dysregulation of the immune response. This results in susceptibility to autoimmunity, impaired B cell class switching with subsequent hypogammaglobulinemia. Additionally, a decreased ability of dendritic cells to prime CD8(+) T cells was observed, leading to impaired tumor eradication. Immune dysfunction in PHTS patients has not yet been extensively studied but might be a manageable contributing factor to the increased cancer risk in PHTS.

Published
2018

28. Cancer prevention by aspirin in children with Constitutional Mismatch Repair Deficiency (CMMRD)

Author

Leenders, E.K.S.M., Westdorp, H., Bruggemann, R.J.M., Loeffen, J., Kratz, C., Burn, J., Hoogerbrugge, N., Jongmans, M.C.J., Leenders, E.K.S.M., Westdorp, H., Bruggemann, R.J.M., Loeffen, J., Kratz, C., Burn, J., Hoogerbrugge, N., and Jongmans, M.C.J.

Abstract

Item does not contain fulltext, Constitutional MisMatch Repair Deficiency (CMMRD) is caused by homozygous or compound heterozygous germline variants in one of the mismatch repair (MMR) genes (MSH2, MSH6, PMS2, MLH1). This syndrome results in early onset colorectal cancer, leukemia and lymphoma, brain tumors and other malignancies. Children with CMMRD are at high risk of developing multiple cancers and cancer surveillance does not guarantee detection of cancer at a curable stage. The development of a preventive treatment strategy would be a major step forward. Long-term daily use of acetylsalicylic acid (ASA) has been shown to reduce cancer risk in individuals with Lynch syndrome (LS). LS is caused by heterozygous germline variants of MSH2, MSH6, PMS2 and MLH1 and characterized by an increased risk of developing colorectal and endometrial cancer at adult age. Here we discuss the potential use of ASA for cancer prevention in patients with CMMRD.

Published
2018

30. In-depth assessment of metastatic prostate cancer with high tumour mutational burden

Author

Mehra, N., primary, van Riet, J., additional, Smits, M., additional, Westdorp, H., additional, Gorris, M., additional, van Ee, T., additional, van der Doelen, M., additional, van Oort, I., additional, Sedelaar, M., additional, Textor, J., additional, Cuppen, E., additional, Grunberg, K., additional, Ligtenberg, M.J.L., additional, Zwart, W., additional, Bergman, A., additional, van de Werken, H.J.G., additional, Schalken, J., additional, de Vries, I.J.M., additional, Lolkema, M.P., additional, and Gerritsen, W.R., additional

Published
2018
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31. Survival of metastatic melanoma patients after dendritic cell vaccination correlates with expression of leukocyte phosphatidylethanolamine-binding protein 1/Raf kinase inhibitory protein

Author

Buschow, S.I., Ramazzotti, M., Reinieren-Beeren, I.M.J., Heinzerling, L.M., Westdorp, H., Stefanini, I., Beltrame, L., Hato, S.V., Ellebaek, E., Gross, S., Nguyen, V.A., Weinlich, G., Ragoussis, J., Baban, D., Schuler-Thurner, B., Svane, I.M., Romani, N., Austyn, J.M., Vries, I.J.M. de, Schuler, G., Cavalieri, D., Figdor, C.G., Buschow, S.I., Ramazzotti, M., Reinieren-Beeren, I.M.J., Heinzerling, L.M., Westdorp, H., Stefanini, I., Beltrame, L., Hato, S.V., Ellebaek, E., Gross, S., Nguyen, V.A., Weinlich, G., Ragoussis, J., Baban, D., Schuler-Thurner, B., Svane, I.M., Romani, N., Austyn, J.M., Vries, I.J.M. de, Schuler, G., Cavalieri, D., and Figdor, C.G.

Abstract

Item does not contain fulltext, Immunotherapy for metastatic melanoma offers great promise but, to date, only a subset of patients have responded. There is an urgent need to identify ways of allocating patients to the most beneficial therapy, to increase survival and decrease therapy-associated morbidity and costs. Blood-based biomarkers are of particular interest because of their straightforward implementation in routine clinical care. We sought to identify markers for dendritic cell (DC) vaccine-based immunotherapy against metastatic melanoma through gene expression analysis of peripheral blood mononuclear cells. A large-scale microarray analysis of 74 samples from two treatment centers, taken directly after the first round of DC vaccination, was performed. We found that phosphatidylethanolamine binding protein 1 (PEBP1)/Raf Kinase inhibitory protein (RKIP) expression can be used to identify a significant proportion of patients who performed poorly after DC vaccination. This result was validated by q-PCR analysis on blood samples from a second cohort of 95 patients treated with DC vaccination in four different centers. We conclude that low PEBP1 expression correlates with poor overall survival after DC vaccination. Intriguingly, this was only the case for expression of PEBP1 after, but not prior to, DC vaccination. Moreover, the change in PEBP1 expression upon vaccination correlated well with survival. Further analyses revealed that PEBP1 expression positively correlated with genes involved in T cell responses but inversely correlated with genes associated with myeloid cells and aberrant inflammation including STAT3, NOTCH1, and MAPK1. Concordantly, PEBP1 inversely correlated with the myeloid/lymphoid-ratio and was suppressed in patients suffering from chronic inflammatory disease.

Published
2017

33. Immunotherapy holds the key to cancer treatment and prevention in constitutional mismatch repair deficiency (CMMRD) syndrome

Author

Westdorp, H., Kolders, S., Hoogerbrugge, N., Vries, I.J.M. de, Jongmans, M.C.J., Schreibelt, G., Westdorp, H., Kolders, S., Hoogerbrugge, N., Vries, I.J.M. de, Jongmans, M.C.J., and Schreibelt, G.

Abstract

Item does not contain fulltext, Monoallelic germline mutations in one of the DNA mismatch repair (MMR) genes cause Lynch syndrome, with a high lifetime risks of colorectal and endometrial cancer at adult age. Less well known, is the constitutional mismatch repair deficiency (CMMRD) syndrome caused by biallelic germline mutations in MMR genes. This syndrome is characterized by the development of childhood cancer. Patients with CMMRD are at extremely high risk of developing multiple cancers including hematological, brain and intestinal tumors. Mutations in MMR genes impair DNA repair and therefore most tumors of patients with CMMRD are hypermutated. These mutations lead to changes in the translational reading frame, which consequently result in neoantigen formation. Neoantigens are recognized as foreign by the immune system and can induce specific immune responses. The growing evidence on the clinical efficacy of immunotherapies, such as immune checkpoint inhibitors, offers the prospect for treatment of patients with CMMRD. Combining neoantigen-based vaccination strategies and immune checkpoint inhibitors could be an effective way to conquer CMMRD-related tumors. Neoantigen-based vaccines might also be a preventive treatment option in healthy biallelic MMR mutation carriers. Future studies need to reveal the safety and efficacy of immunotherapies for patients with CMMRD.

Published
2017

34. Survival of metastatic melanoma patients after dendritic cell vaccination correlates with expression of leukocyte phosphatidylethanolamine-binding protein 1/Raf kinase inhibitory protein

Author

Buschow, S.I. (Sonja I.), Ramazzotti, M. (Matteo), Reinieren-Beeren, I. (Inge), Heinzerling, L. (L.), Westdorp, H. (Harm), Stefanini, I. (Irene), Beltrame, L. (Luca), Hato, S.V. (Stanleyson V.), Ellebaek, E. (Eva), Gross, S. (Stefanie), Nguyen, V.A. (Van Anh), Weinlich, G. (Georg), Ragoussis, J. (Jiannis), Baban, D. (Dilair), Schuler-Thurner, B. (Beatrice), Svane, I.M. (Inge M.), Romani, N. (Nikolaus), Austyn, J.M. (Jonathan), Vries, I.J.M. (Jolanda) de, Schuler, G. (Gerhard), Cavalieri, D. (Duccio), Figdor, C.G. (Carl), Buschow, S.I. (Sonja I.), Ramazzotti, M. (Matteo), Reinieren-Beeren, I. (Inge), Heinzerling, L. (L.), Westdorp, H. (Harm), Stefanini, I. (Irene), Beltrame, L. (Luca), Hato, S.V. (Stanleyson V.), Ellebaek, E. (Eva), Gross, S. (Stefanie), Nguyen, V.A. (Van Anh), Weinlich, G. (Georg), Ragoussis, J. (Jiannis), Baban, D. (Dilair), Schuler-Thurner, B. (Beatrice), Svane, I.M. (Inge M.), Romani, N. (Nikolaus), Austyn, J.M. (Jonathan), Vries, I.J.M. (Jolanda) de, Schuler, G. (Gerhard), Cavalieri, D. (Duccio), and Figdor, C.G. (Carl)

Abstract

Immunotherapy for metastatic melanoma offers great promise but, to date, only a subset of patients have responded. There is an urgent need to identify ways of allocating patients to the most beneficial therapy, to increase survival and decrease therapy-associated morbidity and costs. Blood-based biomarkers are of particular interest because of their straightforward implementation in routine clinical care. We sought to identify markers for dendritic cell (DC) vaccine-based immunotherapy against metastatic melanoma through gene expression analysis of peripheral blood mononuclear cells. A large-scale microarray analysis of 74 samples from two treatment centers, taken directly after the first round of DC vaccination, was performed. We found that phosphatidylethanolamine binding protein 1 (_PEBP1_)/ Raf Kinase inhibitory protein (RKIP) expression can be used to identify a significant proportion of patients who performed poorly after DC vaccination. This result was validated by q-PCR analysis on blood samples from a second cohort of 95 patients treated with DC vaccination in four different centers. We conclude that low _PEBP1_ expression correlates with poor overall survival after DC vaccination. Intriguingly, this was only the case for expression of _PEBP1_ after, but not prior to, DC vaccination. Moreover, the change in _PEBP1_ expression upon vaccination correlated well with survival. Further analyses revealed that _PEBP1_ expression positively correlated with genes involved in T cell responses but inversely correlated with genes associated with myeloid cells and aberrant inflammation including _STAT3, NOTCH1,_ and _MAPK1_. Concordantly, _PEBP1_ inversely correlated with the myeloid/ lymphoid-ratio and was suppressed in patients suffering from chronic inflammatory disease.

Published
2017
Full Text
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35. Survival of metastatic melanoma patients after dendritic cell vaccination correlates with expression of leukocyte phosphatidylethanolamine-binding protein 1/Raf kinase inhibitory protein

Author

Buschow, Sonja, Ramazzotti, M, Reinieren-Beeren, IMJ, Heinzerling, LM, Westdorp, H, Stefanini, I, Beltrame, L, Hato, S V, Ellebaek, E, Gross, S, Nguyen, VA, Weinlich, G, Ragoussis, J, Baban, D, Schuler-Thurner, B, Svane, IM, Romani, N, Austyn, JM, de Vries, IJM, Schuler, G, Cavalieri, D, Figdor, CG, Buschow, Sonja, Ramazzotti, M, Reinieren-Beeren, IMJ, Heinzerling, LM, Westdorp, H, Stefanini, I, Beltrame, L, Hato, S V, Ellebaek, E, Gross, S, Nguyen, VA, Weinlich, G, Ragoussis, J, Baban, D, Schuler-Thurner, B, Svane, IM, Romani, N, Austyn, JM, de Vries, IJM, Schuler, G, Cavalieri, D, and Figdor, CG

Published
2017

36. Ipilimumab administered to metastatic melanoma patients who progressed after dendritic cell vaccination

Author

Boudewijns, S, Koornstra, R.H., Westdorp, H., Schreibelt, G., Eertwegh, A.J. van den, Foppen, M.H. Geukes, Haanen, J.B., Vries, I.J. de, Figdor, C.G., Bol, K.F., Gerritsen, W.R., Boudewijns, S, Koornstra, R.H., Westdorp, H., Schreibelt, G., Eertwegh, A.J. van den, Foppen, M.H. Geukes, Haanen, J.B., Vries, I.J. de, Figdor, C.G., Bol, K.F., and Gerritsen, W.R.

Abstract

Contains fulltext : 167316.pdf (Publisher’s version ) (Open Access), BACKGROUND: Ipilimumab has proven to be effective in metastatic melanoma patients. The purpose of this study was to determine the efficacy of ipilimumab in advanced melanoma patients who showed progressive disease upon experimental dendritic cell (DC) vaccination. METHODS: Retrospective analysis of 48 stage IV melanoma patients treated with ipilimumab after progression upon DC vaccination earlier in their treatment. DC vaccination was given either as adjuvant treatment for stage III disease (n = 18) or for stage IV disease (n = 30). Ipilimumab (3 mg/kg) was administered every 3 weeks for up to 4 cycles. RESULTS: Median time between progression upon DC vaccination and first gift of ipilimumab was 5.4 mo. Progression-free survival (PFS) rates for patients that received ipilimumab after adjuvant DC vaccination, and patients that received DC vaccination for stage IV melanoma, were 35% and 7% at 1 y and 35% and 3% at 2 y, while the median PFS was 2.9 mo and 3.1 mo, respectively. Median overall survival of patients pre-treated with adjuvant DC vaccination for stage III melanoma was not reached versus 8.0 mo (95% CI, 5.2-10.9) in the group pre-treated with DC vaccination for stage IV disease (HR of death, 0.36; p = 0.017). Grade 3 immune-related adverse events occurred in 19% of patients and one death (2%) was related to ipilimumab. CONCLUSIONS: Clinical responses to ipilimumab were found in a considerable number of advanced melanoma patients with progression after adjuvant DC vaccination for stage III disease, while the effect was very limited in patients who showed progression after DC vaccination for stage IV disease.

Published
2016

37. Opportunities for immunotherapy in microsatellite instable colorectal cancer

Author

Westdorp, H., Fennemann, F.L., Weren, R.D.A., Bisseling, T.M., Ligtenberg, M.J., Figdor, C.G., Schreibelt, G., Hoogerbrugge, N., Wimmers, F., Vries, I.J.M. de, Westdorp, H., Fennemann, F.L., Weren, R.D.A., Bisseling, T.M., Ligtenberg, M.J., Figdor, C.G., Schreibelt, G., Hoogerbrugge, N., Wimmers, F., and Vries, I.J.M. de

Abstract

Contains fulltext : 171091.pdf (Publisher’s version ) (Open Access), Microsatellite instability (MSI), the somatic accumulation of length variations in repetitive DNA sequences called microsatellites, is frequently observed in both hereditary and sporadic colorectal cancer (CRC). It has been established that defects in the DNA mismatch repair (MMR) pathway underlie the development of MSI in CRC. After the inactivation of the DNA MMR pathway, misincorporations, insertions and deletions introduced by DNA polymerase slippage are not properly recognized and corrected. Specific genomic regions, including microsatellites, are more prone for DNA polymerase slippage and, therefore, more susceptible for the introduction of these mutations if the DNA MMR capacity is lost. Some of these susceptible genomic regions are located within the coding regions of genes. Insertions and deletions in these regions may alter their reading frame, potentially resulting in the transcription and translation of frameshift peptides with c-terminally altered amino acid sequences. These frameshift peptides are called neoantigens and are highly immunogenic, which explains the enhanced immunogenicity of MSI CRC. Neoantigens contribute to increased infiltration of tumor tissue with activated neoantigen-specific cytotoxic T lymphocytes, a hallmark of MSI tumors. Currently, neoantigen-based vaccination is being studied in a clinical trial for Lynch syndrome and in a trial for sporadic MSI CRC of advanced stage. In this Focussed Research Review, we summarize current knowledge on molecular mechanisms and address immunological features of tumors with MSI. Finally, we describe their implications for immunotherapeutic approaches and provide an outlook on next-generation immunotherapy involving neoantigens and combinatorial therapies in the setting of MSI CRC.

Published
2016

38. Effective Clinical Responses in Metastatic Melanoma Patients after Vaccination with Primary Myeloid Dendritic Cells

Author

Schreibelt, G., Bol, K.F., Westdorp, H., Wimmers, F., Aarntzen, E.H.J.G., Duiveman-de Boer, T., Rakt, M.W.M.M. van de, Scharenborg, N.M., Boer, A.J. de, Pots, J.M., Olde Nordkamp, M.A.M., Oorschot, T.G.M. van, Tel, J., Winkels, G., Petry, K., Blokx, W.A.M., Rossum, M.M. van, Welzen, M.E.B., Mus, R.D.M., Croockewit, S., Koornstra, R.H., Jacobs, J.F.M., Kelderman, S., Blank, C.U., Gerritsen, W.R., Punt, C.J.A., Figdor, C.G., Vries, I.J.M. de, Schreibelt, G., Bol, K.F., Westdorp, H., Wimmers, F., Aarntzen, E.H.J.G., Duiveman-de Boer, T., Rakt, M.W.M.M. van de, Scharenborg, N.M., Boer, A.J. de, Pots, J.M., Olde Nordkamp, M.A.M., Oorschot, T.G.M. van, Tel, J., Winkels, G., Petry, K., Blokx, W.A.M., Rossum, M.M. van, Welzen, M.E.B., Mus, R.D.M., Croockewit, S., Koornstra, R.H., Jacobs, J.F.M., Kelderman, S., Blank, C.U., Gerritsen, W.R., Punt, C.J.A., Figdor, C.G., and Vries, I.J.M. de

Abstract

Contains fulltext : 172415.pdf (publisher's version ) (Closed access), Purpose: Thus far, dendritic cell (DC)-based immunotherapy of cancer was primarily based on in vitro-generated monocyte-derived DCs, which require extensive in vitro manipulation. Here, we report on a clinical study exploiting primary CD1c(+) myeloid DCs, naturally circulating in the blood. Experimental Design: Fourteen stage IV melanoma patients, without previous systemic treatment for metastatic disease, received autologous CD1c(+) myeloid DCs, activated by only brief (16 hours) ex vivo culture and loaded with tumor-associated antigens of tyrosinase and gp100. Results: Our results show that therapeutic vaccination against melanoma with small amounts (3-10 x 10(6)) of myeloid DCs is feasible and without substantial toxicity. Four of 14 patients showed long-term progression-free survival (12-35 months), which directly correlated with the development of multifunctional CD8(+) T-cell responses in three of these patients. In particular, high CD107a expression, indicative for cytolytic activity, and IFN gamma as well as TNF alpha and CCL4 production was observed. Apparently, these T-cell responses are essential to induce tumor regression and promote long-term survival by stalling tumor growth. Conclusions: We show that vaccination of metastatic melanoma patients with primary myeloid DCs is feasible and safe and results in induction of effective antitumor immune responses that coincide with improved progression-free survival. (C) 2015 AACR.

Published
2016

39. Adjuvant Dendritic Cell Vaccination in High-Risk Uveal Melanoma

Author

Bol, K.F., Bosch, T van den, Schreibelt, G., Mensink, H.W., Keunen, J.E.E., Kilic, E., Japing, W.J., Geul, K.W., Westdorp, H., Boudewijns, S, Croockewit, S., Rossum, M.M. van, Goede, A.L. de, Naus, N.C., Graaf, W.T.A. van der, Gerritsen, W.R., Klein, A., Punt, C.J.A., Figdor, C.G., Cohen, V.M., Paridaens, D., Vries, I.J.M. de, Bol, K.F., Bosch, T van den, Schreibelt, G., Mensink, H.W., Keunen, J.E.E., Kilic, E., Japing, W.J., Geul, K.W., Westdorp, H., Boudewijns, S, Croockewit, S., Rossum, M.M. van, Goede, A.L. de, Naus, N.C., Graaf, W.T.A. van der, Gerritsen, W.R., Klein, A., Punt, C.J.A., Figdor, C.G., Cohen, V.M., Paridaens, D., and Vries, I.J.M. de

Abstract

Item does not contain fulltext

Published
2016

40. Adjuvant dendritic cell vaccination induces tumor-specific immune responses in the majority of stage III melanoma patients

Author

Boudewijns, S, Bol, K.F., Schreibelt, G., Westdorp, H., Textor, J.C., Rossum, M.M. van, Scharenborg, N.M., Boer, A.J. de, Rakt, M.W.M.M. van de, Pots, J.M., Oorschot, T.G.M. van, Boer, T. de, Nordkamp, M.A. Olde, Meeteren, W.S. van, Graaf, W.T.A. van der, Bonenkamp, J.J., Wilt, J.H.W. de, Aarntzen, E.H.J.G., Punt, C.J.A., Gerritsen, W.R., Figdor, C.G., Vries, I.J.M. de, Boudewijns, S, Bol, K.F., Schreibelt, G., Westdorp, H., Textor, J.C., Rossum, M.M. van, Scharenborg, N.M., Boer, A.J. de, Rakt, M.W.M.M. van de, Pots, J.M., Oorschot, T.G.M. van, Boer, T. de, Nordkamp, M.A. Olde, Meeteren, W.S. van, Graaf, W.T.A. van der, Bonenkamp, J.J., Wilt, J.H.W. de, Aarntzen, E.H.J.G., Punt, C.J.A., Gerritsen, W.R., Figdor, C.G., and Vries, I.J.M. de

Abstract

Contains fulltext : 170905.pdf (Publisher’s version ) (Open Access), PURPOSE: To determine the effectiveness of adjuvant dendritic cell (DC) vaccination to induce tumor-specific immunological responses in stage III melanoma patients. EXPERIMENTAL DESIGN: Retrospective analysis of stage III melanoma patients, vaccinated with autologous monocyte-derived DC loaded with tumor-associated antigens (TAA) gp100 and tyrosinase after radical lymph node dissection. Skin-test infiltrating lymphocytes (SKILs) obtained from delayed-type hypersensitivity skin-test biopsies were analyzed for the presence of TAA-specific CD8(+) T cells by tetrameric MHC-peptide complexes and by functional TAA-specific T cell assays, defined by peptide-recognition (T2 cells) and/or tumor-recognition (BLM and/or MEL624) with specific production of Th1 cytokines and no Th2 cytokines. RESULTS: Ninety-seven patients were analyzed: 21 with stage IIIA, 34 with stage IIIB, and 42 had stage IIIC disease. Tetramer-positive CD8(+) T cells were present in 68 patients (70%), and 24 of them showed a response against all 3 epitopes tested (gp100:154-162, gp100:280-288, and tyrosinase:369-377) at any point during vaccinations. A functional T cell response was found in 62 patients (64%). Rates of peptide-recognition of gp100:154-162, gp100:280-288, and tyrosinase:369-377 were 40%, 29%, and 45%, respectively. Median recurrence-free survival and distant metastasis-free survival of the whole study population were 23.0 mo and 36.8 mo, respectively. CONCLUSIONS: DC vaccination induces a functional TAA-specific T cell response in the majority of stage III melanoma patients, indicating it is more effective in stage III than in stage IV melanoma patients. Furthermore, performing multiple cycles of vaccinations enhances the chance of a broader immune response.

Published
2016

41. Preclinical exploration of combining plasmacytoid and myeloid dendritic cell vaccination with BRAF inhibition

Author

Tel, J., Koornstra, R., Haas, N. de, Deutekom, V. van, Westdorp, H., Boudewijns, S, Erp, N. van, Blasio, S. Di, Gerritsen, W.R., Figdor, C.G., Vries, I.J.M. de, Hato, S.V., Tel, J., Koornstra, R., Haas, N. de, Deutekom, V. van, Westdorp, H., Boudewijns, S, Erp, N. van, Blasio, S. Di, Gerritsen, W.R., Figdor, C.G., Vries, I.J.M. de, and Hato, S.V.

Abstract

Contains fulltext : 171226.pdf (publisher's version ) (Open Access), Background: Melanoma is the most lethal type of skin cancer and its incidence is progressively increasing. The introductions of immunotherapy and targeted therapies have tremendously improved the treatment of melanoma. Selective inhibition of BRAF by vemurafenib results in objective clinical responses in around 50 % of patients suffering from BRAFV600 mutated melanoma. However, drug resistance often results in hampering long-term tumor control. Alternatively, immunotherapy by vaccination with natural dendritic cells (nDCs) demonstrated long-term tumor control in a proportion of patients. We postulate that the rapid tumor debulking by vemurafenib can synergize the long-term tumor control of nDC vaccination to result in an effective treatment modality in a large proportion of patients. Here, we investigated the feasibility of this combination by analyzing the effect of vemurafenib on the functionality of nDCs. Methods: Plasmacytoid DCs (pDCs) and myeloid DCs (mDCs) were isolated from PBMCs obtained from buffy coats from healthy volunteers or vemurafenib-treated melanoma patients. Maturation of pDCs, mDCs and immature mono-cyte-derived DCs was induced by R848 in the presence or absence of vemurafenib and analyzed by FACS. Cytokine production and T cell proliferation induced by mature DCs were analyzed. Results: Vemurafenib inhibited maturation and cytokine production of highly purified nDCs of healthy volunteers resulting in diminished allogeneic T cell proliferation. This deleterious effect of vemurafenib on nDC functionality was absent when total PBMCs were exposed to vemurafenib. In patients receiving vemurafenib, nDC functionality and T cell allostimulatory capacity were unaffected. Conclusion: Although vemurafenib inhibited the functionality of purified nDC of healthy volunteers, this effect was not observed when nDCs were matured in the complete PBMC fraction. This might have been caused by increased vemurafenib uptake in absence of other cell types. In accordanc

Published
2016

42. Immune-related Adverse Events of Dendritic Cell Vaccination Correlate With Immunologic and Clinical Outcome in Stage III and IV Melanoma Patients

Author

Boudewijns, S, Westdorp, H., Koornstra, R.H., Aarntzen, E.H.J.G., Schreibelt, G., Creemers, J.H., Punt, C.J.A., Figdor, C.G., Vries, I.J.M. de, Gerritsen, W.R., Bol, K.F., Boudewijns, S, Westdorp, H., Koornstra, R.H., Aarntzen, E.H.J.G., Schreibelt, G., Creemers, J.H., Punt, C.J.A., Figdor, C.G., Vries, I.J.M. de, Gerritsen, W.R., and Bol, K.F.

Abstract

Contains fulltext : 172741.pdf (Publisher’s version ) (Open Access), The purpose of this study was to determine the toxicity profile of dendritic cell (DC) vaccination in stage III and IV melanoma patients, and to evaluate whether there is a correlation between side effects and immunologic and clinical outcome. This is a retrospective analysis of 82 stage III and 137 stage IV melanoma patients, vaccinated with monocyte-derived or naturally circulating autologous DCs loaded with tumor-associated antigens gp100 and tyrosinase. Median follow-up time was 54.3 months in stage III patients and 12.9 months in stage IV patients. Treatment-related adverse events occurred in 84% of patients; grade 3 toxicity was present in 3% of patients. Most common adverse events were flu-like symptoms (67%) and injection site reactions (50%), and both correlated with the presence of tetramer-positive CD8 T cells (both P<0.001). In stage III melanoma patients experiencing flu-like symptoms, median overall survival (OS) was not reached versus 32.3 months in patients without flu-like symptoms (P=0.009); median OS in patients with an injection site reaction was not reached versus 53.7 months in patients without an injection site reaction (P<0.05). In stage IV melanoma patients (primary uveal and mucosal melanomas excluded), median OS in patients with or without flu-like symptoms was 13.1 versus 8.9 months, respectively (P=0.03); median OS in patients with an injection site reaction was 15.7 months versus 9.8 months in patients without an injection site reaction (P=0.003). In conclusion, DC vaccination is safe and tolerable and the occurrence of the immune-related side effects, such as flu-like symptoms and injection site reactions, correlates with immunologic and clinical outcome.

Published
2016

44. Preventive dendritic cell vaccination in healthy Lynch syndrome mutation carriers

Author

Westdorp, H., primary, Gorris, M.A.J., additional, Boudewijns, S., additional, Bisseling, T., additional, de Goede, A.L., additional, van Rossum, M.M., additional, Ligtenberg, M.J.L., additional, Schreibelt, G., additional, Nagtegaal, I.D., additional, Figdor, C.G., additional, Gerritsen, W., additional, Hoogerbrugge, N., additional, and de Vries, I.J.M., additional

Published
2016
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45. [Hormone therapy in prostate cancer; a pharmacotherapeutic challenge]

Author

Westdorp, H., Benoist, G.E., Schers, H.J., Erp, P.H. van, Gerritsen, W.R., Mulders, P.F.A., Kramers, C., Westdorp, H., Benoist, G.E., Schers, H.J., Erp, P.H. van, Gerritsen, W.R., Mulders, P.F.A., and Kramers, C.

Abstract

Item does not contain fulltext, Prostate cancer is the most common form of cancer in men in the Western world. One-third of the patients with localised prostate cancer will develop recurrent disease, localised disease spread or distant metastases. The presence of distant metastases is an indication for primary palliative hormone therapy. Intervention in the testosterone metabolism using hormone therapy is frequently accompanied by side effects and has a negative influence on the quality of life. Almost all prostate cancer patients show disease progression while on primary hormone therapy, despite having testosterone concentrations at castration level; they are then said to have castration-resistant prostate cancer (CRPC). The CYP17 inhibitor abiraterone and the non-steroidal anti-androgen enzalutamide are second-generation hormone therapies for metastatic CRPC both before and after treatment with standard docetaxel-based chemotherapy. Abiraterone and enzalutamide can lead to many interactions with other drugs or food. This can lead to higher or lower levels of both the hormone therapy and comedications.

Published
2015

47. Immunotherapy for prostate cancer: lessons from responses to tumor-associated antigens

Author

Westdorp, H., Skold, A., Snijer, B.A., Franik, S., Mulder, S.F., Major, P.P., Foley, R., Gerritsen, W.R., Vries, I.J.M. de, Westdorp, H., Skold, A., Snijer, B.A., Franik, S., Mulder, S.F., Major, P.P., Foley, R., Gerritsen, W.R., and Vries, I.J.M. de

Abstract

Contains fulltext : 134069.pdf (publisher's version ) (Open Access), Prostate cancer (PCa) is the most common cancer in men and the second most common cause of cancer-related death in men. In recent years, novel therapeutic options for PCa have been developed and studied extensively in clinical trials. Sipuleucel-T is the first cell-based immunotherapeutic vaccine for treatment of cancer. This vaccine consists of autologous mononuclear cells stimulated and loaded with an immunostimulatory fusion protein containing the prostate tumor antigen prostate acid posphatase. The choice of antigen might be key for the efficiency of cell-based immunotherapy. Depending on the treatment strategy, target antigens should be immunogenic, abundantly expressed by tumor cells, and preferably functionally important for the tumor to prevent loss of antigen expression. Autoimmune responses have been reported against several antigens expressed in the prostate, indicating that PCa is a suitable target for immunotherapy. In this review, we will discuss PCa antigens that exhibit immunogenic features and/or have been targeted in immunotherapeutic settings with promising results, and we highlight the hurdles and opportunities for cancer immunotherapy.

Published
2014

48. Metastatic melanoma mimicking solitary fibrous tumor: report of two cases

Author

Bekers, E.M., Engen-van Grunsven, A.C.H. van, Groenen, P.J.T.A., Westdorp, H., Koornstra, R.H., Bonenkamp, J.J., Flucke, U.E., Blokx, W.A.M., Bekers, E.M., Engen-van Grunsven, A.C.H. van, Groenen, P.J.T.A., Westdorp, H., Koornstra, R.H., Bonenkamp, J.J., Flucke, U.E., and Blokx, W.A.M.

Abstract

Item does not contain fulltext, Malignant melanomas are known for their remarkable morphological variation and aberrant immunophenotype with loss of lineage-specific markers, especially in recurrences and metastases. Hot spot mutations in BRAF, NRAS, GNAQ, and GNA11 and mutations in KIT are oncogenic events in melanomas. Therefore, genotyping can be a useful ancillary diagnostic tool. We present one case each of recurrent and metastatic melanoma, both showing histological and immunohistochemical features of solitary fibrous tumor (SFT). Mutational analysis detected BRAF and NRAS mutations in the primary and secondary lesions, respectively. This result confirmed the diagnosis of recurrent/metastastic melanoma.

Published
2014

50. Impact of TP53 loss-of-function alterations on the response to PSMA radioligand therapy in metastatic castration-resistant prostate cancer patients.

Author

Slootbeek PHJ, Luna-Velez MV, Privé BM, van der Doelen MJ, Kloots ISH, Pamidimarri Naga S, Onstenk HE, Nagarajah J, Westdorp H, van Oort IM, Kroeze LI, Schalken JA, Bloemendal HJ, and Mehra N

Subjects
Humans, Male, Aged, Retrospective Studies, Middle Aged, Aged, 80 and over, Antigens, Surface metabolism, Antigens, Surface genetics, Mutation, Prostate-Specific Antigen metabolism, Progression-Free Survival, Radiopharmaceuticals therapeutic use, Treatment Outcome, Whole Genome Sequencing, Prostatic Neoplasms, Castration-Resistant radiotherapy, Prostatic Neoplasms, Castration-Resistant genetics, Prostatic Neoplasms, Castration-Resistant pathology, Prostatic Neoplasms, Castration-Resistant metabolism, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Glutamate Carboxypeptidase II metabolism, Glutamate Carboxypeptidase II genetics
Abstract

Rationale: PSMA-targeting radioligand therapy (PSMA-RLT) has shown promise in metastatic castration-resistant prostate cancer (mCRPC), particularly in PSMA-avid tumours. However, predicting response remains challenging. Preclinical data suggests aberrant p53-signalling as a predictor of poor response. Methods: The patient population of this pre-planned retrospective cohort study consists of 96 patients with mCRPC who underwent treatment with PSMA-RLT and were molecularly profiled by whole-genome sequencing and or targeted next-generation sequencing. Response to PSMA-RLT was assessed per molecular subtype, including TP53 -mutational status. Results: Patients with TP53 loss-of-function alterations had a shorter median progression-free survival (3.7 versus 6.2 months, P <0.001), a lower median PSA change (-55% vs. -75%, P =0.012) and shorter overall survival from initiation of PMSA-RLT (7.6 vs. 13.9 months, P =0.003) compared to TP53 -wildtype patients. Pathogenic alterations in AR , MYC , BRCA1 , or BRCA2 as well as in genes linked to the PI3K or MAPK pathways or genes involved in homologous recombination repair, were not associated with response. Only lactate dehydrogenase was, alongside TP53 -status, significantly associated with response. Transcriptome analysis of 21 patients, identified six p53 signalling genes whose low expression was associated to a shorter progression-free survival ( P <0.05). Conclusion: TP53 loss-of-function may serve as a prognostic factor for PSMA-RLT outcomes in patients with mCRPC., Competing Interests: Competing Interests: Maarten J. van der Doelen: Research support: 'Bayer, Janssen-Cilag'. Travel support: 'Astellas'. James Nagarajah: Research support: 'ABX, Novartis'. Advisory role: 'ITM, POINT biopharma, CURIUM, Novartis, Bayer'. Inge M. van Oort: Advisory role: 'Bayer, Astellas, Janssen, MSD/AstraZeneca'. Research support: 'Astellas, Janssen, Bayer'. Jack. A. Schalken: Speaker honorarium: 'Astellas, Bayer'. Niven Mehra: Advisory role: 'Roche, MSD, BMS, Bayer, Astellas, Janssen'. Research support: 'Astellas, Janssen, Pfizer, Roche and Sanofi' Genzyme'. Travel support: 'Astellas, MSD'. The remaining authors declare no conflict of interest., (© The author(s).)

Published
2024
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