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1. p53 immunohistochemistry in endometrial cancer: clinical and molecular correlates in the PORTEC-3 trial

Author

Vermij, Lisa, Léon-Castillo, Alicia, Singh, Naveena, Powell, Melanie E., Edmondson, Richard J., Genestie, Catherine, Khaw, Pearly, Pyman, Jan, McLachlin, C. Meg, Ghatage, Prafull, de Boer, Stephanie M., Nijman, Hans W., Smit, Vincent T.H.B.M., Crosbie, Emma J., Leary, Alexandra, Creutzberg, Carien L., Horeweg, Nanda, Bosse, Tjalling, Horeweg, N., de Boer, S.M., Creutzberg, C.L., Bosse, T., Smit, V.T.H.B.M., Kroep, J., Nout, R.A., Nijman, H.W., de Bruyn, M., Powell, M.E., Singh, N., Kitchener, H.C., Crosbie, E., Edmondson, R., Church, D.N., Leary, A., Mileshkin, L., Pollock, P.M., and MacKay, H.

Published
2022
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3. Author Correction: Prediction of recurrence risk in endometrial cancer with multimodal deep learning.

Author

Volinsky-Fremond, S, Horeweg, N, Andani, S, Barkey Wolf, J, Lafarge, MW, de Kroon, CD, Ørtoft, G, Høgdall, E, Dijkstra, J, Jobsen, JJ, Lutgens, LCHW, Powell, ME, Mileshkin, LR, Mackay, H, Leary, A, Katsaros, D, Nijman, HW, de Boer, SM, Nout, RA, de Bruyn, M, Church, D, Smit, VTHBM, Creutzberg, CL, Koelzer, VH, Bosse, T, Volinsky-Fremond, S, Horeweg, N, Andani, S, Barkey Wolf, J, Lafarge, MW, de Kroon, CD, Ørtoft, G, Høgdall, E, Dijkstra, J, Jobsen, JJ, Lutgens, LCHW, Powell, ME, Mileshkin, LR, Mackay, H, Leary, A, Katsaros, D, Nijman, HW, de Boer, SM, Nout, RA, de Bruyn, M, Church, D, Smit, VTHBM, Creutzberg, CL, Koelzer, VH, and Bosse, T

Published
2024

4. Molecular and Clinicopathologic Characterization of Mismatch Repair-Deficient Endometrial Carcinoma Not Related to MLH1 Promoter Hypermethylation.

Author

Kaya, M, Post, CCB, Tops, CM, Nielsen, M, Crosbie, EJ, Leary, A, Mileshkin, LR, Han, K, Bessette, P, de Boer, SM, Jürgenliemk-Schulz, IM, Lutgens, L, Jobsen, JJ, Haverkort, MAD, Nout, RA, Kroep, J, Creutzberg, CL, Smit, VTHBM, Horeweg, N, van Wezel, T, Bosse, T, Kaya, M, Post, CCB, Tops, CM, Nielsen, M, Crosbie, EJ, Leary, A, Mileshkin, LR, Han, K, Bessette, P, de Boer, SM, Jürgenliemk-Schulz, IM, Lutgens, L, Jobsen, JJ, Haverkort, MAD, Nout, RA, Kroep, J, Creutzberg, CL, Smit, VTHBM, Horeweg, N, van Wezel, T, and Bosse, T

Abstract

Universal tumor screening in endometrial carcinoma (EC) is increasingly adopted to identify individuals at risk of Lynch syndrome (LS). These cases involve mismatch repair-deficient (MMRd) EC without MLH1 promoter hypermethylation (PHM). LS is confirmed through the identification of germline MMR pathogenic variants (PV). In cases where these are not detected, emerging evidence highlights the significance of double-somatic MMR gene alterations as a sporadic cause of MMRd, alongside POLE/POLD1 exonuclease domain (EDM) PV leading to secondary MMR PV. Our understanding of the incidence of different MMRd EC origins not related to MLH1-PHM, their associations with clinicopathologic characteristics, and the prognostic implications remains limited. In a combined analysis of the PORTEC-1, -2, and -3 trials (n = 1254), 84 MMRd EC not related to MLH1-PHM were identified that successfully underwent paired tumor-normal tissue next-generation sequencing of the MMR and POLE/POLD1 genes. Among these, 37% were LS associated (LS-MMRd EC), 38% were due to double-somatic hits (DS-MMRd EC), and 25% remained unexplained. LS-MMRd EC exhibited higher rates of MSH6 (52% vs 19%) or PMS2 loss (29% vs 3%) than DS-MMRd EC, and exclusively showed MMR-deficient gland foci. DS-MMRd EC had higher rates of combined MSH2/MSH6 loss (47% vs 16%), loss of >2 MMR proteins (16% vs 3%), and somatic POLE-EDM PV (25% vs 3%) than LS-MMRd EC. Clinicopathologic characteristics, including age at tumor onset and prognosis, did not differ among the various groups. Our study validates the use of paired tumor-normal next-generation sequencing to identify definitive sporadic causes in MMRd EC unrelated to MLH1-PHM. MMR immunohistochemistry and POLE-EDM mutation status can aid in the differentiation between LS-MMRd EC and DS-MMRd EC. These findings emphasize the need for integrating tumor sequencing into LS diagnostics, along with clear interpretation guidelines, to improve clinical management. Although not impacting

Published
2024

6. MO-0050 Feasibility of the determination of the molecular-integrated risk profile in the PORTEC-4a trial

Author

van den Heerik, A., primary, Horeweg, N., additional, Lutgens, L., additional, Haverkort, D., additional, Kommoss, S., additional, Staebler, A., additional, Koppe, F., additional, Nowee, M., additional, Westerveld, H., additional, de Jong, M., additional, Cibula, D., additional, Dundr, P., additional, Cnossen, J., additional, Mens, J.W., additional, Chargari, C., additional, Genestie, C., additional, Bijmolt, S., additional, Gillham, C., additional, O'Riain, C., additional, Stam, T., additional, Jurgenliemk-Schulz, I., additional, Hamann, M., additional, Smit, V., additional, Bosse, T., additional, and Creutzberg, C., additional

Published
2023
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7. OC-0508 Molecular classification of endometrial cancer is predictive of response to adjuvant radiotherapy

Author

Horeweg, N., primary, Nout, R.A., additional, Jobsen, J.J., additional, Lutgens, J.C., additional, Jürgenliemk-Schulz, I.M., additional, Haverkort, D.M., additional, Mens, J.W.M., additional, de Jong, M.A., additional, Wortman, B.G., additional, de Boer, S.M., additional, Putter, H., additional, Stelloo, E., additional, Smit, V.T., additional, Bosse, T., additional, and Creutzberg, C.L., additional

Published
2023
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8. OC-0602 Development of an evidence-based adjuvant treatment decision support tool for endometrial cancer

Author

Vermij, L., primary, Putter, H., additional, Jobsen, J., additional, Powell, M., additional, de Boer, S., additional, Leary, A., additional, Fyles, A., additional, Khaw, P., additional, Lutgens, L., additional, Jürgenliemk- Schulz, I., additional, de Jong, M., additional, Haverkort, D., additional, Nout, R., additional, Smit, V., additional, Steyerberg, E., additional, Bosse, T., additional, Creutzberg, C., additional, and Horeweg, N., additional

Published
2023
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9. OC-0601 Early toxicity and quality of life after molecular-based adjuvant treatment in the PORTEC-4a trial

Author

van den Heerik, A., primary, Post, C., additional, Lutgens, L., additional, Haverkort, D., additional, Kommoss, S., additional, Koppe, F., additional, Nowee, M., additional, Westerveld, H., additional, de Jong, M., additional, Cibula, D., additional, Cnossen, J., additional, Mens, J.W., additional, Chargari, C., additional, Bijmolt, S., additional, Gillham, C., additional, Stam, T., additional, Jurgenliemk-Schulz, I., additional, Vandecasteele, K., additional, Verhoeven-Adema, K., additional, Nout, R., additional, Putter, H., additional, Smit, V., additional, Horeweg, N., additional, Bosse, T., additional, and Creutzberg, C., additional

Published
2023
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10. PO-1422 Feasibility of bone marrow sparing VMAT and Dixon MRI for the PROTECT study

Author

Corbeau, A., primary, Nout, R., additional, Kuipers, S., additional, Astreinidou, E., additional, Mens, J.W., additional, Harderwijk, E., additional, Nielen, B., additional, Wielopolski, P., additional, Sharfo, A., additional, Horeweg, N., additional, Godart, J., additional, van der Heide, U., additional, Creutzberg, C., additional, and de Boer, S., additional

Published
2023
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11. Vaginal brachytherapy management of stage I and II endometrial cancer

Author

Heerik, A.S.V.M. van den, Horeweg, N., Creutzberg, C.L., and Nout, R.A.

Subjects
Oncology, SDG 3 - Good Health and Well-being, Brachytherapy, Quality of Life, Humans, Obstetrics and Gynecology, Female, Radiotherapy, Adjuvant, Prospective Studies, Neoplasm Recurrence, Local, Endometrial Neoplasms, Neoplasm Staging
Abstract

Adjuvant radiotherapy is an important component of post-operative therapy for patients with early-stage endometrial cancer. In the past decades, many trials have been conducted to determine the optimal adjuvant treatment strategy, pelvic external beam radiotherapy or vaginal brachytherapy. As a result, vaginal brachytherapy became the treatment of choice for patients with early-stage endometrial cancer at high-intermediate risk, based on clinicopathological risk factors. Vaginal brachytherapy maximizes local control and has only mild side effects with limited impact on quality of life, in comparison with pelvic external beam radiotherapy. The most frequently used treatment schedule is the one which was used in the PORTEC-2 trial (21 Gy in three fractions specified at 5 mm depth) and, whenever available, image-guided brachytherapy should be used. However, the most convenient and effective treatment schedule remains to be established. More recently, the discovery and integration of four molecular classes in the risk assessment of endometrial cancer patients has created new opportunities to prevent over- and undertreatment. The 2021 endometrial cancer guideline of the European Society of Gynaecological Oncology (ESGO), European Society for Radiotherapy and Oncology (ESTRO), and the European Society of Pathology (ESP) now proposes an integrated risk stratification, in which both clinicopathologic and molecular factors are combined, to direct adjuvant therapy. This rationale is now investigated in multiple prospective trials. This review provides an overview of the rationale and currently recommended and new strategies for vaginal brachytherapy in patients with stage I and II endometrial cancer.

Published
2022
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12. Prognostic relevance of the molecular classification in high-grade endometrial cancer for patients staged by lymphadenectomy and without adjuvant treatment

Author

Leon-Castillo, A., Horeweg, N., Peters, E.E.M., Rutten, T., Haar, N. ter, Smit, V.T.H.B.M., Kroon, C.D., Boennelycke, M., Hogdall, E., Hogdall, C., Nout, R.R.A., Creutzberg, C.L., Ortoft, G., and Bosse, T.

Subjects
Lymphovascular space invasion, Obstetrics and Gynecology, Lymphadenectomy, Prognosis, Endometrial Neoplasms, Endometrial cancer, Oncology, Mutation, Biomarkers, Tumor, Humans, Lymph Node Excision, Female, Tumor Suppressor Protein p53, Molecular risk factors
Abstract

Introduction: The clinical role of the molecular endometrial cancer (EC) classification has not been fully explored in patients staged with lymphadenectomy or without adjuvant treatment, conditions that could potentially moderate the prognostic value of the classification. We aimed to evaluate the clinical outcome of the molecular subgroups in patients with high-grade EC staged by lymphadenectomy and those without adjuvant treatment.Methods: DNA-sequencing for the detection of pathogenic POLE-exonuclease domain mutations and immunohistochemistry for mismatch repair (MMR) proteins and p53 expression were performed on 412 high-grade EC from the Danish Gynaecological Cancer Database (2005-2012) to classify them as POLE-ultramutated (POLEmut), MMR-deficient (MMRd), p53-mutant (p53abn), or no specific molecular profile (NSMP). Patients with stage IV or residual disease after surgery were excluded. Kaplan-Meier method, log-rank test and Cox proportional hazard models were used for analysis.Results: Molecular analysis was successful in 367 EC; 251 patients had undergone lymphadenectomy. Five-year recurrence rates in this subgroup of patients was 36.7% for women with p53abn EC, 0.0% for POLEmut EC, 13.4% for MMRd EC and 42.9% for NSMP EC (p < 0.001). Similar results were observed among stage IA-IB patients. Among patients without adjuvant treatment (n = 264), none with POLEmut EC (n = 26) had a recurrence.Conclusion: The molecular EC classification has strong prognostic value, independent of clinicopathological factors, also among high-grade EC patients staged by lymphadenectomy and those without adjuvant treatment. The unfavourable prognosis of early-stage p53abn EC is not due to undetected lymph node metastasis, and the indolent behaviour of POLEmut EC is independent of adjuvant treatment.

Published
2022
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13. Prognostic refinement of NSMP high-risk endometrial cancers using oestrogen receptor immunohistochemistry

Author

Vermij, L., Jobsen, J.J., Leon-Castillo, A., Brinkhuis, M., Roothaan, S., Powell, M.E., Boer, S.M. de, Khaw, P., Mileshkin, L.R., Fyles, A., Leary, A., Genestie, C., Jnrgenliemk-Schulz, I.M., Crosbie, E.J., Mackay, H.J., Nijman, H.W., Nout, R.A., Smit, V.T.H.B.M., Creutzberg, C.L., Horeweg, N., Bosse, T., and TransPORTEC Consortium

Subjects
Cancer Research, Oncology, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc
Abstract

Background Risk-assessment of endometrial cancer (EC) is based on clinicopathological factors and molecular subgroup. It is unclear whether adding hormone receptor expression, L1CAM expression or CTNNB1 status yields prognostic refinement. Methods Paraffin-embedded tumour samples of women with high-risk EC (HR-EC) from the PORTEC-3 trial (n = 424), and a Dutch prospective clinical cohort called MST (n = 256), were used. All cases were molecularly classified. Expression of L1CAM, ER and PR were analysed by whole-slide immunohistochemistry and CTNNB1 mutations were assessed with a next-generation sequencing. Kaplan–Meier method, log-rank tests and Cox’s proportional hazard models were used for survival analysis. Results In total, 648 HR-EC were included. No independent prognostic value of ER, PR, L1CAM, and CTNNB1 was found, while age, stage, and adjuvant chemotherapy had an independent impact on risk of recurrence. Subgroup-analysis showed that only in NSMP HR-EC, ER-positivity was independently associated with a reduced risk of recurrence (HR 0.33, 95%CI 0.15–0.75). Conclusions We confirmed the prognostic impact of the molecular classification, age, stage, and adjuvant CTRT in a large cohort of high-risk EC. ER-positivity is a strong favourable prognostic factor in NSMP HR-EC and identifies a homogeneous subgroup of NSMP tumours. Assessment of ER status in high-risk NSMP EC is feasible in clinical practice and could improve risk stratification and treatment.

Published
2023
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14. Refining adjuvant treatment in endometrial cancer based on molecular features: the RAINBO clinical trial program

Author

Bosse, T., Creutzberg, C.L., Crosbie, E.J., Han, K., Horeweg, N., Leary, A., Kroep, J.R., McAlpine, J.N., Powell, M.E., Blanc-Durand, F., Bruyn, M. de, Church, D.N., Koelzer, V.H., Kommoss, S., Singh, N., Bardet, A., Counsell, N., Putter, H., Tu, D., Edmondson, R., Gordon, C., Ledermann, J., Morice, P., MacKay, H., Nijman, H., Nout, R.A., Smit, V.T.H.B.M., White, H., Alexandre, J., Boer, S.M. de, Boere, I., Cooper, R., Ethier, J.L., Frenel, J.S., McGrane, J., Taylor, A., Welch, S., Westermann, A.M., Linden, H.D. van der, Farrelly, L., Feeney, A., Kaya, M., Liu, W., Melis, A., Ngadjeua-Tchouatieu, F., Parulekar, W., Verhoeven-Adema, K., and RAINBO Res Consortium

Subjects
endometrial neoplasms, Oncology, Obstetrics and Gynecology
Abstract

BackgroundThe endometrial cancer molecular classification has been integrated into the 2020 World Health Organization (WHO) diagnostic classification and European treatment guidelines, and provides direction towards more effective and less toxic adjuvant treatment strategies for women with endometrial cancer.Primary Objective(s)The RAINBO program of clinical trials will investigate four molecular class-directed adjuvant treatment strategies following surgical resection to either increase cure rates through the addition of novel targeted therapies or safely reduce toxicity and improve quality of life through treatment de-escalation.Study HypothesisMolecular-directed adjuvant treatment strategies will improve clinical outcomes and reduce toxicity of unwarranted therapies in women with endometrial cancer. The overarching and translational research RAINBO program will advance knowledge of predictive and prognostic (bio)markers that will improve prognostication and treatment allocation.Trial DesignThe RAINBO program is a platform of four international clinical trials and an overarching research program. The randomized phase III p53abn-RED trial for women with invasive stage I–III p53abn endometrial cancer compares adjuvant chemoradiation followed by olaparib for 2 years with adjuvant chemoradiation alone. The randomized phase III MMRd-GREEN trial for women with stage II (with lymphovascular space invasion (LVSI)) or stage III mismatch repair-deficient (MMRd) endometrial cancer compares adjuvant radiotherapy with concurrent and adjuvant durvalumab for 1 year to radiotherapy alone. The randomized phase III NSMP-ORANGE trial is a treatment de-escalation trial for women with estrogen receptor positive stage II (with LVSI) or stage III no specific molecular profile (NSMP) endometrial cancer comparing radiotherapy followed by progestin for 2 years to adjuvant chemoradiation. ThePOLEmut-BLUE trial is a phase II trial in which the safety of de-escalation of adjuvant therapy is investigated for women with stage I–IIIPOLEmut endometrial cancer: no adjuvant therapy for lower-risk disease and no adjuvant therapy or radiotherapy alone for higher-risk disease. The overarching RAINBO program will combine data and tumor material of all participants to perform translational research and evaluate molecular class-based adjuvant therapy in terms of efficacy, toxicity, quality of life, and cost-utility.Major Inclusion/Exclusion CriteriaInclusion criteria include a histologically confirmed diagnosis of endometrial cancer treated by hysterectomy and bilateral salpingo-oophorectomy with or without lymphadenectomy or sentinel lymph node biopsy, with no macroscopic residual disease after surgery and no distant metastases, and molecular classification according to the WHO 2020 algorithm.Primary Endpoint(s)Recurrence-free survival at 3 years in the p53abn-RED, MMRd-GREEN, and NSMP-ORANGE trials and pelvic recurrence at 3 years in thePOLEmut-BLUE trial.Sample SizeThe p53abn-RED trial will include 554 patients, the MMRd-GREEN trial 316, the NSMP-ORANGE trial 600, and thePOLEmut-BLUE trial 145 (120 for lower-risk disease and approximately 25 for higher-risk disease). The overarching research program will pool the four sub-trials resulting in a total sample size of around 1600.Estimated Dates for Completing Accrual and Presenting ResultsThe four clinical trials will have different completion dates; main results are expected from 2028.Trial Registration NumberThe RAINBO program is registered at clinicaltrials.gov (NCT05255653).

Published
2023

16. Tertiary lymphoid structures critical for prognosis in endometrial cancer patients

Author

Horeweg, N, Workel, HH, Loiero, D, Church, DN, Vermij, L, Leon-Castillo, A, Krog, RT, de Boer, SM, Nout, RA, Powell, ME, Mileshkin, LR, MacKay, H, Leary, A, Singh, N, Juergenliemk-Schulz, IM, Smit, VTHBM, Creutzberg, CL, Koelzer, VH, Nijman, HW, Bosse, T, de Bruyn, M, Horeweg, N, Workel, HH, Loiero, D, Church, DN, Vermij, L, Leon-Castillo, A, Krog, RT, de Boer, SM, Nout, RA, Powell, ME, Mileshkin, LR, MacKay, H, Leary, A, Singh, N, Juergenliemk-Schulz, IM, Smit, VTHBM, Creutzberg, CL, Koelzer, VH, Nijman, HW, Bosse, T, and de Bruyn, M

Abstract

B-cells play a key role in cancer suppression, particularly when aggregated in tertiary lymphoid structures (TLS). Here, we investigate the role of B-cells and TLS in endometrial cancer (EC). Single cell RNA-sequencing of B-cells shows presence of naïve B-cells, cycling/germinal center B-cells and antibody-secreting cells. Differential gene expression analysis shows association of TLS with L1CAM overexpression. Immunohistochemistry and co-immunofluorescence show L1CAM expression in mature TLS, independent of L1CAM expression in the tumor. Using L1CAM as a marker, 378 of the 411 molecularly classified ECs from the PORTEC-3 biobank are evaluated, TLS are found in 19%. L1CAM expressing TLS are most common in mismatch-repair deficient (29/127, 23%) and polymerase-epsilon mutant EC (24/47, 51%). Multivariable Cox regression analysis shows strong favorable prognostic impact of TLS, independent of clinicopathological and molecular factors. Our data suggests a pivotal role of TLS in outcome of EC patients, and establishes L1CAM as a simple biomarker.

Published
2022

17. Assessment of patient symptom burden and information needs helps tailoring palliative care consultations: An observational study

Author

Verhoef, M.J., Sweep, B., Nijs, E.J.M. de, Valkenburg, A.C., Horeweg, N., Pieterse, A.H., Steen, J.T. van der, Linden, Y.M. van der, Verhoef, M.J., Sweep, B., Nijs, E.J.M. de, Valkenburg, A.C., Horeweg, N., Pieterse, A.H., Steen, J.T. van der, and Linden, Y.M. van der

Abstract

Item does not contain fulltext, OBJECTIVE: The objective of this study is to study (1) the relationship between patient-reported symptom burden and information needs in hospital-based palliative care and (2) differences in patient-reported needs during the disease trajectory. METHODS: Observational study: patient-reported symptom burden and information needs were collected via a conversation guide comprising assessment scales for 12 symptoms (0-10), the question which symptom has priority to be solved and a question prompt list on 75 palliative care-related items (35 topics, 40 questions). Non-parametric tests assessed associations. RESULTS: Conversation guides were used by 266 patients. Median age was 65 years (IQ-range, 57-72), 49% were male and 96% had cancer. Patients reported highest burden for Fatigue (median = 7) and Loss of appetite (median = 6) and prioritised Pain (26%), Fatigue (9%) and Shortness of breath (9%). Patients wanted information about 1-38 (median = 14) items, mostly Fatigue (68%), Possibilities to manage future symptoms (68%) and Possible future symptoms (67%). Patients also wanted information about symptoms for which they reported low burden. Patients in the symptom-directed phase needed more information about hospice care. CONCLUSION: Symptom burden and information needs are related. Patients often also want information about non-prioritised symptoms and other palliative care domains. Tailored information-provision includes inviting patients to also discuss topics they did not consider themselves.

Published
2022

18. p53 immunohistochemistry in endometrial cancer: clinical and molecular correlates in the PORTEC-3 trial

Author

Vermij, L, Leon-Castillo, A, Singh, N, Powell, ME, Edmondson, RJ, Genestie, C, Khaw, P, Pyman, J, McLachlin, CM, Ghatage, P, de Boer, SM, Nijman, HW, Smit, VTHBM, Crosbie, EJ, Leary, A, Creutzberg, CL, Horeweg, N, Bosse, T, Vermij, L, Leon-Castillo, A, Singh, N, Powell, ME, Edmondson, RJ, Genestie, C, Khaw, P, Pyman, J, McLachlin, CM, Ghatage, P, de Boer, SM, Nijman, HW, Smit, VTHBM, Crosbie, EJ, Leary, A, Creutzberg, CL, Horeweg, N, and Bosse, T

Abstract

Standard molecular classification of endometrial cancers (EC) is now endorsed by the WHO and identifies p53-abnormal (p53abn) EC as the subgroup with the poorest prognosis and the most likely to benefit from adjuvant chemo(radio)therapy. P53abn EC are POLE wildtype, mismatch repair proficient and show abnormal immunohistochemical (IHC) staining for p53. Correct interpretation of routinely performed p53 IHC has therefore become of paramount importance. We aimed to comprehensively investigate abnormal p53 IHC patterns and their relation to clinicopathological and molecular features. Tumor material of 411 molecularly classified high-risk EC from consenting patients from the PORTEC-3 clinical trial were collected. p53 IHC was successful in 408 EC and was considered abnormal when the tumor showed a mutant expression pattern (including subclonal): overexpression, null or cytoplasmic. The presence of pathogenic mutations was determined by next generation sequencing (NGS). Abnormal p53 expression was observed in 131/408 (32%) tumors. The most common abnormal p53 IHC pattern was overexpression (n = 89, 68%), followed by null (n = 12, 9%) and cytoplasmic (n = 3, 2%). Subclonal abnormal p53 staining was observed in 27 cases (21%), which was frequently but not exclusively, associated with POLE mutations and/or MMRd (n = 22/27; p < 0.001). Agreement between p53 IHC and TP53 NGS was observed in 90.7%, resulting in a sensitivity and specificity of 83.6% and 94.3%, respectively. Excluding POLEmut and MMRd EC, as per the WHO-endorsed algorithm, increased the accuracy to 94.5% with sensitivity and specificity of 95.0% and 94.1%, respectively. Our data shows that awareness of the abnormal p53 IHC patterns are prerequisites for correct EC molecular classification. Subclonal abnormal p53 expression is a strong indicator for POLEmut and/or MMRd EC. No significant differences in clinical outcomes were observed among the abnormal p53 IHC patterns. Our data support use of the WHO-endorsed a

Published
2022

19. Microcystic elongated and fragmented (MELF) pattern of invasion:Molecular features and prognostic significance in the PORTEC-1 and -2 trials

Author

van den Heerik, A. S.V.M., Aiyer, K. T.S., Stelloo, E., Jürgenliemk-Schulz, I. M., Lutgens, L. C.H.W., Jobsen, J. J., Mens, J. W.M., van der Steen-Banasik, E. M., Creutzberg, C. L., Smit, V. T.H.B.M., Horeweg, N., Bosse, T., van den Heerik, A. S.V.M., Aiyer, K. T.S., Stelloo, E., Jürgenliemk-Schulz, I. M., Lutgens, L. C.H.W., Jobsen, J. J., Mens, J. W.M., van der Steen-Banasik, E. M., Creutzberg, C. L., Smit, V. T.H.B.M., Horeweg, N., and Bosse, T.

Abstract

Objective: Microcystic, elongated fragmented (MELF) pattern of myometrial invasion is a distinct histologic feature occasionally seen in low-grade endometrial carcinomas (EC). The prognostic relevance of MELF invasion was uncertain due to conflicting data, and it had not yet appropriately been studied in the context of the molecular EC classification. We aimed to determine the relation of MELF invasion with clinicopathological and molecular characteristics, and define its prognostic relevance in early-stage low/intermediate risk EC. Methods: Single whole tumor slides of 979 (85.8%) out of 1141 (high)intermediate-risk EC of women who participated in the PORTEC-1/−2 trials were available for review. Clinicopathological and molecular features were compared between MELF invasion positive and negative cases. Time-to-event analyses were done by Kaplan-Meier method, log-rank tests and Cox’ proportional hazards models. Results: MELF invasion was found in 128 (13.1%) cases, and associated with grade 1–2 histology, deep myometrial invasion and substantial lymph-vascular space invasion (LVSI). 85.6% of MELF invasion positive tumors were no-specific-molecular-profile (NSMP) EC. NSMP EC with MELF invasion were CTNNB1 wild type in 92.2% and KRAS mutated in 24.4% of cases. Risk of recurrence was lower for MELF invasion positive as compared to MELF invasion negative cases (4.9% vs. 12.7%, p = 0.026). However, MELF invasion had no independent impact on risk of recurrence (HR 0.65, p = 0.30) after correction for clinicopathological and molecular factors. Conclusions: MELF invasion has no independent impact on risk of recurrence in early-stage EC, and is frequently observed in low-grade NSMP tumors. Routine assessment of MELF invasion has no clinical implications and is not recommended.

Published
2022

20. Microcystic elongated and fragmented (MELF) pattern of invasion: Molecular features and prognostic significance in the PORTEC-1 and -2 trials

Author

MS Radiotherapie, Cancer, van den Heerik, A. S.V.M., Aiyer, K. T.S., Stelloo, E., Jürgenliemk-Schulz, I. M., Lutgens, L. C.H.W., Jobsen, J. J., Mens, J. W.M., van der Steen-Banasik, E. M., Creutzberg, C. L., Smit, V. T.H.B.M., Horeweg, N., Bosse, T., MS Radiotherapie, Cancer, van den Heerik, A. S.V.M., Aiyer, K. T.S., Stelloo, E., Jürgenliemk-Schulz, I. M., Lutgens, L. C.H.W., Jobsen, J. J., Mens, J. W.M., van der Steen-Banasik, E. M., Creutzberg, C. L., Smit, V. T.H.B.M., Horeweg, N., and Bosse, T.

Published
2022

21. MO-0802 Five-year oncological outcomes after two different APBI techniques; a prospective cohort study

Author

Mast, M., primary, Jacobs, D., additional, Horeweg, N., additional, Speijer, G., additional, Petoukhova, A., additional, Straver, M., additional, Coerkamp, E., additional, Hazelbag, H.M., additional, Merkus, J., additional, Roeloffzen, E., additional, Zwanenburg, L., additional, van der Sijp, J., additional, Fiocco, M., additional, Marijnen, C., additional, and Koper, P., additional

Published
2022
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23. The evolving role of morphology in endometrial cancer diagnostics: From histopathology and molecular testing towards integrative data analysis by deep learning

Author

Fremond, S., Koelzer, V.H., Horeweg, N., Bosse, T., University of Zurich, and Bosse, Tjalling

Subjects
Cancer Research, Oncology, 10049 Institute of Pathology and Molecular Pathology, 610 Medicine & health, 2730 Oncology, 1306 Cancer Research
Abstract

Endometrial cancer (EC) diagnostics is evolving into a system in which molecular aspects are increasingly important. The traditional histological subtype-driven classification has shifted to a molecular-based classification that stratifies EC into DNA polymerase epsilon mutated (POLEmut), mismatch repair deficient (MMRd), and p53 abnormal (p53abn), and the remaining EC as no specific molecular profile (NSMP). The molecular EC classification has been implemented in the World Health Organization 2020 classification and the 2021 European treatment guidelines, as it serves as a better basis for patient management. As a result, the integration of the molecular class with histopathological variables has become a critical focus of recent EC research. Pathologists have observed and described several morphological characteristics in association with specific genomic alterations, but these appear insufficient to accurately classify patients according to molecular subgroups. This requires pathologists to rely on molecular ancillary tests in routine workup. In this new era, it has become increasingly challenging to assign clinically relevant weights to histological and molecular features on an individual patient basis. Deep learning (DL) technology opens new options for the integrative analysis of multi-modal image and molecular datasets with clinical outcomes. Proof-of-concept studies in other cancers showed promising accuracy in predicting molecular alterations from H&E-stained tumor slide images. This suggests that some morphological characteristics that are associated with molecular alterations could be identified in EC, too, expanding the current understanding of the molecular-driven EC classification. Here in this review, we report the morphological characteristics of the molecular EC classification currently identified in the literature. Given the new challenges in EC diagnostics, this review discusses, therefore, the potential supportive role that DL could have, by providing an outlook on all relevant studies using DL on histopathology images in various cancer types with a focus on EC. Finally, we touch upon how DL might shape the management of future EC patients.

Published
2022

24. Clinical Outcomes after International Referral of Uveal Melanoma Patients for Proton Therapy

Author

Marinkovic, M., Pors, L.J., Berg, V. van den, Peters, F.P., Schalenbourg, A., Zografos, L., Pica, A., Hrbacek, J., Duinen, S.G. van, Vu, T.H.K., Bleeker, J.C., Rasch, C.R.N., Jager, M.J., Luyten, G.P.M., and Horeweg, N.

Subjects
Cancer Research, visual acuity, genetic structures, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, neoplasm recurrence, survival, Article, eye diseases, uveal melanoma, proton therapy, organ preservation, local, Oncology, sense organs, RC254-282
Abstract

Simple Summary This study aims to assess cancer control and preservation of the eye and visual acuity after proton therapy abroad for eye melanoma. For this, medical files were reviewed of Dutch uveal melanoma patients who were treated in Switzerland with proton therapy from 1987 to 2019. The tumours of these patients were too large and/or localised too close to the optic nerve to be treated with local plaque irradiation. There were 103 patients, of whom one had a uveal melanoma in both eyes. The tumours were relatively large and often localised around the central part of the retina. At five years after treatment, proton therapy had controlled the uveal melanomas of 94% of the patients and 81% had preserved their eye. Spread of the cancer beyond the eye was observed in 30% of the patients. Most patients (79%) became blind or had severe visual impairment after proton therapy; a small group of patients had mild or no visual impairment (17%). The size of the tumour, its localisation and the dose of proton therapy were important for the risk of decline in visual acuity. This study shows that proton therapy abroad for uveal melanoma is feasible and yields good results. Abstract Objective: To assess oncological and ophthalmological outcomes after international referral of uveal melanoma patients for proton therapy. Materials and Methods: This is a retrospective study among Dutch uveal melanoma patients who were treated in Switzerland with 60.0 CGE proton therapy (in 4 fractions) from 1987 to 2019. All patients were ineligible for brachytherapy due to tumour size and/or proximity to the optic nerve. Time-to-event analyses were performed using Kaplan–Meier’s methodology and Cox proportional hazards models. Results: There were 103 patients (104 eyes) with a median largest tumour diameter of 19 mm (range 6–26 mm). Tumours were localised centrally (11%), mid-peripherally (65%) or peripherally (34%). Median follow-up was 7 years. Five-year local control, distant metastasis-free survival and eye preservation rates were 94%, 70% and 81% respectively. At five years, severe, moderate and mild visual impairment was observed in respectively 79%, 4% and 6% of the patients. Larger tumour volumes and more central tumour localisation were associated with severe visual impairment. After correction for these factors, dose to the macula, optic disc and retina, but not optic nerve was significantly associated with severe visual impairment. Conclusion: International referral for proton therapy yielded good tumour control and eye preservation rates, but risk of distant metastasis and severe visual impairment were substantial, possibly due to the selection of advanced tumour stages and/or central localisation. Dose to the macula may be more relevant than dose to the optic nerve for preservation of visual acuity, which is relevant for the treatment planning of proton therapy.

Published
2021
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25. PROTECT: Prospective Phase-II-Trial Evaluating Adaptive Proton Therapy for Cervical Cancer to Reduce the Impact on Morbidity and the Immune System: Prospective Phase-II-Trial Evaluating Adaptive Proton Therapy for Cervical Cancer to Reduce the Impact on Morbidity and the Immune System

Author

Corbeau, Anouk, Nout, Remi, Mens, Jan Willem, Horeweg, N, Godart, Jérémy, Kerkhof, E.M., Kuipers, S.C. (Sander), van Poelgeest, M, Kroep, JR, Boere, Ingrid, van Doorn, Lena, Hoogeman, Mischa, van der Heide, UA, Putter, H., Welters, MJP, van der Burg, SH, Creutzberg, CL, de Boer, SM, Radiotherapy, Medical Oncology, and Gynecological Oncology

Subjects
SDG 3 - Good Health and Well-being
Abstract

External beam radiation therapy (EBRT) with concurrent chemotherapy followed by brachytherapy is a very effective treatment for locally advanced cervical cancer (LACC). However, treatment-related toxicity is common and reduces the patient’s quality of life (QoL) and ability to complete treatment or undergo adjuvant therapies. Intensity modulated proton therapy (IMPT) enables a significant dose reduction in organs at risk (OAR), when compared to that of standard intensity-modulated radiation therapy (IMRT) or volumetric-modulated arc therapy (VMAT). However, clinical studies evaluating whether IMPT consequently reduces side effects for LACC are lacking. The PROTECT trial is a nonrandomized prospective multicenter phase-II-trial comparing clinical outcomes after IMPT or IMRT/VMAT in LACC. Thirty women aged >18 years with a histological diagnosis of LACC will be included in either the IMPT or IMRT/VMAT group. Treatment includes EBRT (45 Gy in 25 fractions of 1.8 Gy), concurrent five weekly cisplatin (40 mg/m2), and 3D image (MRI)-guided adaptive brachytherapy. The primary endpoint is pelvic bones Dmean and mean bowel V15Gy. Secondary endpoints include dosimetric parameters, oncological outcomes, health-related QoL, immune response, safety, and tolerability. This study provides the first data on the potential of IMPT to reduce OAR dose in clinical practice and improve toxicity and QoL for patients with LACC

Published
2021

26. Health-related quality of life of early-stage breast cancer patients after different radiotherapy regimens

Author

Jacobs, D.H.M., Charaghvandi, R.K., Horeweg, N., Maduro, J.H., Speijer, G., Roeloffzen, E.M.A., Mast, M., Bantema-Joppe, E., Petoukhova, A.L., Bongard, D.H.J.G. van den, Koper, P., Crijns, A.P.G., Marijnen, C.A.M., and Verkooijen, H.M.

Subjects
Intraoperative radiotherapy, Health-related quality of life, Early-stage breast cancer, Accelerated Partial Breast Irradiation
Abstract

Purpose To evaluate and compare health-related quality of life (HRQL) of women with early-stage breast cancer (BC) treated with different radiotherapy (RT) regimens. Methods Data were collected from five prospective cohorts of BC patients treated with breast-conserving surgery and different RT regimens: intraoperative RT (IORT, 1 x 23.3 Gy; n = 267), external beam accelerated partial breast irradiation (EB-APBI, 10 x 3.85 Gy; n = 206), hypofractionated whole breast irradiation(hypo-WBI, 16 x 2.67 Gy; n = 375), hypo-WBI + boost(hypo-WBI-B, 21-26 x 2.67 Gy; n = 189), and simultaneous WBI + boost(WBI-B, 28 x 2.3 Gy; n = 475). Women >= 60 years with invasive/in situ carcinoma

Published
2021

29. 397 Molecular profiling of NSMP high-risk endometrial cancers of the PORTEC-3 trial – prognostic refinement and druggable targets

Author

Vermij, L, primary, Powell, M, additional, Leon-Castillo, A, additional, De Boer, S, additional, Mileshkin, L, additional, Mackay, H, additional, Leary, A, additional, Nijman, HW, additional, Singh, N, additional, Pollock, P, additional, Bessette, P, additional, Haie-Meder, C, additional, Smit, V, additional, Edmondson, R, additional, Crosbie, E, additional, Nout, R, additional, Horeweg, N, additional, Creutzberg, CL, additional, and Bosse, T, additional

Published
2021
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30. 595 Implementation of collaborative translational research (TransPORTEC) findings in an international endometrial cancer clinical trials program (RAINBO)

Author

Bosse, T, primary, Powell, M, additional, Crosbie, E, additional, Leary, A, additional, Kroep, J, additional, Han, K, additional, Mcalpine, J, additional, Horeweg, N, additional, De Boer, S, additional, De Bruyn, M, additional, Nout, R, additional, Smit, V, additional, Nijman, HW, additional, Singh, N, additional, Mackay, H, additional, Edmondson, R, additional, Mileshkin, L, additional, Church, D, additional, Kitchener, H, additional, and Creutzberg, CL, additional

Published
2021
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32. 406 Prognostic relevance of the molecular endometrial cancer classification among patients staged by lymphadenectomy and/or without adjuvant treatment

Author

Leon-Castillo, A, primary, Horeweg, N, additional, Peters, E, additional, Rutten, T, additional, Ter Haar, N, additional, Smit, V, additional, Boennelycke, M, additional, Høgdall, E, additional, Høgdall, C, additional, Nout, R, additional, Creutzberg, CL, additional, Ortoft, G, additional, and Bosse, T, additional

Published
2021
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33. 482 Tertiary lymphoid structures as markers of anti-tumor immunity with independent prognostic value in the PORTEC-3 trial of high-risk endometrial cancer

Author

Horeweg, N, primary, Workel, H, additional, Loiero, D, additional, Church, D, additional, Vermij, L, additional, Leon-Castillo, A, additional, De Boer, S, additional, Nout, R, additional, Powell, M, additional, Mileshkin, L, additional, Mackay, H, additional, Leary, A, additional, Singh, N, additional, Jürgenliemk-Schulz, I, additional, Creutzberg, CL, additional, Kölzer, V, additional, Nijman, HW, additional, Bosse, T, additional, and De Bruyn, M, additional

Published
2021
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35. Prevalence and Prognosis of Lynch Syndrome and Sporadic Mismatch Repair Deficiency in Endometrial Cancer

Author

Post, CCB, Stelloo, E, Smit, VTHBM, Ruano, D, Tops, CM, Vermij, L, Rutten, TA, Jurgenliemk-Schulz, IM, Lutgens, LCHW, Jobsen, JJ, Nout, RA, Crosbie, EJ, Powell, ME, Mileshkin, L, Leary, A, Bessette, P, Putter, H, de Boer, SM, Horeweg, N, Nielsen, M, van Wezel, T, Bosse, T, Creutzberg, CL, Post, CCB, Stelloo, E, Smit, VTHBM, Ruano, D, Tops, CM, Vermij, L, Rutten, TA, Jurgenliemk-Schulz, IM, Lutgens, LCHW, Jobsen, JJ, Nout, RA, Crosbie, EJ, Powell, ME, Mileshkin, L, Leary, A, Bessette, P, Putter, H, de Boer, SM, Horeweg, N, Nielsen, M, van Wezel, T, Bosse, T, and Creutzberg, CL

Abstract

BACKGROUND: Standard screening of endometrial cancer (EC) for Lynch syndrome (LS) is gaining traction; however, the prognostic impact of an underlying hereditary etiology is unknown. We established the prevalence, prognosis, and subsequent primary cancer incidence of patients with LS-associated EC in relation to sporadic mismatch repair deficient (MMRd)-EC in the large combined Post Operative Radiation Therapy in Endometrial Carcinoma-1, -2, and -3 trial cohort. METHODS: After MMR-immunohistochemistry, MLH1-promoter methylation testing, and next-generation sequencing, tumors were classified into 3 groups according to the molecular cause of their MMRd-EC. Kaplan-Meier method, log-rank test, and Cox model were used for survival analysis. Competing risk analysis was used to estimate the subsequent cancer probability. All statistical tests were 2-sided. RESULTS: Among the 1336 ECs, 410 (30.7%) were MMRd. A total of 380 (92.7%) were fully triaged: 275 (72.4%) were MLH1-hypermethylated MMRd-ECs; 36 (9.5%) LS MMRd-ECs, and 69 (18.2%) MMRd-ECs due to other causes. Limiting screening of EC patients to 60 years or younger or to 70 years or younger would have resulted in missing 18 (50.0%) and 6 (16.7%) LS diagnoses, respectively. Five-year recurrence-free survival was 91.7% (95% confidence interval [CI] = 83.1% to 100%; hazard ratio = 0.45, 95% CI = 0.16 to 1.24, P = .12) for LS, 95.5% (95% CI = 90.7% to 100%; hazard ratio = 0.17, 95% CI = 0.05 to 0.55, P = .003) for "other" vs 78.6% (95% CI = 73.8% to 83.7%) for MLH1-hypermethylated MMRd-EC. The probability of subsequent LS-associated cancer at 10 years was 11.6% (95% CI = 0.0% to 24.7%), 1.5% (95% CI = 0.0% to 4.3%), and 7.0% (95% CI = 3.0% to 10.9%) within the LS, "other," and MLH1-hypermethylated MMRd-EC groups, respectively. CONCLUSIONS: The LS prevalence in the Post Operative Radiation Therapy in Endometrial Carcinoma trial population was 2.8% and among MMRd-ECs was 9.5%. Patients with LS-associated ECs showed a trend t

Published
2021

36. PROTECT: Prospective Phase-II-Trial Evaluating Adaptive Proton Therapy for Cervical Cancer to Reduce the Impact on Morbidity and the Immune System:Prospective Phase-II-Trial Evaluating Adaptive Proton Therapy for Cervical Cancer to Reduce the Impact on Morbidity and the Immune System

Author

Corbeau, Anouk, Nout, Remi, Mens, Jan Willem, Horeweg, N, Godart, Jérémy, Kerkhof, E.M., Kuipers, S.C. (Sander), van Poelgeest, M, Kroep, JR, Boere, Ingrid, van Doorn, Lena, Hoogeman, Mischa, van der Heide, UA, Putter, H., Welters, MJP, van der Burg, SH, Creutzberg, CL, de Boer, SM, Corbeau, Anouk, Nout, Remi, Mens, Jan Willem, Horeweg, N, Godart, Jérémy, Kerkhof, E.M., Kuipers, S.C. (Sander), van Poelgeest, M, Kroep, JR, Boere, Ingrid, van Doorn, Lena, Hoogeman, Mischa, van der Heide, UA, Putter, H., Welters, MJP, van der Burg, SH, Creutzberg, CL, and de Boer, SM

Abstract

External beam radiation therapy (EBRT) with concurrent chemotherapy followed by brachytherapy is a very effective treatment for locally advanced cervical cancer (LACC). However, treatment-related toxicity is common and reduces the patient’s quality of life (QoL) and ability to complete treatment or undergo adjuvant therapies. Intensity modulated proton therapy (IMPT) enables a significant dose reduction in organs at risk (OAR), when compared to that of standard intensity-modulated radiation therapy (IMRT) or volumetric-modulated arc therapy (VMAT). However, clinical studies evaluating whether IMPT consequently reduces side effects for LACC are lacking. The PROTECT trial is a nonrandomized prospective multicenter phase-II-trial comparing clinical outcomes after IMPT or IMRT/VMAT in LACC. Thirty women aged >18 years with a histological diagnosis of LACC will be included in either the IMPT or IMRT/VMAT group. Treatment includes EBRT (45 Gy in 25 fractions of 1.8 Gy), concurrent five weekly cisplatin (40 mg/m2), and 3D image (MRI)-guided adaptive brachytherapy. The primary endpoint is pelvic bones Dmean and mean bowel V15Gy. Secondary endpoints include dosimetric parameters, oncological outcomes, health-related QoL, immune response, safety, and tolerability. This study provides the first data on the potential of IMPT to reduce OAR dose in clinical practice and improve toxicity and QoL for patients with LACC

Published
2021

37. This week in the journal

Author

Koning, H.J. de, Aalst, C.M. van der, Jong, P.A. de, Scholten, E.T., Nackaerts, K., Heuvelmans, M.A., Lammers, J.W.J., Weenink, C., Yousaf-Khan, U., Horeweg, N., van't Westeinde, S., Prokop, M., Mali, W.P., Hoesein, F.A.A.M., Ooijen, P.M.A. van, Aerts, J.G.J.V., Bakker, M.A. den, Thunnissen, E., Verschakelen, J., Vliegenthart, R., Walter, J.E., Haaf, K. ten, Groen, H.J.M., and Oudkerk, M.

Abstract

Health care's institutional goals of abbreviating hospital stays and accelerating clinic visits are feeding professional loneliness, and meaningful advances in technology have levied a significant toll in the form of separation from patients and colleagues. The transition away from routine interaction with patients and colleagues toward more individual activities has contributed to loneliness and burnout. Addressing physicians' loneliness in the 21st century requires finding innovative ways to interact with each other. In recent years, health care leaders have increasingly turned to "nudges" to influence health-related behaviors. But harmful health and health care behaviors often arise in circumstances that give us . . .

Published
2020

38. Reduced Lung-Cancer Mortality with Volume CT Screening in a Randomized Trial

Author

Koning, H.J. de, Aalst, C.M. van der, Jong, Pa. de, Scholten, E.T., Nackaerts, K., Heuvelmans, M.A., Lammers, J.J., Weenink, C., Yousaf-Khan, U., Horeweg, N., Westeinde, S. van 't, Prokop, M., Mali, W.P., Hoesein, F.A.A.M., Ooijen, PM van, Aerts, J., Bakker, M.A. den, Thunnissen, E., Verschakelen, J., Vliegenthart, R., Walter, J.E., Haaf, K. Ten, Groen, H.J.M., Oudkerk, M., Koning, H.J. de, Aalst, C.M. van der, Jong, Pa. de, Scholten, E.T., Nackaerts, K., Heuvelmans, M.A., Lammers, J.J., Weenink, C., Yousaf-Khan, U., Horeweg, N., Westeinde, S. van 't, Prokop, M., Mali, W.P., Hoesein, F.A.A.M., Ooijen, PM van, Aerts, J., Bakker, M.A. den, Thunnissen, E., Verschakelen, J., Vliegenthart, R., Walter, J.E., Haaf, K. Ten, Groen, H.J.M., and Oudkerk, M.

Abstract

Contains fulltext : 219680.pdf (Publisher’s version ) (Open Access), BACKGROUND: There are limited data from randomized trials regarding whether volume-based, low-dose computed tomographic (CT) screening can reduce lung-cancer mortality among male former and current smokers. METHODS: A total of 13,195 men (primary analysis) and 2594 women (subgroup analyses) between the ages of 50 and 74 were randomly assigned to undergo CT screening at T0 (baseline), year 1, year 3, and year 5.5 or no screening. We obtained data on cancer diagnosis and the date and cause of death through linkages with national registries in the Netherlands and Belgium, and a review committee confirmed lung cancer as the cause of death when possible. A minimum follow-up of 10 years until December 31, 2015, was completed for all participants. RESULTS: Among men, the average adherence to CT screening was 90.0%. On average, 9.2% of the screened participants underwent at least one additional CT scan (initially indeterminate). The overall referral rate for suspicious nodules was 2.1%. At 10 years of follow-up, the incidence of lung cancer was 5.58 cases per 1000 person-years in the screening group and 4.91 cases per 1000 person-years in the control group; lung-cancer mortality was 2.50 deaths per 1000 person-years and 3.30 deaths per 1000 person-years, respectively. The cumulative rate ratio for death from lung cancer at 10 years was 0.76 (95% confidence interval [CI], 0.61 to 0.94; P = 0.01) in the screening group as compared with the control group, similar to the values at years 8 and 9. Among women, the rate ratio was 0.67 (95% CI, 0.38 to 1.14) at 10 years of follow-up, with values of 0.41 to 0.52 in years 7 through 9. CONCLUSIONS: In this trial involving high-risk persons, lung-cancer mortality was significantly lower among those who underwent volume CT screening than among those who underwent no screening. There were low rates of follow-up procedures for results suggestive of lung cancer. (Funded by the Netherlands Organization of Health Research and Development and

Published
2020

39. PORTEC-4a: international randomized trial of molecular profile-based adjuvant treatment for women with high-intermediate risk endometrial cancer

Author

Heerik, A. van den, Horeweg, N., Nout, R.A., Lutgens, L., Steen-Banasik, E.M. van der, Westerveld, G.H., Berg, H.A. van den, Slot, Annerie, Koppe, F.L.A., Kommoss, S., Mens, J.W.M., Nowee, M.E., Bijmolt, S., Cibula, D., Stam, T.C., Jurgenliemk-Schulz, I.M., Snyers, A., Hamann, Moritz, Zwanenburg, A.G., Coen, V., Vandecasteele, K., Gillham, C., Chargari, C., Verhoeven-Adema, K.W., Putter, H., Hout, W.B. Van den, Wortman, B.G., Nijman, Hans, Bosse, T., Creutzberg, C.L., Heerik, A. van den, Horeweg, N., Nout, R.A., Lutgens, L., Steen-Banasik, E.M. van der, Westerveld, G.H., Berg, H.A. van den, Slot, Annerie, Koppe, F.L.A., Kommoss, S., Mens, J.W.M., Nowee, M.E., Bijmolt, S., Cibula, D., Stam, T.C., Jurgenliemk-Schulz, I.M., Snyers, A., Hamann, Moritz, Zwanenburg, A.G., Coen, V., Vandecasteele, K., Gillham, C., Chargari, C., Verhoeven-Adema, K.W., Putter, H., Hout, W.B. Van den, Wortman, B.G., Nijman, Hans, Bosse, T., and Creutzberg, C.L.

Abstract

Contains fulltext : 229912.pdf (Publisher’s version ) (Open Access), BACKGROUND: Vaginal brachytherapy is currently recommended as adjuvant treatment in patients with high-intermediate risk endometrial cancer to maximize local control and has only mild side effects and no or limited impact on quality of life. However, there is still considerable overtreatment and also some undertreatment, which may be reduced by tailoring adjuvant treatment to the patients' risk of recurrence based on molecular tumor characteristics. PRIMARY OBJECTIVES: To compare the rates of vaginal recurrence in women with high-intermediate risk endometrial cancer, treated after surgery with molecular-integrated risk profile-based recommendations for either observation, vaginal brachytherapy or external pelvic beam radiotherapy or with standard adjuvant vaginal brachytherapy STUDY HYPOTHESIS: Adjuvant treatment based on a molecular-integrated risk profile provides similar local control and recurrence-free survival as current standard adjuvant brachytherapy in patients with high-intermediate risk endometrial cancer, while sparing many patients the morbidity of adjuvant treatment and reducing healthcare costs. TRIAL DESIGN: A multicenter, international phase III randomized trial (2:1) of molecular-integrated risk profile-based adjuvant treatment (experimental arm) or adjuvant vaginal brachytherapy (standard arm). MAJOR INCLUSION/EXCLUSION CRITERIA: Women aged 18 years and over with a histological diagnosis of high-intermediate risk endometrioid endometrial cancer after total abdominal or laparoscopic hysterectomy and bilateral salpingo-oophorectomy. High-intermediate risk factors are defined as: (i) International Federation of Gynecology and Obstetrics stage IA (with invasion) and grade 3; (ii) stage IB grade 1 or 2 with age ≥60 and/or lymph-vascular space invasion; (iii) stage IB, grade 3 without lymph-vascular space invasion; or (iv) stage II (microscopic and grade 1). ENDPOINTS: The primary endpoint is vaginal recurrence. Secondary endpoints are recurrence-free a

Published
2020

40. PORTEC-4a: International randomized trial of molecular profile-based adjuvant treatment for women with high-intermediate risk endometrial cancer

Author

Van Den Heerik, A.S.V.M., Horeweg, N., Nout, R.A., Lutgens, L.C. (Ludy), Van Der Steen-Banasik, E.M., Westerveld, G.H., Van Den Berg, H.A., Slot, A. (Annerie), Koppe, F.L.A., Kommoss, S, Mens, J.-W. (Jan-Willem), Nowee, M.E., Bijmolt, S., Cibula, D, Stam, T.C., Jürgenliemk-Schulz, I.-M. (Ina-M.), Snyers, A., Hamann, M., Zwanenburg, A.G., Coen, VL, Vandecasteele, K., Gillham, C., Chargari, C., Verhoeven-Adema, KW, Putter, H. (Hein), Van Den Hout, W.B., Wortman, B.G., Nijman, H.W. (Hans), Bosse, T., Creutzberg, CL, Van Den Heerik, A.S.V.M., Horeweg, N., Nout, R.A., Lutgens, L.C. (Ludy), Van Der Steen-Banasik, E.M., Westerveld, G.H., Van Den Berg, H.A., Slot, A. (Annerie), Koppe, F.L.A., Kommoss, S, Mens, J.-W. (Jan-Willem), Nowee, M.E., Bijmolt, S., Cibula, D, Stam, T.C., Jürgenliemk-Schulz, I.-M. (Ina-M.), Snyers, A., Hamann, M., Zwanenburg, A.G., Coen, VL, Vandecasteele, K., Gillham, C., Chargari, C., Verhoeven-Adema, KW, Putter, H. (Hein), Van Den Hout, W.B., Wortman, B.G., Nijman, H.W. (Hans), Bosse, T., and Creutzberg, CL

Abstract

Background Vaginal brachytherapy is currently recommended as adjuvant treatment in patients with highintermediate risk endometrial cancer to maximize local control and has only mild side effects and no or limited impact on quality of life. However, there is still considerable overtreatment and also some undertreatment, which may be reduced by tailoring adjuvant treatment to the patients’ risk of recurrence based on molecular tumor characteristics. Primary objectives To compare the rates of vaginal recurrence in women with high-intermediate risk endometrial cancer, treated after surgery with molecularintegrated risk profile-based recommendations for either observation, vaginal brachytherapy or external pelvic beam radiotherapy or with standard adjuvant vaginal brachytherapy Study hypothesis Adjuvant treatment based on a molecular-integrated risk profile provides similar local control and recurrence-free survival as current standard adjuvant brachytherapy in patients with high-intermediate risk endometrial cancer, while sparing many patients the morbidity of adjuvant tr

Published
2020
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41. Molecular Classification of the PORTEC-3 Trial for High-Risk Endometrial Cancer: Impact on Prognosis and Benefit From Adjuvant Therapy

Author

Leon-Castillo, A, de Boer, SM, Powell, ME, Mileshkin, LR, Mackay, HJ, Leary, A, Nijman, HW, Singh, N, Pollock, PM, Bessette, P, Fyles, A, Haie-Meder, C, Smit, VTHBM, Edmondson, RJ, Putter, H, Kitchener, HC, Crosbie, EJ, de Bruyn, M, Nout, RA, Horeweg, N, Creutzberg, CL, Bosse, T, Leon-Castillo, A, de Boer, SM, Powell, ME, Mileshkin, LR, Mackay, HJ, Leary, A, Nijman, HW, Singh, N, Pollock, PM, Bessette, P, Fyles, A, Haie-Meder, C, Smit, VTHBM, Edmondson, RJ, Putter, H, Kitchener, HC, Crosbie, EJ, de Bruyn, M, Nout, RA, Horeweg, N, Creutzberg, CL, and Bosse, T

Abstract

PURPOSE: The randomized Adjuvant Chemoradiotherapy Versus Radiotherapy Alone in Women With High-Risk Endometrial Cancer (PORTEC-3) trial investigated the benefit of combined adjuvant chemotherapy and radiotherapy (CTRT) versus radiotherapy alone (RT) for women with high-risk endometrial cancer (EC). Because The Cancer Genome Atlas defined an EC molecular classification with strong prognostic value, we investigated prognosis and impact of chemotherapy for each molecular subgroup using tissue samples from PORTEC-3 trial participants. METHODS: Paraffin-embedded tissues of 423 consenting patients were collected. Immunohistochemistry for p53 and mismatch repair (MMR) proteins, and DNA sequencing for POLE exonuclease domain were done to classify tumors as p53 abnormal (p53abn), POLE-ultramutated (POLEmut), MMR-deficient (MMRd), or no specific molecular profile (NSMP). The primary end point was recurrence-free survival (RFS). Kaplan-Meier method, log-rank test, and Cox model were used for analysis. RESULTS: Molecular analysis was successful in 410 high-risk EC (97%), identifying the 4 subgroups: p53abn EC (n = 93; 23%), POLEmut (n = 51; 12%), MMRd (n = 137; 33%), and NSMP (n = 129; 32%). Five-year RFS was 48% for patients with p53abn EC, 98% for POLEmut EC, 72% for MMRd EC, and 74% for NSMP EC (P < .001). The 5-year RFS with CTRT versus RT for p53abn EC was 59% versus 36% (P = .019); 100% versus 97% for patients with POLEmut EC (P = .637); 68% versus 76% (P = .428) for MMRd EC; and 80% versus 68% (P = .243) for NSMP EC. CONCLUSION: Molecular classification has strong prognostic value in high-risk EC, with significantly improved RFS with adjuvant CTRT for p53abn tumors, regardless of histologic type. Patients with POLEmut EC had an excellent RFS in both trial arms. EC molecular classification should be incorporated in the risk stratification of these patients as well as in future trials to target specific subgroups of patients.

Published
2020

42. PORTEC-4a: International randomized trial of molecular profile-based adjuvant treatment for women with high-intermediate risk endometrial cancer

Author

van den Heerik, ASVM, Horeweg, N, Nout, Remi, Lutgens, LC, van der Steen-Banasik, E, Westerveld, GH, van den Berg, HA, Slot, A, Koppe, FLA, Kommoss, S, Mens, Jan Willem, Nowee, ME, Bijmolt, S, Cibula, D, Stam, TC, Jurgenliemk-Schulz, IM, Snyers, A, Hamann, M, Zwanenburg, AG, Coen, VL, Vandecasteele, K, Gillham, C, Chargari, C, Verhoeven-Adema, KW, Putter, H, van den Hout, WB, Wortman, BG, Nijman, HW, Bosse, T, Creutzberg, CL, van den Heerik, ASVM, Horeweg, N, Nout, Remi, Lutgens, LC, van der Steen-Banasik, E, Westerveld, GH, van den Berg, HA, Slot, A, Koppe, FLA, Kommoss, S, Mens, Jan Willem, Nowee, ME, Bijmolt, S, Cibula, D, Stam, TC, Jurgenliemk-Schulz, IM, Snyers, A, Hamann, M, Zwanenburg, AG, Coen, VL, Vandecasteele, K, Gillham, C, Chargari, C, Verhoeven-Adema, KW, Putter, H, van den Hout, WB, Wortman, BG, Nijman, HW, Bosse, T, and Creutzberg, CL

Published
2020

43. Patient Reported Outcomes of Early-Stage Breast Cancer Patients after Different Radiotherapy Regimes

Author

Onderzoek Radiotherapie, PMC Medisch specialisten, MS Radiotherapie, Cancer, Trialbureau Beeld, JC onderzoeksprogramma Kanker, Jacobs, D., Charaghvandi, R. K., Horeweg, N., Maduro, J. H., II, Speijer, G., Roeloffzen, E. M. A., Fisscher, U., Mast, M., Bantema-Joppe, E. J., Petoukhova, A., van den Bongard, H. J. G. D., Koper, P., Crijns, A. P. G., Marijnen, C., Verkooijen, H., Onderzoek Radiotherapie, PMC Medisch specialisten, MS Radiotherapie, Cancer, Trialbureau Beeld, JC onderzoeksprogramma Kanker, Jacobs, D., Charaghvandi, R. K., Horeweg, N., Maduro, J. H., II, Speijer, G., Roeloffzen, E. M. A., Fisscher, U., Mast, M., Bantema-Joppe, E. J., Petoukhova, A., van den Bongard, H. J. G. D., Koper, P., Crijns, A. P. G., Marijnen, C., and Verkooijen, H.

Published
2020

45. Patient Reported Outcomes of Early-Stage Breast Cancer Patients after Different Radiotherapy Regimes

Author

Jacobs, D., primary, Charaghvandi, R.K., additional, Horeweg, N., additional, Maduro, J.H., additional, Speijer, G., additional, Roeloffzen, E.M.A., additional, Fisscher, U., additional, Mast, M., additional, Bantema-Joppe, E.J., additional, Petoukhova, A., additional, van den Bongard, H.J.G.D., additional, Koper, P., additional, Crijns, A.P.G., additional, Marijnen, C., additional, and Verkooijen, H., additional

Published
2020
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46. PO-0936: Comparison of local recurrence rates after two different APBI techniques, a prospective study

Author

Jacobs, D., primary, Mast, M., additional, Speijer, G., additional, Horeweg, N., additional, Petoukhova, A., additional, Fisscher, U., additional, Straver, M., additional, Coerkamp, E., additional, Hazelbag, H.M., additional, Merkus, J., additional, Roeloffzen, E., additional, Zwanenburg, L., additional, Fiocco, M., additional, Marijnen, C., additional, and Koper, P., additional

Published
2020
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47. 28 Prevalence and prognosis of lynch syndrome and sporadic mismatch repair deficiency in the combined PORTEC-1,-2 and -3 endometrial cancer trials

Author

Post, C, primary, Stelloo, E, additional, Smit, V, additional, Ruano, D, additional, Tops, CM, additional, Vermij, L, additional, Rutten, TA, additional, Jürgenliemk-Schulz, IM, additional, Lutgens, LC, additional, Jobsen, JJ, additional, Nout, RA, additional, Crosbie, EJ, additional, Powell, ME, additional, Mileshkin, L, additional, Leary, A, additional, Bessette, P, additional, de Boer, SM, additional, Horeweg, N, additional, van Wezel, T, additional, Bosse, T, additional, and Creutzberg, CL, additional

Published
2020
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48. End-of-Life Trajectories of Patients With Hematological Malignancies and Patients With Advanced Solid Tumors Visiting the Emergency Department: The Need for a Proactive Integrated Care Approach

Author

Verhoef, M.J., Nijs, E.J.M. de, Ootjers, C.S., Fiocco, M., Fogteloo, A.J., Heringhaus, C., Marijnen, C.A.M., Horeweg, N., and Linden, Y.M. van der

Subjects
supportive care, hematological malignancy, palliative care, emergency department, cancer, end-of-life care
Abstract

Purpose: Patients with hematological malignancies (HM) have more unpredictable disease trajectories compared to patients with advanced solid tumors (STs) and miss opportunities for a palliative care approach. They often undergo intensive disease-directed treatments until the end of life with frequent emergency department (ED) visits and in-hospital deaths. Insight into end-of-life trajectories and quality of end-of-life care can support arranging appropriate care according to patients' wishes. Method: Mortality follow-back study to compare of end-of-life trajectories of HM and ST patients who died

Published
2019

50. Prognostic relevance of the molecular classification in high-risk endometrial cancer: analysis of the PORTEC-3 trial

Author

Leon-Castillo, A, primary, de Boer, SM, additional, Powell, ME, additional, Mileshkin, LR, additional, Mackay, HJ, additional, Leary, A, additional, Nijman, HW, additional, Singh, N, additional, Pollock, P, additional, Bessette, P, additional, Haie-Meder, C, additional, Smit, VTHBM, additional, Edmondson, RJ, additional, Putter, H, additional, Kitchener, HC, additional, Crosbie, EJ, additional, de Bruyn, M, additional, Nout, RA, additional, Horeweg, N, additional, Bosse, T, additional, and Creutzberg, CL, additional

Published
2019
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