Your search keyword '"Stefan Aebi"' showing total 153 results

1. Molecular characterization of breast cancer cell pools with normal or reduced ability to respond to progesterone: a study based on RNA-seq

Author

Mariana Bustamante Eduardo, Irene Keller, Nathalie Schuster, Stefan Aebi, and Rolf Jaggi

Subjects

Breast cancer, Estrogen receptor alpha, Progesterone receptor, Gene expression, RNA sequencing, CRISPR/Cas9, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

Abstract Background About one-third of patients with estrogen receptor alpha (ERα)-positive breast cancer have tumors which are progesterone receptor (PR) negative. PR is an important prognostic factor in breast cancer. Patients with ERα-positive/PR-negative tumors have shorter disease-free and overall survival than patients with ERα-positive/PR-positive tumors. New evidence has shown that progesterone (P4) has an anti-proliferative effect in ERα-positive breast cancer cells. However, the role of PR in breast cancer is only poorly understood. Methods We disrupted the PR gene (PGR) in ERα-positive/PR-positive T-47D cells using the CRISPR/Cas9 system. This resulted in cell pools we termed PR-low as P4 mediated effects were inhibited or blocked compared to control T-47D cells. We analyzed the gene expression profiles of PR-low and control T-47D cells in the absence of hormone and upon treatment with P4 alone or P4 together with estradiol (E2). Differentially expressed (DE) genes between experimental groups were characterized based on RNA-seq and Gene Ontology (GO) enrichment analyses. Results The overall gene expression pattern was very similar between untreated PR-low and untreated control T-47D cells. More than 6000 genes were DE in control T-47D cells upon stimulation with P4 or P4 plus E2. When PR-low pools were subjected to the same hormonal treatment, up- or downregulation was either blocked/absent or consistently lower. We identified more than 3000 genes that were DE between hormone-treated PR-low and control T-47D cells. GO analysis revealed seven significantly enriched biological processes affected by PR and associated with G protein-coupled receptor (GPCR) pathways which have been described to support growth, invasiveness, and metastasis in breast cancer cells. Conclusions The present study provides new insights into the complex role of PR in ERα-positive/PR-positive breast cancer cells. Many of the genes affected by PR are part of central biological processes of tumorigenesis.

Published

2023

2. Evaluation of multiple transcriptomic gene risk signatures in male breast cancer

Author

Jane Bayani, Coralie Poncet, Cheryl Crozier, Anouk Neven, Tammy Piper, Carrie Cunningham, Monika Sobol, Stefan Aebi, Kim Benstead, Oliver Bogler, Lissandra Dal Lago, Judith Fraser, Florentine Hilbers, Ingrid Hedenfalk, Larissa Korde, Barbro Linderholm, John Martens, Lavinia Middleton, Melissa Murray, Catherine Kelly, Cecilia Nilsson, Monika Nowaczyk, Stephanie Peeters, Aleksandra Peric, Peggy Porter, Carolien Schröder, Isabel T. Rubio, Kathryn J. Ruddy, Christi van Asperen, Danielle Van Den Weyngaert, Carolien van Deurzen, Elise van Leeuwen-Stok, Joanna Vermeij, Eric Winer, Sharon H. Giordano, Fatima Cardoso, and John M. S. Bartlett

Subjects

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

Abstract

Abstract Male breast cancer (BCa) is a rare disease accounting for less than 1% of all breast cancers and 1% of all cancers in males. The clinical management is largely extrapolated from female BCa. Several multigene assays are increasingly used to guide clinical treatment decisions in female BCa, however, there are limited data on the utility of these tests in male BCa. Here we present the gene expression results of 381 M0, ER+ve, HER2-ve male BCa patients enrolled in the Part 1 (retrospective analysis) of the International Male Breast Cancer Program. Using a custom NanoString™ panel comprised of the genes from the commercial risk tests Prosigna®, OncotypeDX®, and MammaPrint®, risk scores and intrinsic subtyping data were generated to recapitulate the commercial tests as described by us previously. We also examined the prognostic value of other risk scores such as the Genomic Grade Index (GGI), IHC4-mRNA and our prognostic 95-gene signature. In this sample set of male BCa, we demonstrated prognostic utility on univariate analysis. Across all signatures, patients whose samples were identified as low-risk experienced better outcomes than intermediate-risk, with those classed as high risk experiencing the poorest outcomes. As seen with female BCa, the concordance between tests was poor, with C-index values ranging from 40.3% to 78.2% and Kappa values ranging from 0.17 to 0.58. To our knowledge, this is the largest study of male breast cancers assayed to generate risk scores of the current commercial and academic risk tests demonstrating comparable clinical utility to female BCa.

Published

2021

3. Clinical Implementation of DPYD Pharmacogenetic Testing to Prevent Early-Onset Fluoropyrimidine-Related Toxicity in Cancer Patients in Switzerland

Author

Ursina B. M. Begré, Markus Jörger, Stefan Aebi, Ursula Amstutz, and Carlo R. Largiadèr

Subjects

adverse drug reactions, chemotherapy, clinical implementation, dihydropyrimidine dehydrogenase, DPYD, early adopter, Therapeutics. Pharmacology, RM1-950

Abstract

The implementation of pharmacogenetic testing into clinical practice has been a slow process so far. Here, we review the implementation of pre-treatment testing of dihydropyrimidine dehydrogenase gene (DPYD) risk variants to prevent early-onset fluoropyrimidine (FP)-related toxicity in cancer patients in Switzerland based on data of a large Swiss diagnostic center. In January 2017, the Swiss Federal Office of Public Health introduced the reimbursement of DPYD testing by the compulsory health insurance in Switzerland based on evidence for the clinical relevance of DPYD-risk variants and the cost-effectiveness of pre-treatment testing, and on the availability of international guidelines. However, we did not observe a strong increase in DPYD testing at our diagnostic center from 2017 to 2019. Only a low number of DPYD-testing requests (28–42 per year), concerning mostly retrospective investigations of suspected FP-toxicity, were received. In contrast, we observed a 14-fold increase in DPYD testing together with a strong shift from retrospective to pre-treatment test requests upon the release of recommendations for DPYD testing prior to FP-treatment in April 2020 by the European Medicines Agency. This increase was mainly driven by three geographic regions of Switzerland, where partner institutions of previous research collaborations regarding FP-related toxicity are located and who acted as early-adopting institutions of DPYD testing. Our data suggest the important role of early adopters as accelerators of clinical implementation of pharmacogenetic testing by introducing these policies to their working environment and educating health workers from their own and nearby institutions.

Published

2022

4. Locally advanced breast cancer

Author

Stefan Aebi, Per Karlsson, and Irene L. Wapnir

Subjects

Locally advanced breast cancer, Neoadjuvant systemic therapy, Multidisciplinary care, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Locally advanced breast cancer (LABC) is defined here as inoperable breast adenocarcinoma without distant metastases. Patients with LABC require a multidisciplinary approach. Given the risk of distant metastasis, staging exams are necessary. The incidence of LABC (stages IIIB and IIIC) has decreased in recent years. LABC has rarely been investigated separately: patients with LABC have participated both in clinical trials of palliative and of neoadjuvant therapy. Most trials did not analyze responses and long-term outcomes independently; thus, the treatment of patients with LABC is extrapolated from studies of patients with less or more advanced disease. Pathologic confirmation and molecular profiling are essential for the choice of neoadjuvant chemotherapy. Preoperative endocrine therapy may be considered in certain clinical situations; the addition of a CDK4/6 inhibitor is being investigated. HER2 positive LABCs are targeted with anti-HER2 agents combined with chemotherapy. PD-1 and PD-L1 antibodies in ‘triple-negative’ LABC are promising. Excellent responses to neoadjuvant therapy enable conservative surgery in many patients; however, inflammatory breast cancer may still indicate mastectomy. Postoperative radiotherapy is usually indicated. Target volumes include breast/chest wall, axillary, supraclavicular and internal mammary nodal basins. Preoperative radiation therapy can be useful in patients without response to systemic therapies. Palliative surgery for poor responders after neoadjuvant systemic and radiation therapy can be considered. Multidisciplinary teams can optimize local control and prevent relapses. However, modest improvement in survival was achieved between 2000 and 2014 underscoring the unmet need in patients with LABC who will benefit from specific research efforts in this disease entity.

Published

2022

5. Long-term responders to trastuzumab monotherapy in first-line HER-2+ advanced breast cancer: characteristics and survival data

Author

Sabine Schmid, Dirk Klingbiel, Stefan Aebi, Aron Goldhirsch, Christoph Mamot, Elisabetta Munzone, Franco Nolè, Christian Oehlschlegel, Olivia Pagani, Bernhard Pestalozzi, Christoph Rochlitz, Beat Thürlimann, Roger von Moos, Patrik Weder, Khalil Zaman, and Thomas Ruhstaller

Subjects

HER-positive breast cancer, Trastuzumab monotherapy, Long-term responders, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background The impact of HER2-targeted therapy alone followed by the addition of chemotherapy at disease progression (PD) versus upfront combination was investigated by the SAKK 22/99 trial. The aim of this exploratory analysis of the SAKK 22/99 trial was to characterize the specific subset of patients deriving long-term benefit from trastuzumab monotherapy alone and to identify potential predictive factors of long-term response. Methods This is an unplanned post-hoc analysis of patients randomized to Arm A (trastuzumab monotherapy). Patients were divided in two groups: patients with durable clinical benefit from trastuzumab monotherapy and short-term responders without durable clinical benefit from trastuzumab monotherapy Univariate and multivariate analyses of clinical characteristics correlating with response duration was performed. Results Eighty six patients were randomized in arm A, 24 patients (28%) were long-term responders and 62 (72%) were short-term responders with a 5y-overall survival (OS) of 54% (95% CI 31–72) and of 18% (95%CI 10–30), respectively. Absence of ER expression, absence of PgR expression and presence of visceral disease emerged as possible negative predictive factors for durable clinical benefit. Conclusion Durable clinical benefit can be achieved with trastuzumab monotherapy in a subgroup of HER2-positive patients with advanced disease and it is predictive for longer OS. Further investigations of predictive biomarkers are necessary to better characterize this subgroup of patients and develop further de-escalating strategies. Trial registration NCT00004935; first posted 27.01.2003, retrospectively registered.

Published

2019

6. Characterization of molecular scores and gene expression signatures in primary breast cancer, local recurrences and brain metastases

Author

Mariana Bustamante Eduardo, Vlad Popovici, Sara Imboden, Stefan Aebi, Nadja Ballabio, Hans Jörg Altermatt, Andreas Günthert, and Rolf Jaggi

Subjects

Breast cancer, Molecular risk scores, Local recurrence, Brain metastasis, PAM50 subtypes, Gene expression measurement, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Breast cancer is a leading cause of cancer-related death in women worldwide. Despite extensive studies in all areas of basic, clinical and applied research, accurate prognosis remains elusive, thus leading to overtreatment of many patients. Diagnosis could be improved by introducing multigene molecular scores in standard clinical practice. Several tests that work with formalin-fixed tissue have become routine. Molecular scores usually include several genes representing processes, response to oestrogens, progestogens and human epidermal growth factor receptor 2 (Her2), respectively, which are combined additively in single values. These multi-gene scores have the advantage of being more robust and reproducible than single-gene scores. Their utility may be further enhanced by combining them with classical diagnostic parameters. Here, we present an exploratory study comparing the RISK and research versions of Oncotype DX recurrence score (RS), Prosigna Risk of Recurrence (ROR) and EndoPredict (EP) with respect to their prognostic potential for ipsilateral recurrence and/or distant relapse in brain, and we compared the scores to the intrinsic subtypes based on PAM50. Methods RNA was extracted from formalin-fixed, paraffin-embedded (FFPE) tissue cores of primary tumours, local recurrences and brain metastases. Gene expression was measured on a NanoString nCounter Analysis System. Intrinsic subtypes and molecular scores were computed according to published literature and RISK, RS, ROR and EP were compared against each other and to the intrinsic subtypes Luminal A (lumA), Luminal B (lumB), Her2-enriched (Her2↑), Basal-like (basal), and Normal-like (normal) of PAM50. Local recurrences and brain metastases were compared to their corresponding primary tumours. Results All four molecular scores were highly correlated. Highest correlations were observed among genes related to proliferation while lower correlations were found among oestrogen-related genes. The scores were significantly higher in primary tumours progressing to brain metastases as compared to recurrence-free primary tumours and primary tumours that relapsed as local recurrences. Conclusions RISK and ROR-P are prognostic for primary tumours metastasizing to the brain. All four scores, RISK, RS, EP and ROR-P failed to discriminate between primary tumours that remained recurrence-free and primary tumours relapsing as local recurrences.

Published

2019

7. Fluoropyrimidine chemotherapy: recommendations for DPYD genotyping and therapeutic drug monitoring of the Swiss Group of Pharmacogenomics and Personalised Therapy

Author

Seid Hamzic, Stefan Aebi, Markus Joerger, Michael Montemurro, Marc Ansari, Ursula Amstutz, and Carlo Largiadèr

Subjects

fluoropyrimidines, 5-fluorouracil, capecitabine, therapeutic drug monitoring, chemotherapy, pharmacogenomics, Medicine

Abstract

Fluoropyrimidines (FPs), mainly 5-fluorouracil (5-FU) and its oral prodrug capecitabine (Cap), remain the backbone of the treatment of many different solid tumors. Despite their broad use in clinical routine, 10–40% of patients experience severe, and in rare cases (0.2–0.5%) even lethal, FP-related toxicity in early chemotherapy cycles. Today, there is a plethora of evidence that genetic variants in the gene encoding for the 5-FU catabolising enzyme dihydropyrimidine dehydrogenase (DPD, encoded by DPYD) are predictive of severe FP-related toxicities, and international clinical practice recommendations for DPYD genotype-guided FP dosing and therapeutic drug monitoring (TDM) are available. In spite of this strong evidence and DPYD genotyping becoming standard practice in other countries, it is has not been widely adopted in Switzerland to date. Here, we discuss current guidelines on genotype-guided FP dosing and TDM, and propose recommendations tailored to the situation in Switzerland to facilitate their clinical uptake for the further individualisation of FP chemotherapy. We recommend preemptive testing of four DPYD variants (c.1905+1G>A (rs3918290), c.1679T>G (rs55886062), c.2846A>T (rs67376798) and c.1129-5923C>G (rs75017182, c.1236G>A/HapB3)) in patients with an indication for FP-based chemotherapy, with the costs reimbursed through the compulsory health insurance in Switzerland. Carriers of these variants (6.5% in the Swiss population) have a 40–50% risk of developing severe early-onset toxicity when treated with standard FP doses. In these patients, we therefore recommend the use of a reduced starting dose, based on a dose adjustment scheme provided herein. Furthermore, we recommend the use of infusional 5-FU in patients with a DPYD risk genotype in order to enable TDM-based dose escalation. Only if the use of an infusional 5-FU regimen is not feasible should a slow titration of Cap, starting with the recommended reduced dose and basing further doses on monitoring of toxicity, be considered. Given that several studies have shown that TDM in 5-FU treatment improves not only the therapy’s safety, but potentially also its efficacy, we also include detailed TDM-based dosing guidelines and discuss the pre-analytical aspects of 5-FU TDM.

Published

2020

8. Adjuvant treatment recommendations for patients with ER-positive/HER2-negative early breast cancer by Swiss tumor boards using the 21-gene recurrence score (SAKK 26/10)

Author

Bernhard C. Pestalozzi, Christoph Tausch, Konstantin J. Dedes, Christoph Rochlitz, Stefan Zimmermann, Roger von Moos, Ralph Winterhalder, Thomas Ruhstaller, Andreas Mueller, Katharina Buser, Markus Borner, Urban Novak, Catrina Uhlmann Nussbaum, Bettina Seifert, Martin Bigler, Vincent Bize, Simona Berardi Vilei, Christoph Rageth, Stefan Aebi, and The Swiss Group for Clinical Cancer Research (SAKK)

Subjects

ER-positive early breast cancer, Adjuvant treatment recommendation, Multigene expression profiling, Recurrence score, Oncotype DX, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background To evaluate the effect of Recurrence Score® results (RS; Oncotype DX® multigene assay ODX) on treatment recommendations by Swiss multidisciplinary tumor boards (TB). Methods SAKK 26/10 is a multicenter, prospective cohort study of early breast cancer patients: Eligibility: R0-resection, ≥10% ER+ malignant cells, HER2–, pN0/pN1a. Patients were stratified into low-risk (LR) and non-low-risk (NLR) groups based on involved nodes (0 vs 1–3) and five additional predefined risk factors. Recommendations were classified as hormonal therapy (HT) or chemotherapy plus HT (CT + HT). Investigators were blinded to the statistical analysis plan. A 5%/10% rate of recommendation change in LR/NLR groups, respectively, was assumed independently of RS (null hypotheses). Results Two hundred twenty two evaluable patients from 18 centers had TB recommendations before and after consideration of the RS result. A recommendation change occurred in 45 patients (23/154 (15%, 95% CI 10–22%) in the LR group and 22/68 (32%, 95% CI 22–45%) in the NLR group). In both groups the null hypothesis could be rejected (both p

Published

2017

9. Abstract PD6-11: PD6-11 Evaluation of the Sensitivity to Endocrine Therapy Index (SET2,3) in Early Male Breast Cancer: Results from an analysis in the EORTC 10085/TBCRC/BIG/NCTN International Male Breast Cancer Program

Author

Danielle B. Zakon, Coralie Poncet, Fatima Cardoso, Neven Anouk, Vicente Valero, Stefan Aebi, Kim Benstead, Oliver Bogler, Lissandra Dal Lago, Judith Fraser, Carmela Caballero, Ingrid A. Hedenfalk, Larissa A. Korde, Barbro Linderholm, John WM Martens, Lavinia P. Middleton, Melissa Murray, Catherine M. Kelly, Cecilia Nilsson, Monika Nowaczyk, Stephanie Peeters, Melanie Beauvois, Peggy Porter, Carolien P. Schroder, Isabel T. Rubio, Kathryn Ruddy, Christi van Asperen, Danielle Van Den Weyngaert, Carolien HM van Deurzen, Elise van Leeuwen-Stok, Joanna M. Vermeij, John MS Bartlett, Antonio C. Wolff, Sharon H. Giordano, and W. Fraser Symmans

Subjects

Cancer Research, Oncology

Abstract

Introduction Breast cancer is uncommon in men. Almost all male breast cancers are hormone receptor-positive, HER2-negative, although the pathogenesis is not always attributable to an endocrine condition. A few studies have compared biological characteristics or molecular signatures with breast cancers in women. We sought to evaluate whether hormone receptor-related gene expression is different in cancers from men compared to equivalent cancers from women. SET2,3 index measures non-proliferative hormone receptor-related transcriptional activity in the cancer (SET-ER/PR index) and adjusts this for a Baseline Prognosis Index (BPI) that combines the measurements of tumor and nodal stage with a 4-gene molecular subtype (ESR1, PGR, ERBB2, and AURKA). Methods We received aliquots of total RNA from male patients with breast cancer included in the retrospective cohort study of the EORTC 10085/BCG/TBCRC/BIG/NCTN International Male Breast Cancer Program (NCT01101425). SET2,3 assay was performed using the QuantiGene assay (Thermo Fisher) using bead-based hybridization and laser spectroscopy (Luminex). The statistical analyses were performed by the EORTC statistician. The primary objective of the study was the assessment of the prognostic value of the SET2,3 index score in patients with early-stage hormone receptor-positive, HER2-negative male breast cancer, treated with endocrine therapy. Clinical outcomes (recurrence-free survival – RFS; overall survival – OS) were estimated by Kaplan-Meier curves and secondarily compared using multivariable Cox models adjusted for continuous SET2,3 index, tumor size, nodal status, age, and chemotherapy and radiotherapy use. An exploratory analysis to compare the SET2,3 index scores distribution in female and male breast cancer patients was also performed using results from the same assay performed on cancers from women selected on the same inclusion criteria. Due to the low numbers of male patients treated with neoadjuvant treatment (N=6), this analysis was restricted to patients treated with adjuvant treatment (n=315 male and 660 female). Results Of the 321 male patients with breast cancer analyzed, treated between 1990 and 2010, 211 (65.7%) were categorized as high SET2,3 index score, reflecting a high endocrine activity in the cancer and low risk of recurrence, and 110 patients (34.3%) categorized as being low score, reflecting low endocrine activity and high risk of recurrence. At 5 years, the RFS was 75.0% (95% CI, 67.4-81.1) in the high SET2,3 group versus 60.7% (95% CI, 49.1-70.5) in the low SET2,3 group (HR univariate, 0.49; 95% CI, 0.34-0.70; P< 0.0001). The 5-year OS rate among patients with a high SET2,3 index was 84.3% (95% CI, 45.5-73.8), in contrast of 67.8% (95% CI, 56.6-76.7) in the low SET2,3 group (HR univariate, 0.44; 95% CI, 0.30-0.65; P< 0.0001). SET2,3 was independently prognostic for OS, but not RFS in multivariable Cox models. In patients classified as low SET2,3, the addition of neo/adjuvant chemotherapy to adjuvant endocrine therapy was associated with 5-year OS of 76.0% (95% CI, 59.5-86.4) and in patients who received endocrine therapy alone the 5-year OS was 61.3% (95% CI, 45.5-73.8), an absolute difference of 14.7 percentage points. Overall, we did not observe a difference in the distributions (median, interquartile range) of SET2,3 index between men (2.4, 1.9–2.6) and women (2.3, 2.0–2.7). Conclusion SET2,3 index measurements of endocrine-related transcriptional activity in male patients with breast cancer were not different from measurements in female patients with breast cancer. SET2,3 was prognostic in male breast cancer and our exploratory analysis suggests that chemotherapy might improve the poor prognosis for men with breast cancer that has low SET2,3 index. This study was funded by the Breast Cancer Research Foundation (BCRF). Citation Format: Danielle B. Zakon, Coralie Poncet, Fatima Cardoso, Neven Anouk, Vicente Valero, Stefan Aebi, Kim Benstead, Oliver Bogler, Lissandra Dal Lago, Judith Fraser, Carmela Caballero, Ingrid A. Hedenfalk, Larissa A. Korde, Barbro Linderholm, John WM Martens, Lavinia P. Middleton, Melissa Murray, Catherine M. Kelly, Cecilia Nilsson, Monika Nowaczyk, Stephanie Peeters, Melanie Beauvois, Peggy Porter, Carolien P. Schroder, Isabel T. Rubio, Kathryn Ruddy, Christi van Asperen, Danielle Van Den Weyngaert, Carolien HM van Deurzen, Elise van Leeuwen-Stok, Joanna M. Vermeij, John MS Bartlett, Antonio C. Wolff, Sharon H. Giordano, W. Fraser Symmans. PD6-11 Evaluation of the Sensitivity to Endocrine Therapy Index (SET2,3) in Early Male Breast Cancer: Results from an analysis in the EORTC 10085/TBCRC/BIG/NCTN International Male Breast Cancer Program [abstract]. In: Proceedings of the 2022 San Antonio Breast Cancer Symposium; 2022 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2023;83(5 Suppl):Abstract nr PD6-11.

Published

2023

10. Abstract P3-05-28: Impact of increased adiposity on extended aromatase inhibitor treatment in postmenopausal patients with estrogen receptor positive (ER+) breast cancer: a retrospective analysis of the SOLE trial

Author

Edoardo Isnaldi, François Richard, Giuseppe Marano, Patrizia Boracchi, Marion Maetens, Giuseppe Floris, Guy Jerusalem, Andrea Gombos, Alastair M. Thompson, Erika Hitre, Stefan Aebi, Marco Colleoni, Patrizia Dell’Orto, Roswitha Kammler, Patrick Neven, Giuseppe Viale, Meredith Regan, Elia Biganzoli, and Christine Desmedt

Subjects

Cancer Research, Oncology

Abstract

Background: The risk of late distant recurrence (≥ 5 years) in post-menopausal patients with ER+ BC remains significant even after standard adjuvant endocrine therapy (ET). Obesity, which has reached high proportions in Western Countries, is one of the modifiable factors that can contribute to BC recurrences. While body mass index (BMI) is an easily available surrogate measure of adiposity, it might not reflect accurately patient adiposity, especially in post-menopausal patients. We therefore hypothesize that mammary adipocyte measurements might better capture the adiposity of the patient. In this study, we retrospectively evaluated the prognostic role of both BMI and adipocyte measurements in the SOLE trial. Patients & Methods: The SOLE trial (NCT00553410) consisted of 4,884 postmenopausal women with hormone receptor positive, lymph node-positive BC treated with 5 years of letrozole after having completed 4-6 years of adjuvant ET. BMI was available for 3,606 patients with ER+/HER2- BC and categorized according to the WHO classification (underweight: < 18.5, normal weight 18.5 – 24.9, overweight 25 – 29.9, obesity ≥ 30 kg/m2). Considering the small sample size, patients with underweight (n=35) were grouped together with patients with normal weight for the subsequent analyses. We evaluated the association between clinico-pathological characteristics and BMI using Fisher exact test and Kruskal-Wallis test. Given the previously reported association of BMI with distant recurrences (PMID: 21115856), we considered distant-relapse free interval (DRFI) as the main study endpoint. Cox regression analyses were adjusted for histology, chemotherapy (yes/no), type of local therapy, in addition to previously reported clinico-pathological variables (PMID: 29158011). Then, we conducted a stratified case-cohort study consisting of 311 patients (97 with distant relapse-cases) with successful digital assessment of adipocytes on normal mammary adipose tissue sample collected at surgery, as previously described (PMID: 33120083). Stratification factors were treatment arm and type of prior ET. Weighted Cox regression models (PMID: 17554753, 18712477) were used to evaluate prognostic association with adipocyte size (area in µm²) categorized in quartile of the 75th percentile (Q4 vs Q1-3), as done previously (PMID: 33753731). Results: 1392 (39%) patients were normal weight, 1315 (36%) were overweight and 899 (25%) were obese. Older age at diagnosis, lymph node involvement (≥4), large tumor size and menopausal status were associated with overweight and obesity. After a median follow-up of 84 months, no associations were found between DRFI and BMI in the univariable and multivariable analysis (adjusted HR overweight vs normal=0.99, 95%CI: 0.76 – 1.29, p=0.977 and HR obese vs normal=1.11, 95%CI: 0.84 - 1.47, p=0.425). In the case-cohort study, patients with larger adipocytes had an increased hazard of distant recurrence in the univariable and multivariable analysis (see table 1). Conclusion: In this study, we did not detect any association between BMI and survival outcomes. We however found that larger mammary adipocytes were independently associated with an increased hazard of distant recurrence. These results suggest that mammary adipocytes, which can be easily evaluated on H&E slides using digital pathology, should be considered as a novel marker to evaluate the risk of late recurrence in patients with breast cancer. Citation Format: Edoardo Isnaldi, François Richard, Giuseppe Marano, Patrizia Boracchi, Marion Maetens, Giuseppe Floris, Guy Jerusalem, Andrea Gombos, Alastair M. Thompson, Erika Hitre, Stefan Aebi, Marco Colleoni, Patrizia Dell’Orto, Roswitha Kammler, Patrick Neven, Giuseppe Viale, Meredith Regan, Elia Biganzoli, Christine Desmedt. Impact of increased adiposity on extended aromatase inhibitor treatment in postmenopausal patients with estrogen receptor positive (ER+) breast cancer: a retrospective analysis of the SOLE trial [abstract]. In: Proceedings of the 2022 San Antonio Breast Cancer Symposium; 2022 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2023;83(5 Suppl):Abstract nr P3-05-28.

Published

2023

11. Endokrine Therapien beim Mammakarzinom

Author

Sonja Stettler and Stefan Aebi

Subjects

General Medicine

Abstract

Zusammenfassung. Das Mammakarzinom, die häufigste Krebserkrankung der Frau, exprimiert bei etwa 75% Östrogen- und/oder Progesteronrezeptoren. Diese therapeutisch und prognostisch wichtige Eigenschaft erlaubt den Einsatz der endokrinen Therapien. Die adjuvante endokrine Therapie mit Tamoxifen über fünf Jahre reduziert die Sterblichkeit um 33%, und das Restrisiko lässt sich mit Aromatasehemmern und mit verlängerter Behandlung um weitere 20% vermindern. Bei Patientinnen mit fortgeschrittener Erkrankung ist die mediane Wirkdauer einer ersten endokrinen Therapie etwa zwölf Monate, die mediane Überlebenszeit zwischen 20 und 40 Monaten. Je nach Situation der Tumorerkrankung unterscheidet sich der Einsatz der verschiedenen Substanzen in Therapiedauer, -sequenz und Wirkstoffkombinationen, besonders mit CDK4/6-Inhibitoren. Endokrine Therapien werden über einen längeren Zeitraum verschrieben. Eine optimale Kontrolle der Nebenwirkungen zur Verbesserung der Therapietreue ist daher wichtig.

Published

2022

12. Table S1 from Genomic Aberrations and Late Recurrence in Postmenopausal Women with Hormone Receptor–positive Early Breast Cancer: Results from the SOLE Trial

Author

Marco Colleoni, Meredith M. Regan, Massimo Barberis, Giuseppe Viale, Aron Goldhirsch, Angelo Di Leo, Seamus O’Reilly, Bettina Müller, Katsumasa Kuroi, Joaquín Gavilá, Sibylle Loibl, Christel Fontaine, Matthew Barber, Marie-Pascale Graas, Alastair Thompson, Vincenzo Di Lauro, Jacquie Chirgwin, Stefan Aebi, Per Karlsson, Ines Deleu, Andrea Gombos, Edda Simoncini, Guy Jerusalem, Erika Hitre, Patrick Neven, Roswitha Kammler, Elisabetta Munzone, Paola Rafaniello Raviele, Isabella Leone, Marta Rita Reforgiato, Caterina Fumagalli, Kathryn P. Gray, and Elena Guerini-Rocco

Abstract

Clinico-pathologic characteristics of patients according to NGS results (success/failure).

Published

2023

13. Figure S2 from Genomic Aberrations and Late Recurrence in Postmenopausal Women with Hormone Receptor–positive Early Breast Cancer: Results from the SOLE Trial

Author

Marco Colleoni, Meredith M. Regan, Massimo Barberis, Giuseppe Viale, Aron Goldhirsch, Angelo Di Leo, Seamus O’Reilly, Bettina Müller, Katsumasa Kuroi, Joaquín Gavilá, Sibylle Loibl, Christel Fontaine, Matthew Barber, Marie-Pascale Graas, Alastair Thompson, Vincenzo Di Lauro, Jacquie Chirgwin, Stefan Aebi, Per Karlsson, Ines Deleu, Andrea Gombos, Edda Simoncini, Guy Jerusalem, Erika Hitre, Patrick Neven, Roswitha Kammler, Elisabetta Munzone, Paola Rafaniello Raviele, Isabella Leone, Marta Rita Reforgiato, Caterina Fumagalli, Kathryn P. Gray, and Elena Guerini-Rocco

Abstract

Weighted Kaplan-Meier (KM) estimates of breast cancer-free interval (BCFI) and distant recurrence-free interval (DRFI) according to tumor subtype, separately by PIK3CA mutational status (mutated, MUT vs wild-type, WT). The 5-year event-free estimates (95% CI) are provided. Hazard ratio (HR) estimates (95% CI) and log-rank tests from weighted univariate models.

Published

2023

14. Data from Genomic Aberrations and Late Recurrence in Postmenopausal Women with Hormone Receptor–positive Early Breast Cancer: Results from the SOLE Trial

Author

Marco Colleoni, Meredith M. Regan, Massimo Barberis, Giuseppe Viale, Aron Goldhirsch, Angelo Di Leo, Seamus O’Reilly, Bettina Müller, Katsumasa Kuroi, Joaquín Gavilá, Sibylle Loibl, Christel Fontaine, Matthew Barber, Marie-Pascale Graas, Alastair Thompson, Vincenzo Di Lauro, Jacquie Chirgwin, Stefan Aebi, Per Karlsson, Ines Deleu, Andrea Gombos, Edda Simoncini, Guy Jerusalem, Erika Hitre, Patrick Neven, Roswitha Kammler, Elisabetta Munzone, Paola Rafaniello Raviele, Isabella Leone, Marta Rita Reforgiato, Caterina Fumagalli, Kathryn P. Gray, and Elena Guerini-Rocco

Abstract

Purpose:Women with hormone receptor–positive early breast cancers have a persistent risk of relapse and biomarkers for late recurrence are needed. We sought to identify tumor genomic aberrations associated with increased late-recurrence risk.Experimental Design:In a secondary analysis of Study of Letrozole Extension trial, a case-cohort–like sampling selected 598 primary breast cancers for targeted next-generation sequencing analysis of gene mutations and copy-number gains (CNGs). Correlations of genomic aberrations with clinicopathologic factors and breast and distant recurrence-free intervals (BCFIs and DRFIs) were analyzed using weighted Cox models.Results:Analysis of mutations and CNGs was successfully performed for 403 and 350 samples, including 148 and 134 patients with breast cancer recurrences (median follow-up time, 5.2 years), respectively. The most frequent alterations were PIK3CA mutations (42%) and CNGs of CCND1 (15%), ERBB2 (10%), FGFR1 (8%), and MYC (8%). PIK3CA mutations and MYC CNGs were associated with lower (P = 0.03) and higher (P = 0.004) tumor grade, respectively; a higher Ki-67 was seen in tumor with CCND1, ERBB2, and MYC CNGs (P = 0.01, P < 0.001, and P = 0.03, respectively). FGFR1 CNG was associated with an increased risk of late events in univariate analyses [17/29 patients; BCFI: HR, 3.2; 95% confidence interval (CI), 1.48–6.92; P = 0.003 and DRFI: HR, 3.5; 95% CI, 1.61–7.75; P = 0.002) and in multivariable models adjusted for clinicopathologic factors.Conclusions:Postmenopausal women with hormone receptor–positive early breast cancer harboring FGFR1 CNG had an increased risk of late recurrence despite extended therapy. FGFR1 CNG may represent a useful prognostic biomarker for late recurrence and a therapeutic target.

Published

2023

15. «Less is more» pour les traitements médicamenteux des cancers

Author

Magdalena Hecz, Stefan Aebi, Beat Mller, Thilo Zander, Christian Riklin, Ralph Winterhalder, Daniela Weiler, Kristin Zeidler, Veronika Blum, Philipp Niederberger, Benedetta Campana, and Oliver Gautschi

Subjects

General Medicine

Published

2023

16. «Less is more» bei medikamentösen Tumortherapien

Author

Magdalena Hecz, Stefan Aebi, Beat Mller, Thilo Zander, Christian Riklin, Ralph Winterhalder, Daniela Weiler, Kristin Zeidler, Veronika Blum, Philipp Niederberger, Benedetta Campana, and Oliver Gautschi

Subjects

General Medicine

Published

2023

17. Continuous versus intermittent extended adjuvant letrozole for breast cancer: final results of randomized phase III SOLE (Study of Letrozole Extension) and SOLE Estrogen Substudy

Author

Richard D. Gelber, Erika Hitre, Andrea Gombos, Alan S. Coates, Alastair M. Thompson, Sole Investigators, Barbara Ruepp, J Chirgwin, Bettina Müller, Marie-Pascale Graas, Stefan Aebi, Subrina Farah, Joaquín Gavilá, Patrick Neven, K. Ribi, A Courtois, Christian Marth, E Abdi, Per Karlsson, Harold J. Burstein, Katsumasa Kuroi, Seamus O'Reilly, A. Goldhirsch, Thomas Ruhstaller, S. Loibl, Manuela Rabaglio, Marco Colleoni, G. Jerusalem, Giulia Viale, C Kamby, Sherene Loi, Edda Simoncini, and Meredith M. Regan

Subjects

medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Population, Urology, Breast Neoplasms, Disease-Free Survival, Breast cancer, Nitriles, medicine, Humans, 610 Medicine & health, Adverse effect, education, education.field_of_study, Aromatase Inhibitors, business.industry, Letrozole, Hazard ratio, Estrogens, Hematology, Triazoles, medicine.disease, Confidence interval, Postmenopause, Tamoxifen, Receptors, Estrogen, Oncology, Chemotherapy, Adjuvant, Estrogen, Female, Receptors, Progesterone, business, Adjuvant, medicine.drug

Abstract

BACKGROUND Late recurrences in postmenopausal women with hormone receptor-positive breast cancers remain an important challenge. Avoidance or delayed development of resistance represents the main objective in extended endocrine therapy (ET). In animal models, resistance was reversed with restoration of circulating estrogen levels during interruption of letrozole treatment. This phase III, randomized, open-label Study of Letrozole Extension (SOLE) studied the effect of extended intermittent letrozole treatment in comparison with continuous letrozole. In parallel, the SOLE estrogen substudy (SOLE-EST) analyzed the levels of estrogen during the interruption of treatment. PATIENTS AND METHODS SOLE enrolled 4884 postmenopausal women with hormone receptor-positive, lymph node-positive, operable breast cancer between December 2007 and October 2012 and among them, 104 patients were enrolled in SOLE-EST. They must have undergone local treatment and have completed 4-6 years of adjuvant ET. Patients were randomized between continuous letrozole (2.5 mg/day orally for 5 years) and intermittent letrozole treatment (2.5 mg/day for 9 months followed by a 3-month interruption in years 1-4 and then 2.5 mg/day during all of year 5). RESULTS Intention-to-treat population included 4851 women in SOLE (n��= 2425 in the intermittent and n��= 2426 in the continuous letrozole groups) and 103 women in SOLE-EST (n��= 78 in the intermittent and n��= 25 in the continuous letrozole groups). After a median follow-up of 84 months, 7-year disease-free survival (DFS) was 81.4% in the intermittent group and 81.5% in the continuous group (hazard ratio: 1.03, 95% confidence interval: 0.91-1.17). Reported adverse events were similar in both groups. Circulating estrogen recovery was demonstrated within 6 weeks after the stop of letrozole treatment. CONCLUSIONS Extended adjuvant ET by intermittent administration of letrozole did not improve DFS compared with continuous use, despite the recovery of circulating estrogen levels. The similar DFS coupled with previously reported quality-of-life advantages suggest intermittent extended treatment is a valid option for patients who require or prefer a treatment interruption.

Published

2021

18. [Endocrine Treatments in Breast Cancer]

Author

Sonja, Stettler and Stefan, Aebi

Subjects

Tamoxifen, Aromatase Inhibitors, Chemotherapy, Adjuvant, Humans, Breast Neoplasms, Female

Abstract

Endocrine Treatments in Breast Cancer

Published

2022

19. Genomic Aberrations and Late Recurrence in Postmenopausal Women with Hormone Receptor–positive Early Breast Cancer: Results from the SOLE Trial

Author

Vincenzo Di Lauro, Andrea Gombos, Ines Deleu, Matthew Barber, Bettina Müller, Roswitha Kammler, Jacquie Chirgwin, Caterina Fumagalli, Guy Jerusalem, Edda Simoncini, Katsumasa Kuroi, Meredith M. Regan, Christel Fontaine, Isabella Leone, Massimo Barberis, Marta Rita Reforgiato, Marco Colleoni, Stefan Aebi, Erika Hitre, Kathryn P. Gray, Paola Rafaniello Raviele, Joaquín Gavilá, Aron Goldhirsch, Angelo Di Leo, Per Karlsson, Elena Guerini-Rocco, Seamus O'Reilly, Elisabetta Munzone, Patrick Neven, Sibylle Loibl, Giuseppe Viale, Alastair M. Thompson, Marie-Pascale Graas, Clinical sciences, Medical Oncology, and Laboratory of Molecular and Medical Oncology

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Antineoplastic Agents, Breast Neoplasms, Kaplan-Meier Estimate, Gene mutation, Polymorphism, Single Nucleotide, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Cyclin D1, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Aged, Chromosome Aberrations, Proportional hazards model, business.industry, Fibroblast growth factor receptor 1, Letrozole, High-Throughput Nucleotide Sequencing, Genomics, Middle Aged, medicine.disease, Postmenopause, Treatment Outcome, 030104 developmental biology, Receptors, Estrogen, Hormone receptor, 030220 oncology & carcinogenesis, Mutation, Female, Neoplasm Recurrence, Local, business, Hormone, medicine.drug

Abstract

Purpose:Women with hormone receptor–positive early breast cancers have a persistent risk of relapse and biomarkers for late recurrence are needed. We sought to identify tumor genomic aberrations associated with increased late-recurrence risk.Experimental Design:In a secondary analysis of Study of Letrozole Extension trial, a case-cohort–like sampling selected 598 primary breast cancers for targeted next-generation sequencing analysis of gene mutations and copy-number gains (CNGs). Correlations of genomic aberrations with clinicopathologic factors and breast and distant recurrence-free intervals (BCFIs and DRFIs) were analyzed using weighted Cox models.Results:Analysis of mutations and CNGs was successfully performed for 403 and 350 samples, including 148 and 134 patients with breast cancer recurrences (median follow-up time, 5.2 years), respectively. The most frequent alterations were PIK3CA mutations (42%) and CNGs of CCND1 (15%), ERBB2 (10%), FGFR1 (8%), and MYC (8%). PIK3CA mutations and MYC CNGs were associated with lower (P = 0.03) and higher (P = 0.004) tumor grade, respectively; a higher Ki-67 was seen in tumor with CCND1, ERBB2, and MYC CNGs (P = 0.01, P < 0.001, and P = 0.03, respectively). FGFR1 CNG was associated with an increased risk of late events in univariate analyses [17/29 patients; BCFI: HR, 3.2; 95% confidence interval (CI), 1.48–6.92; P = 0.003 and DRFI: HR, 3.5; 95% CI, 1.61–7.75; P = 0.002) and in multivariable models adjusted for clinicopathologic factors.Conclusions:Postmenopausal women with hormone receptor–positive early breast cancer harboring FGFR1 CNG had an increased risk of late recurrence despite extended therapy. FGFR1 CNG may represent a useful prognostic biomarker for late recurrence and a therapeutic target.

Published

2021

20. Abstract P4-10-03: The genomic landscape of male breast cancers using the oncomine comprehensive assay for actionable mutations

Author

John M. S. Bartlett, Megan Hopkins, C. Poncet, Stefan Aebi, Peggy L. Porter, Elise van Leeuwen-Stok, Carolien H.M. van Deurzen, Quang M. Trinh, Kim Benstead, M Nowaczyk, Cecilia Nilsson, Lavinia P. Middleton, Lincoln Stein, Cheryl Crozier, Monika Sobol, Ingrid Hedenfalk, Sharon H. Giordano, Oliver Bogler, Jane Bayani, Joanna Vermeij, Lissandra Dal Lago, Christi J. van Asperen, Melissa Murray, Catherine M. Kelly, Kathryn J. Ruddy, Stéphanie Peeters, Tammy Piper, Carolien P. Schröder, Carrie Cunningham, Florentine Hilbers, Fatima Cardoso, Danielle Van den Weyngaert, Aime Lambert Uwimana, Aleksandra Peric, John W.M. Martens, Eric P. Winer, Isabel T. Rubio, Barbro Linderholm, and Larissa A. Korde

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Point mutation, Biology, medicine.disease, medicine.disease_cause, Breast cancer, Internal medicine, Male breast cancer, medicine, biology.protein, PTEN, Copy-number variation, KRAS, Indel, ATRX

Abstract

Introduction: Male breast cancer (BCa) is a rare disease accounting for less than 1% of all breast cancers (BC) and 1% of all cancers in males. The clinical management is largely extrapolated from female BCa. Few studies have examined the genomic landscape of male BCas, with six male BCas included in The Cancer Genome Atlas (TCGA). Familial studies of male BCas have shown genomic changes similar to female BCa, while a larger targeted sequencing study of 59 male breast cancers identified recurrent mutations affecting PIK3CA and GATA3. To date, there is still limited information regarding the genomic landscape of male BCas; particularly in the context of identifying targeted treatments. To reveal genomic changes that characterize male BCas in the context of known cancer driver genes linked to prognosis and targeted agents, we performed a targeted sequencing study on 248 male BCas from the International Male Breast Cancer Program. Methods: 248 primary M0, ER+ve, HER2-ve male BCas enrolled in the Part 1 (retrospective joint analysis) International Male Breast Cancer Program of 1483 patients diagnosed between 1990-2010 (Cardoso et al. Annals of Oncology, 2018) were processed for nucleic acid extraction from formalin-fixed paraffin embedded (FFPE) tissues. Using the Thermo Fisher Scientific Oncomine Comprehensive Assay v3 (OCAv3), a validated targeted sequencing panel currently used in the NCI-MATCH trial (NCT02465060), we evaluated mutational and copy number variations (CNVs) of genes that are prognostic or predictive to targeted therapies currently in use in the clinic or late-stage clinical trials. The OCAv3 DNA pan-cancer panel assays 115 genes for determining mutational status (48 full coding and 67 hotspot) as well as copy-number assessment in 43 genes. The OCAv3 uses Ampliseq-based technology linked to the Oncomine NGS workflow to identify actionable mutations and CNVs Results: Of the 248 samples assayed, 216 passed strict quality control parameters (87.1%). Using the Oncomine NGS workflow, actionable mutations at ≥5% variant allele frequency (VAF) were most frequently identified in PIK3CA (29.2%), BRCA2 (11.1%), NF1 (11.6%), indels in TP53 (10.6%), ATR (5.6%), ATRX (5.1%), indel BRCA2 (5.1%), TP53 point mutations (4.6%), MET (4.6%), ATM (4.6%), NOTCH2 (4.6%), CHEK1 (4.2%), FANCI (4.2%), PTEN (3.2%) with a number of additional genes identified at lower frequencies. Gene amplifications were most frequently detected in MYC (24.5%), FGFR1 (14.8%), CCND1 (12%), FGF3 (9.7%), FGF19 (9.7%), MDM2 (6.5%), CDK4 (1.4%), FGFR3, MDM4, ERBB2 (0.9% each), and FLT3, AR, MYCL, CDK6, IGF1R, FGFR4, KRAS, AKT3 and ESR1 (0.5% each). Although the results here describe the mutations and copy-number changes deemed to be actionable, further analysis of all non-actionable somatic mutations and CNVs will be presented and compared to female BCas previously assayed using the same panel. Conclusion: In this targeted sequencing study of the largest series of male BCas to our knowledge, we have revealed that PIK3CA continues to be a frequently altered gene in both male and female BCas. However, there is an enrichment of mutations in genes related to DNA repair in male BCs. Interestingly, while MYC is commonly amplified in female BCa, a higher frequency of amplified cases were seen in male BCas, in contrast to female BCas. Together with our previously generated transcriptional profiling data in this data set, we believe that both common and unique biological processes comprising male and female BCas will ultimately improve their clinical management and move towards the goal of precision medicine. This work has been funded by the Breast Cancer Research Foundation (BCRF). Citation Format: Jane Bayani, Coralie Poncet, Cheryl Crozier, Quang M Trinh, Megan Hopkins, Aime Lambert Uwimana, Tammy Piper, Carrie Cunningham, Monika Sobol, Stefan Aebi, Kim Benstead, Oliver Bogler, Lissandra Dal Lago, Florentine Hilbers, Ingrid Hedenfalk, Larissa Korde, Barbro Linderholm, John Martens, Lavinia Middleton, Melissa Murray, Catherine Kelly, Cecilia Nilsson, Monika Nowaczyk, Stephanie Peeters, Aleksandra Peric, Peggy Porter, Carolien Schröder, Isabel T Rubio, Kathryn J Ruddy, Christi van Asperen, Danielle Van Den Weyngaert, Carolien HM van Deurzen, Elise van Leeuwen-Stok, Joanna Vermeij, Eric Winer, Lincoln D Stein, Sharon H Giordano, Fatima Cardoso, John MS Bartlett. The genomic landscape of male breast cancers using the oncomine comprehensive assay for actionable mutations [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P4-10-03.

Published

2020

21. Abstract P5-12-01: SOLE (study of letrozole extension), a phase 3 randomized clinical trial of continuous vs intermittent letrozole in postmenopausal women who have received 4-6 years of adjuvant endocrine therapy for lymph node-positive, early breast cancer (BC): Final analysis and sole estrogen substudy (SOLE-EST)

Author

Bettina Müller, Per Karlsson, Stefan Aebi, Giuseppe Viale, Andrea Gombos, Edda Simoncini, Meredith M. Regan, Joaquín Gavilá, Christian Marth, Richard D. Gelber, Thomas Ruhstaller, Subrina Farah, Guy Jerusalem, Erika Hitre, Jacquie Chirgwin, Angelo Di Leo, Harold J. Burstein, Barbara Ruepp, Alan S. Coates, Aron Goldhirsch, Sibylle Loibl, Katsumasa Kuroi, Patrick Neven, Alastair M. Thompson, Seamus O'Reilly, Marie-Pascale Graas, Claus Kamby, Manuela Rabaglio, and Marco Colleoni

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Randomization, business.industry, medicine.drug_class, Letrozole, Cancer, medicine.disease, law.invention, Breast cancer, Randomized controlled trial, law, Estrogen, Internal medicine, medicine, Clinical endpoint, Adjuvant therapy, business, medicine.drug

Abstract

Background: In animal models of hormone receptor positive (HR+) breast cancer, acquired resistance to continued letrozole was shown to be reversed by estrogen-induced apoptosis. We hypothesized that the rise in estrogen levels during short treatment interruptions would resensitize breast cancer cells to letrozole and improve treatment outcome. SOLE tested the hypothesis that 3 mos treatment-free intervals during extended adjuvant therapy will improve disease-free survival (DFS). We previously reported the primary endpoint after 60 mos median follow-up: extended intermittent letrozole did not improve DFS vs extended continuous letrozole. However, only 9% of pts had breast cancer events, justifying updating the analysis with longer follow-up. The dynamic of recovery of estrogen levels after stopping letrozole therapy has not been previously reported. Methods: SOLE enrolled 4884 postmenopausal women with HR+ lymph node-positive BC who had completed 4-6 yrs of adjuvant endocrine therapy (19% SERM, 43% AI, 38% both; stratification factor). Pts were randomized to an additional 5 yrs continuous letrozole (2.5 mg daily; n=2441) vs 5 yrs intermittent letrozole (taken for the first 9 mos of yrs 1-4, and 12 mos in yr 5; n=2443). We report the final analysis of the SOLE trial after 84 mos median follow-up. In SOLE-EST, levels of estradiol (E2), estrone (E1) and estrone sulphate (E1S) at 0, 9, 10.5 and 12 mos after randomization were determined using a highly sensitive assay in a subgroup of 90 evaluable patients (21 in the continuous and 69 in the intermittent group). Results: There were 923 DFS events. 7 yr DFS was 81.5% in both groups. More pts had distant metastases in the continuous group (8.7% vs 7.5%) while second (non-breast) malignancies were more frequent in the intermittent group (5.5% vs 4.7%). Similar outcomes were observed for breast cancer-free interval (BCFI) (88.6% vs 88.0%), distant recurrence-free interval (DRFI) (91.6% vs 90.4%), and overall survival (OS) (90.6% vs 89.6%) for pts assigned intermittent vs continuous letrozole. In the intermittent group, median E2, E1 and E1S levels more than doubled compared with levels at 9 mos after randomization in the first 6 weeks after stopping letrozole during the treatment free interval while levels were stable for the 21 pts tested in the continuous group. Conclusions: Among postmenopausal women with HR+ BC, extended intermittent letrozole did not improve DFS vs continuous letrozole. Similar outcome was consistently observed for BCFI, DRFI and OS. The SOLE-EST substudy indicates an important increase in estrogen levels as soon as 6 weeks after stopping letrozole therapy in the intermittent group. Further investigation of prior exposure to aromatase inhibitors in relation with outcome and with E2, E1 and E1S levels in SOLE-EST are underway. Citation Format: Guy Jerusalem, Subrina Farah, Jacquie Chirgwin, Stefan Aebi, Per Karlsson, Patrick Neven, Erika Hitre, Marie-Pascale Graas, Edda Simoncini, Claus Kamby, Alastair Thompson, Sibylle Loibl, Joaquín Gavilá, Katsumasa Kuroi, Christian Marth, Bettina Müller, Seamus O'Reilly, Andrea Gombos, Thomas Ruhstaller, Harold Burstein, Manuela Rabaglio, Barbara Ruepp, Giuseppe Viale, Richard D Gelber, Alan S Coates, Angelo Di Leo, Aron Goldhirsch, Meredith Regan, Marco Colleoni. SOLE (study of letrozole extension), a phase 3 randomized clinical trial of continuous vs intermittent letrozole in postmenopausal women who have received 4-6 years of adjuvant endocrine therapy for lymph node-positive, early breast cancer (BC): Final analysis and sole estrogen substudy (SOLE-EST) [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P5-12-01.

Published

2020

22. Clinical Implementation of

Author

Ursina B M, Begré, Markus, Jörger, Stefan, Aebi, Ursula, Amstutz, and Carlo R, Largiadèr

Abstract

The implementation of pharmacogenetic testing into clinical practice has been a slow process so far. Here, we review the implementation of pre-treatment testing of dihydropyrimidine dehydrogenase gene (

Published

2022

23. Abstract P4-01-25: Safety analysis after 11 years of follow-up of the randomized phase III trial SAKK22/99: upfront chemotherapy in advanced HER2 positive breast cancer

Author

Manuela Rabaglio, Daniel Dietrich, Bernhard Scheibe, Thomas Ruhstaller, Franco Nole, Serenella Eppenberger, Christian Oehlschlegel, Dagmar Hess, Christoph Mamot, Elisabetta Munzone, Bernhard Pestalozzi, Stefan Aebi, Marcus Vetter, Beat Thuerlimann, Roger von Moos, Khalil Zaman, and Olivia Pagani

Subjects

Cancer Research, Oncology

Abstract

Background: The SAKK 22/99 is a phase III randomized clinical trial launched by the Swiss Group for Clinical Cancer Research and the European Institute of Oncology in Milan in 99 for women with HER2-positive advanced breast cancer (ABC). 175 patients were randomized 1:1 from Sept 99 to Jan 2013 to receive first-line trastuzumab (T) alone followed at disease progression by the combination with chemo (Arm A) vs the upfront combination of T and chemo (Arm B). The results were published in 2017 (O. Pagani et al Ann Onc 28: 305–312, 2017). The outcome was similar for sequential T-chemo or upfront combination The patients’ treatment and FU continued until March 2022 and we now report the safety data after 135.2 months of median FU. Patients and methods: at the time of study termination 1 patient with SD was still receiving T alone in the study and T was continued after trial closure. The safety analyses include 86 pts allocated to arm A and 88 to arm B. 1 pt did not receive any trial treatment and was excluded from this analyses. 19 of the 86 patients in arm A stopped trial treatment after T alone, 67 continued with T+ chemo. Baseline characteristics were well balanced and are summarized in Table 1. Treatment The T loading dose of 4 mg/kg/iv was followed by 2 mg/kg/iv weekly. In the 1st-line population (84) chemo was weekly paclitaxel (90 mg/m2/iv-3/4 weeks). After amendment 1 chemo was at investigator’s choice (taxanes, vinorelbine, platin) according to label indications and could be stopped after 24 weeks (6–8 cycles) in responding patients or after unacceptable toxicity. Results: 7 patients in arm A (8%) and 11 in arm B (13%) stopped trial treatment due to toxicities (Fisher’s exact test, p=0.46). 3 of the 7 patients in arm A stopped under T alone and 4 under T+chemo (all paclitaxel weekly) Treatment durations of these 7 and 11 patients were 7.7 months (range 0.5 – 49) in arm A and 5.5 months (range 0.6 – 31 months) in arm B, respectively. Cardiovascular toxicities: The most common toxicities were thromboembolic events, blood pressure disorders and arrhythmia. 6 patients (7%) in arm A and 10 (11%) in arm B had cardiac events (Fisher’s exact test, p=0.43). G1-3 toxicities occurred in 2 (2%), 2 (2%) and 2 (2%) patients of arm A and in 5 (7%), 2 (2%) and 3 (3%) of arm B. We observed no grade 4 events. Split by treatment phase in arm A, G1-3 toxicities were seen in in 1 (1%), 2 (2%) and 1 (1%) patient under T alone (N=86) and in 1 (1%), 0 (0%) and 2 (3%) under T+chemo (N=67). LVEF-decline: 78 patients in arm A and 74 in arm B had sequential LVEF measurements. A decline ≥ 10% was found in 35 patients (45%) in arm A and in 20 (27%) in arm B (Fisher’s exact test, p=0.028). Among the 35 patients in arm A, 12 had the decline under T alone, 14 under T+chemo, and 9 under both T alone and T+chemo. A decline ≥ 20% was found in 10 patients (13%) in arm A and in 3 (4%) in arm B (Fisher’s exact test, p=0.08). Among the 10 patients in arm A, 7 had the decline under T alone, 3 under T+chemo. Sensory neuropathy 43 patients (50%) in arm A and 48 (54%) in arm B had neuropathy (Fisher’s exact test, p=0.65). G1-3 toxicity in arm A was developed by 26 (30%), 11 (13%) and 6 (7%) patients, respectively; in arm B 30 (34%), 12 (14%) and 6 (7%). No grades 4 events occurred. Conclusion: After more than 11 years of follow-up, no relevant toxicities were found in these patients receiving T for ABC. In particular, the incidence and grade of cardiac toxicity was low. The decline in LVEF was numerically higher in the arm A and in particular in the T alone group, but was not clinically relevant. Our data potentially suggest that T+chemo followed by T maintenance could have less cardiotoxicity than T followed by T+chemo. The possible causes for the difference in LVEF decline between the two arms are unclear, but could be related to treatment duration. The women in Arm A shows a trend to longer therapy: Median treatment duration (months) in Arm A was 7.92 (0.46 - 135.98) vs 6.62 (0.56 - 71.28) in Arm B. This long-term analysis confirms the favorable safety and good tolerability of the reported regimes. Table 2: Treatment duration Citation Format: Manuela Rabaglio, Daniel Dietrich, Bernhard Scheibe, Thomas Ruhstaller, Franco Nole, Serenella Eppenberger, Christian Oehlschlegel, Dagmar Hess, Christoph Mamot, Elisabetta Munzone, Bernhard Pestalozzi, Stefan Aebi, Marcus Vetter, Beat Thuerlimann, Roger von Moos, Khalil Zaman, Olivia Pagani. Safety analysis after 11 years of follow-up of the randomized phase III trial SAKK22/99: upfront chemotherapy in advanced HER2 positive breast cancer [abstract]. In: Proceedings of the 2022 San Antonio Breast Cancer Symposium; 2022 Dec 6-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2023;83(5 Suppl):Abstract nr P4-01-25.

Published

2023

24. Evaluation of multiple transcriptomic gene risk signatures in male breast cancer

Author

Kim Benstead, Carolien H.M. van Deurzen, C. Poncet, Lavinia P. Middleton, Elise van Leeuwen-Stok, Isabel T. Rubio, Joanna Vermeij, Oliver Bogler, Barbro Linderholm, Tammy Piper, Carolien P. Schröder, Larissa A. Korde, Carrie Cunningham, Stéphanie Peeters, Anouk Neven, John W.M. Martens, Ingrid Hedenfalk, M Nowaczyk, Fatima Cardoso, Sharon H. Giordano, Florentine Hilbers, Eric P. Winer, Peggy L. Porter, Christi J. van Asperen, Kathryn J. Ruddy, John M. S. Bartlett, Stefan Aebi, Judith Fraser, Lissandra Dal Lago, Cecilia Nilsson, Danielle Van den Weyngaert, Jane Bayani, Monika Sobol, Catherine M. Kelly, Melissa Murray, Cheryl Crozier, Aleksandra Peric, Institut Català de la Salut, [Bayani J] Ontario Institute for Cancer Research, Toronto, ON, Canada. Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, Canada. [Poncet C, Neven A] Department of Statistics, European Organization for Research and Treatment of Cancer (EORTC) Headquarters, Brussels, Belgium. [Crozier C] Ontario Institute for Cancer Research, Toronto, ON, Canada. [Piper T, Cunningham C] University of Edinburgh, Scotland, UK. [Rubio IT] Unitat de Cirurgia Mamària. Vall d’Hebron Hospital Universitari, Barcelona, Spain, Vall d'Hebron Barcelona Hospital Campus, Medical Oncology, Pathology, and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects

0301 basic medicine, Oncology, EXPRESSION, medicine.medical_specialty, Mama - Càncer - Prognosi, Other subheadings::/methods [Other subheadings], Concordance, Neoplasms::Neoplasms by Site::Breast Neoplasms [DISEASES], Otros calificadores::/diagnóstico [Otros calificadores], Estrogen receptor, Article, Tumour biomarkers, Transcriptome, Prognostic markers, 03 medical and health sciences, 0302 clinical medicine, PROGNOSTIC-FACTORS, SDG 3 - Good Health and Well-being, Otros calificadores::/métodos [Otros calificadores], Internal medicine, medicine, Other subheadings::/diagnosis [Other subheadings], Pharmacology (medical), Radiology, Nuclear Medicine and imaging, BENEFIT, RECURRENCE, skin and connective tissue diseases, Gene, RC254-282, Univariate analysis, neoplasias::neoplasias por localización::neoplasias de la mama [ENFERMEDADES], business.industry, Investigative Techniques::Genetic Techniques::Gene Expression Profiling [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Généralités, Cromosomes humans - Anomalies - Diagnòstic, medicine.disease, BRCA2, Expressió gènica, Subtyping, técnicas de investigación::técnicas genéticas::perfiles de expresión génica [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], 030104 developmental biology, ESTROGEN-RECEPTOR, 030220 oncology & carcinogenesis, Male breast cancer, business, Kappa

Abstract

Male breast cancer (BCa) is a rare disease accounting for less than 1% of all breast cancers and 1% of all cancers in males. The clinical management is largely extrapolated from female BCa. Several multigene assays are increasingly used to guide clinical treatment decisions in female BCa, however, there are limited data on the utility of these tests in male BCa. Here we present the gene expression results of 381 M0, ER+ve, HER2-ve male BCa patients enrolled in the Part 1 (retrospective analysis) of the International Male Breast Cancer Program. Using a custom NanoString™ panel comprised of the genes from the commercial risk tests Prosigna®, OncotypeDX®, and MammaPrint®, risk scores and intrinsic subtyping data were generated to recapitulate the commercial tests as described by us previously. We also examined the prognostic value of other risk scores such as the Genomic Grade Index (GGI), IHC4-mRNA and our prognostic 95-gene signature. In this sample set of male BCa, we demonstrated prognostic utility on univariate analysis. Across all signatures, patients whose samples were identified as low-risk experienced better outcomes than intermediate-risk, with those classed as high risk experiencing the poorest outcomes. As seen with female BCa, the concordance between tests was poor, with C-index values ranging from 40.3% to 78.2% and Kappa values ranging from 0.17 to 0.58. To our knowledge, this is the largest study of male breast cancers assayed to generate risk scores of the current commercial and academic risk tests demonstrating comparable clinical utility to female BCa., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2021

25. Long-term responders to trastuzumab monotherapy in first-line HER-2+ advanced breast cancer: characteristics and survival data

Author

Bernhard C. Pestalozzi, Patrik Weder, Dirk Klingbiel, Stefan Aebi, Sabine Schmid, Christoph Mamot, Franco Nolè, Christoph Rochlitz, Roger von Moos, Elisabetta Munzone, Thomas Ruhstaller, Christian Oehlschlegel, Olivia Pagani, Aron Goldhirsch, Khalil Zaman, Beat Thürlimann, University of Zurich, and Schmid, Sabine

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Multivariate analysis, HER-positive breast cancer, Receptor, ErbB-2, Advanced breast, medicine.medical_treatment, First line, 610 Medicine & health, Breast Neoplasms, lcsh:RC254-282, Disease-Free Survival, 03 medical and health sciences, 0302 clinical medicine, Text mining, Antineoplastic Agents, Immunological, Long-term responders, 1311 Genetics, Surgical oncology, Trastuzumab, Internal medicine, Genetics, Medicine, Humans, 1306 Cancer Research, 030212 general & internal medicine, Trastuzumab monotherapy, Aged, Retrospective Studies, Chemotherapy, business.industry, Cancer, Middle Aged, medicine.disease, Prognosis, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Antineoplastic Agents, Immunological/therapeutic use, Breast Neoplasms/drug therapy, Breast Neoplasms/metabolism, Female, Trastuzumab/therapeutic use, 030220 oncology & carcinogenesis, 10032 Clinic for Oncology and Hematology, 2730 Oncology, business, medicine.drug, Research Article

Abstract

Background The impact of HER2-targeted therapy alone followed by the addition of chemotherapy at disease progression (PD) versus upfront combination was investigated by the SAKK 22/99 trial. The aim of this exploratory analysis of the SAKK 22/99 trial was to characterize the specific subset of patients deriving long-term benefit from trastuzumab monotherapy alone and to identify potential predictive factors of long-term response. Methods This is an unplanned post-hoc analysis of patients randomized to Arm A (trastuzumab monotherapy). Patients were divided in two groups: patients with durable clinical benefit from trastuzumab monotherapy and short-term responders without durable clinical benefit from trastuzumab monotherapy Univariate and multivariate analyses of clinical characteristics correlating with response duration was performed. Results Eighty six patients were randomized in arm A, 24 patients (28%) were long-term responders and 62 (72%) were short-term responders with a 5y-overall survival (OS) of 54% (95% CI 31–72) and of 18% (95%CI 10–30), respectively. Absence of ER expression, absence of PgR expression and presence of visceral disease emerged as possible negative predictive factors for durable clinical benefit. Conclusion Durable clinical benefit can be achieved with trastuzumab monotherapy in a subgroup of HER2-positive patients with advanced disease and it is predictive for longer OS. Further investigations of predictive biomarkers are necessary to better characterize this subgroup of patients and develop further de-escalating strategies. Trial registration NCT00004935; first posted 27.01.2003, retrospectively registered.

Published

2019

26. Pembrolizumab plus trastuzumab in trastuzumab-resistant, advanced, HER2-positive breast cancer (PANACEA): a single-arm, multicentre, phase 1b–2 trial

Author

Barbara Ruepp, Rupert Bartsch, Andrea Gombos, Frances M. Boyle, Giuseppe Viale, Anita Hiltbrunner, Thomas Bachelot, Martine Piccart-Gebhart, Caitlin Mahoney, Debora Fumagalli, Rina Hui, Theodora Goulioti, Fabrice Andre, Marco Colleoni, Carmen Comune, Magdelena Weber, Michelle Jenkins, Stefan Aebi, Stefania Andrighetto, Stamatina Fournarakou, Meredith M. Regan, Colleen King, Angelo Di Leo, Alan S. Coates, Rita Hui, Aron Goldhirsch, Mario Campone, Per Karlsson, Rolf A. Stahel, Vassiliki Karantza, Hui Huang, Laura Biganzoli, Hervé Bonnefoi, Sabrina Ribeli-Hofmann, Roswitha Kammler, Magdalena Sánchez-Hohl, Karolyn Scott, Patrick Schneier, Giuseppe Curigliano, Ingrid Kössler, Sherene Loi, Heather Findlay, Richard D. Gelber, Holly Shaw, Guy Jerusalem, Susan Fischer, Anita Giobbie-Hurder, Daniela Celotto, Manuela Rabaglio-Poretti, Rita Pfister, Michela Frapolli, Monica Greco, Adriana Gasca, Mark J. Smyth, Jaime A. Mejia, Karen N. Price, Heidi Roschitzki, and Rudolf Maibach

Subjects

Adult, 0301 basic medicine, Oncology, medicine.medical_specialty, Adolescent, Receptor, ErbB-2, Programmed Cell Death 1 Receptor, Population, Phases of clinical research, Breast Neoplasms, Pembrolizumab, Antibodies, Monoclonal, Humanized, B7-H1 Antigen, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Trastuzumab, Internal medicine, Clinical endpoint, Humans, Medicine, education, Adverse effect, Aged, education.field_of_study, Dose-Response Relationship, Drug, business.industry, Respiratory infection, Middle Aged, medicine.disease, Treatment Outcome, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Female, business, medicine.drug

Abstract

Summary Background HER2-positive breast cancers usually contain large amounts of T-cell infiltrate. We hypothesised that trastuzumab resistance in HER2-positive breast cancer could be mediated by immune mechanisms. We assessed the safety and anti-tumour activity of pembrolizumab, a programmed cell death protein 1 (PD-1) inhibitor, added to trastuzumab in trastuzumab-resistant, advanced HER2-positive breast cancer. Methods We did this single-arm, multicentre, phase 1b–2 trial in 11 centres based in five countries. Eligible participants were women aged 18 years or older, who had advanced, histologically confirmed, HER2-positive breast cancer; documented progression during previous trastuzumab-based therapy; an Eastern Cooperative Oncology Group performance status of 0 or 1; and a formalin-fixed, paraffin-embedded metastatic tumour biopsy for central assessment of programmed cell death 1 ligand 1 (PD-L1) status. In phase 1b, we enrolled patients with PD-L1-positive tumours in a 3 + 3 dose-escalation of intravenous pembrolizumab (2 mg/kg and 10 mg/kg, every 3 weeks) plus 6 mg/kg of intravenous trastuzumab. The primary endpoint of the phase 1b study was the incidence of dose-limiting toxicity and recommended phase 2 dose; however, a protocol amendment on Aug 28, 2015, stipulated a flat dose of pembrolizumab of 200 mg every 3 weeks in all Merck-sponsored trials. In phase 2, patients with PD-L1-positive and PD-L1-negative tumours were enrolled in parallel cohorts and received the flat dose of pembrolizumab plus standard trastuzumab. The primary endpoint of the phase 2 study was the proportion of PD-L1-positive patients achieving an objective response. This trial is registered in ClinicalTrials.gov, number NCT02129556, and with EudraCT, number 2013-004770-10, and is closed. Findings Between Feb 2, 2015, and April 5, 2017, six patients were enrolled in phase 1b (n=3 received 2 mg/kg pembrolizumab, n=3 received 10 mg/kg pembrolizumab) and 52 patients in phase 2 (n=40 had PD-L1-positive tumours, n=12 had PD-L1-negative tumours). The data cutoff for this analysis was Aug 7, 2017. During phase 1b, there were no dose-limiting toxicities in the dose cohorts tested. Median follow-up for the phase 2 cohort was 13·6 months (IQR 11·6–18·4) for patients with PD-L1-positive tumours, and 12·2 months (7·9–12·2) for patients with PD-L1-negative tumours. Six (15%, 90% CI 7–29) of 40 PD-L1-positive patients achieved an objective response. There were no objective responders among the PD-L1-negative patients. The most common treatment-related adverse event of any grade was fatigue (12 [21%] of 58 patients). Grade 3–5 adverse events occurred in 29 (50%) of patients, treatment-related grade 3–5 adverse events occurred in 17 (29%), and serious adverse events occurred in 29 (50%) patients. The most commonly occurring serious adverse events were dyspnoea (n=3 [5%]), pneumonitis (n=3 [5%]), pericardial effusion (n=2 [3%]), and upper respiratory infection (n=2 [3%]). There was one treatment-related death due to Lambert-Eaton syndrome in a PD-L1-negative patient during phase 2. Interpretation Pembrolizumab plus trastuzumab was safe and showed activity and durable clinical benefit in patients with PD-L1-positive, trastuzumab-resistant, advanced, HER2-positive breast cancer. Further studies in this breast cancer subtype should focus on a PD-L1-positive population and be done in less heavily pretreated patients. Funding Merck, International Breast Cancer Study Group.

Published

2019

27. Abstract P6-19-01: Evaluation of multiple transcriptomic gene risk signatures in male breast cancer

Author

Jwm Martens, Oliver Bogler, Stéphanie Peeters, C. P. Schroder, EP Winer, Isabel T. Rubio, Barbro Linderholm, Larissa A. Korde, Judith Fraser, C.H.M. van Deurzen, Aleksandra Peric, Ingrid Hedenfalk, C. Poncet, Lavinia P. Middleton, Fatima Cardoso, Carrie Cunningham, Catherine M. Kelly, Joanna Vermeij, Peggy L. Porter, Melissa Murray, Sharon H. Giordano, L. Dal Lago, Cecilia Nilsson, M Nowaczyk, CQ Yao, Monika Sobol, Stefan Aebi, E van Leeuwen-Stok, D van den Weyngaert, T Piper, Jms Bartlett, Kathryn J. Ruddy, Kim Benstead, FH Hilbers, Jane Bayani, C. J. van Asperen, N Anouk, Paul C. Boutros, and Cheryl Crozier

Subjects

Oncology, Transcriptome, Cancer Research, medicine.medical_specialty, Internal medicine, Male breast cancer, medicine, Biology, medicine.disease, Gene

Abstract

Introduction: Male breast cancer (MBC) is a rare disease accounting for less than 1% of all breast cancers (BC) and 1% of all cancers in males. The clinical management is largely extrapolated from female BC. Several multigene assays are increasingly used to guide clinical treatment decisions in female BC, however there is little data on the utility of these tests in MBC. Methods: Here we present the gene expression results of 380 M0, ER+ve, HER2-ve MBCs enrolled in the Part 1 (retrospective joint analysis) International Male Breast Cancer Program of 1483 patients diagnosed between 1990-2010 (Cardoso et al. Annals of Oncology, 2018). Using a custom Nanostring™ panel comprised of the genes from the commercial risk tests Prosigna®, OncotypeDx® and Mammaprint®, risk scores and intrinsic subtyping data were generated to recapitulate the commercial tests as described by Bayani and Yao et al (npjBreast Cancer, 2017). Survival outcomes by risk classification were analyzed using Cox models with time-dependent covariates when the proportional hazard assumption was not met and adjusted for clinical and treatment variables. Results: Prosigna-like risk scores identified 99 (26.1%) as low-risk, 159 (41.8%) as intermediate-risk, and 122 (32.1%) as high-risk. Using the TAILORx cut-off (25) for OncotypeDx-like risk of recurrence scoring, 158 (41.6%) were identified as low-risk, while 222 (58.4%) were identified as high-risk. MammaPrint-like results identified 175 (46.1%) as low-risk and 205 (53.9%) as high-risk. Overall, patients classified as high-risk had higher grade, more nodal involvement, larger tumors, and more frequently treated with chemotherapy than low-risk patients. Survival analyses demonstrated clear clinical utility for each test, showing patients at high-risk with poor relapse-free survival (RFS) as compared to patients classified as low-risk: Prosigna-like RFS at 3-years (HR=2.20, 95% CI, 1.28-3.80); Oncotype-like RFS at 3-years (HR=1.92, 95% CI, 1.17-3.17); MammaPrint-like RFS (HR=1.51, 95% CI, 1.00-2.27); with similar findings for distant relapse-free survival (DRFS) and overall survival (OS). Across outcomes and all gene signatures, patients with concordant Low/Low risk classification had better prognosis than those with concordant High/High risk classification. PAM50 intrinsic subtyping identified 147 (38.7%) as Luminal A, 57 (15.0%) as Luminal B, 80 (21.1%) as Her2-enriched and 96 (25.3%) as Basal-like; showing overall 34.5% concordance to clinic-pathological subtyping by central pathology (95% CI, 29.7%-39.5%). Comparison between the tests in the MBC cohort and a comparable cohort of female BC from the Tamoxifen Exemestane Adjuvant Multinational (TEAM) trial processed in the same way will be presented. Conclusion: Common transcriptomic assays designed to assess residual risk, validated in female BC, provide similar information in male BC patients. Not surprisingly, disagreement between test results at the individual patient level was observed. To our knowledge, this is the largest study of MBC assayed to generate risk scores of the current commercial BC tests to demonstrate their clinical utility and their differences and similarity to female BC. This work has been funded by the Breast Cancer Research Foundation (BCRF). Citation Format: Bayani J, Poncet C, Yao CQ, Crozier C, Anouk N, Piper T, Cunningham C, Sobol M, Aebi S, Benstead K, Bogler O, Dal Lago L, Fraser J, Hilbers FH, Hedenfalk I, Korde L, Linderholm B, Martens J, Middleton L, Murray M, Kelly C, Nilsson C, Nowaczyk M, Peeters S, Peric A, Porter P, Schröder C, Rubio IT, Ruddy KJ, van Asperen C, Van Den Weyngaert D, van Deurzen C, van Leeuwen-Stok E, Vermeij J, Winer E, Boutros PC, Giordano SH, Cardoso F, Bartlett JM. Evaluation of multiple transcriptomic gene risk signatures in male breast cancer [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr P6-19-01.

Published

2019

28. P-227: Alternate day dosing of pomalidomide in patients with refractory/relapsed multiple myeloma (RRMM): Results of a multicenter, single arm phase 2 trial (SAKK 39/16 OptiPOM Study)

Author

Christoph Renner, Ulrich Mey, Christoph Driessen, Jeroen S. Goede, Thomas Pabst, Stefanie Hayoz, Thilo Zander, Erika Lerch, Tobias Pabst, Axel Rüfer, Sämi Schär, Gaëlle Rhyner, Urban Novak, Stefan Aebi, and Zuzanna Maniecka

Subjects

Cancer Research, medicine.medical_specialty, Bortezomib, business.industry, Phases of clinical research, Hematology, Neutropenia, medicine.disease, Pomalidomide, Carfilzomib, Gastroenterology, chemistry.chemical_compound, Oncology, chemistry, Internal medicine, medicine, Dosing, Progression-free survival, 610 Medicine & health, business, medicine.drug, Lenalidomide

Abstract

Background Pomalidomide (POM) with dexamethasone (DEX) is approved in patients (pts) with relapsed and refractory (RRMM) myeloma and achieved a progression free survival (PFS) between 4.0 and 4.6 months in two pivotal phase III trials (MM-003 and MM-010). In addition, POM-DEX is a current standard backbone for triplet combinations in RRMM. However, POM-DEX with registered POM dosing (4mg daily, 21/28 day cycle) has significant toxicity with G3/4 neutropenia (48%), anemia (33%), infections (34%) and thrombocytopenia (22%) in MM-003, and up to 85% G3/4 neutropenia in triplets containing CD38 antibodies. The relationship between dose, efficacy and toxicity of POM is poorly established and POM delivered on a 2mg daily continuous schedule was similarly active compared to the standard schedule, but less toxic. Half life time of POM (7.5h) is significantly longer compared to lenalidomide (3h) with a slow decline of the POM plasma concentration at the terminal phase. Alternate day dosing of POM 4mg may therefore maintain efficacy while mitigating toxicity. This multicenter, open label, non-randomized phase II study investigated the activity and toxicity of POM 4mg given continuously every second day in RRMM pts. Methods Inclusion criteria matched MM-003. Pts with RRMM must have had ≥ 2 prior lines including bortezomib (BORT), lenalidomide (LEN), adequate alkylator treatment, and progressive myeloma on or within 60 days of the last MM treatment. Continuous oral POM 4mg on alternate days 1 to 28 was combined with weekly oral DEX 40mg (pts > 75 years 20mg) until intolerance or progression (PD). Pts received prophylaxis with acyclovir/valacyclovir, cotrimoxazole and ASS. Prophylactic G-CSF was not allowed. Primary endpoint was overall response rate (ORR, minimal response (MR) or better by IMWG criteria). Secondary objectives were overall survival (OS), 12 months OS, PFS and adverse events (AE). Results 34 patients were enrolled (median age 75 yrs, range 52-87) with time from diagnosis of 5.1 yrs (range 1.9-16.8). Prior treatments included LEN (100%), BORT (100%), alkylator (100%), carfilzomib (29%) and daratumumab (27%); 14 (41%) pts had high-risk cytogenetic features. Median treatment duration was 3.6 months. G3/4 AE occurred in less than one quarter of patients: (neutropenia 24%; anemia 18%; infections 18%; thrombocytopenia 12%). Neutropenic fever was not observed. ORR was 29 % (95% confidence interval [CI], 16%-50%; 3 (9%) VGPRs, 6 (8%) PRs and 1 (3%) MR; 15 pts (44%) achieved SD. 9 pts (26%) progressed. Median PFS was 4.2 months (95% CI, 1.9-5.5 months). OS at 12 months was 66.5% (95% CI, 47.6-79.9). Conclusion POM 4mg on an alternate day continuous dosing schedule is an active and well-tolerated option to deliver POM-DEX to RRMM pts and is especially reasonable for patients at increased risk of toxicity. This dosing schedule may have comparable efficacy, improved safety and should be explored in triplet combination.

Published

2021

29. Population-level effect of molecular testing and targeted therapy in patients with advanced pulmonary adenocarcinoma: a prospective cohort study

Author

Oliver Gautschi, Joachim Diebold, David Pfeiffer, Christine Schwegler, Stefan Aebi, and Dinu Kaufmann

Subjects

Adult, Male, Oncology, medicine.medical_specialty, Lung Neoplasms, medicine.medical_treatment, Adenocarcinoma of Lung, Antineoplastic Agents, Kaplan-Meier Estimate, Adenocarcinoma, medicine.disease_cause, Proto-Oncogene Mas, Pathology and Forensic Medicine, Targeted therapy, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Anaplastic lymphoma kinase, Molecular Targeted Therapy, Prospective Studies, 030212 general & internal medicine, Epidermal growth factor receptor, Prospective cohort study, Molecular Biology, Aged, Proportional Hazards Models, Aged, 80 and over, biology, business.industry, Cancer, Cell Biology, General Medicine, Middle Aged, medicine.disease, Cancer registry, Clinical trial, Treatment Outcome, 030220 oncology & carcinogenesis, biology.protein, Female, KRAS, business, Switzerland

Abstract

Large cancer centres in the USA demonstrated that molecular diagnosis and targeted therapy improved overall survival of patients with advanced pulmonary adenocarcinoma. We validated this finding in a rural area of Switzerland, served by private practices, community hospitals and a tertiary referral centre. We conducted a prospective cohort study with the Cancer Registry of Central Switzerland, covering 4 cantons and 517,000 inhabitants. All residents newly diagnosed with stage IV pulmonary adenocarcinoma from 2010 to 2014 were enrolled. We obtained information on patients, tumour, molecular testing, therapy and survival. Three hundred forty-eight patients were included in the study. Molecular testing was performed in 279 (80%); 132 (38%) had oncogenic driver mutations: Kirsten rat sarcoma (KRAS, 16%), epidermal growth factor receptor (EGFR, 11%), anaplastic lymphoma kinase (ALK, 5%), human epidermal growth factor receptor 2 (HER2, 2%), B rapidly accelerated fibrosarcoma (BRAF, 1%), rearranged during transfection (RET, 0.5%), MET proto-oncogene (0.5%) and multiple mutations (2%). Fifty-six patients with an oncogenic driver mutation, mostly epidermal growth factor receptor (34) and anaplastic lymphoma kinase (12), received genotype-matched targeted therapy, at least 25 (45%) of whom in a clinical trial or named patient programme. Median overall survival was 18 months for patients with driver mutations and targeted therapy, 8 months for patients with driver mutations and conventional therapy and 10 months for patients with no driver mutation and conventional therapy. For patients with driver mutations and targeted therapy, overall survival was significantly better than that for patients with driver mutations and conventional therapy (HR 0.64, p = 0.04). Rigorous testing combined with optimal access to targeted therapy in clinical trials improved the prognosis of patients with advanced pulmonary adenocarcinoma in Central Switzerland. This effect was mainly driven by therapies targeting epidermal growth factor receptor and anaplastic lymphoma kinase.

Published

2017

30. Principles of Systemic Therapy

Author

Martin F. Fey and Stefan Aebi

Subjects

Oncology, medicine.medical_specialty, Chemotherapy, business.industry, medicine.drug_class, medicine.medical_treatment, Cancer drugs, Monoclonal antibody, Systemic therapy, Internal medicine, Adjuvant therapy, Medicine, business, Neoadjuvant therapy

Published

2017

31. Characterization of molecular scores and gene expression signatures in primary breast cancer, local recurrences and brain metastases

Author

Andreas R. Günthert, Rolf Jaggi, Mariana Bustamante Eduardo, Hans Jörg Altermatt, Nadja Ballabio, Sara Imboden, Stefan Aebi, and Vlad Popovici

Subjects

0301 basic medicine, Oncology, Cancer Research, Luma, Hierarchical clustering, Basal (phylogenetics), 0302 clinical medicine, Breast cancer, Surgical oncology, Gene expression, Local recurrence, Gene expression measurement, PAM50 subtypes, Molecular risk scores, Aged, 80 and over, medicine.diagnostic_test, Brain Neoplasms, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Prognosis, Immunohistochemistry, 3. Good health, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, Female, Oncotype DX, Research Article, Adult, medicine.medical_specialty, RNA isolation and processing, 610 Medicine & health, Breast Neoplasms, lcsh:RC254-282, 03 medical and health sciences, Internal medicine, Genetics, medicine, Biomarkers, Tumor, Humans, Aged, business.industry, Brain metastasis, Gene Expression Profiling, Computational Biology, medicine.disease, 030104 developmental biology, Neoplasm Grading, Neoplasm Recurrence, Local, business, Transcriptome, Follow-Up Studies

Abstract

Background Breast cancer is a leading cause of cancer-related death in women worldwide. Despite extensive studies in all areas of basic, clinical and applied research, accurate prognosis remains elusive, thus leading to overtreatment of many patients. Diagnosis could be improved by introducing multigene molecular scores in standard clinical practice. Several tests that work with formalin-fixed tissue have become routine. Molecular scores usually include several genes representing processes, response to oestrogens, progestogens and human epidermal growth factor receptor 2 (Her2), respectively, which are combined additively in single values. These multi-gene scores have the advantage of being more robust and reproducible than single-gene scores. Their utility may be further enhanced by combining them with classical diagnostic parameters. Here, we present an exploratory study comparing the RISK and research versions of Oncotype DX recurrence score (RS), Prosigna Risk of Recurrence (ROR) and EndoPredict (EP) with respect to their prognostic potential for ipsilateral recurrence and/or distant relapse in brain, and we compared the scores to the intrinsic subtypes based on PAM50. Methods RNA was extracted from formalin-fixed, paraffin-embedded (FFPE) tissue cores of primary tumours, local recurrences and brain metastases. Gene expression was measured on a NanoString nCounter Analysis System. Intrinsic subtypes and molecular scores were computed according to published literature and RISK, RS, ROR and EP were compared against each other and to the intrinsic subtypes Luminal A (lumA), Luminal B (lumB), Her2-enriched (Her2↑), Basal-like (basal), and Normal-like (normal) of PAM50. Local recurrences and brain metastases were compared to their corresponding primary tumours. Results All four molecular scores were highly correlated. Highest correlations were observed among genes related to proliferation while lower correlations were found among oestrogen-related genes. The scores were significantly higher in primary tumours progressing to brain metastases as compared to recurrence-free primary tumours and primary tumours that relapsed as local recurrences. Conclusions RISK and ROR-P are prognostic for primary tumours metastasizing to the brain. All four scores, RISK, RS, EP and ROR-P failed to discriminate between primary tumours that remained recurrence-free and primary tumours relapsing as local recurrences. Electronic supplementary material The online version of this article (10.1186/s12885-019-5752-8) contains supplementary material, which is available to authorized users.

Published

2019

32. Effets indésirables des immunothérapies oncologiques

Author

Oliver Gautschi, Justus E. Roos, Richard Kobza, Stefan Aebi, Bernhard Schwizer, C. U. Brand, Lukas Schmid, Michael Christ, Urs Odermatt, Joachim Diebold, Michael Gregor, Dominique Criblez, Einar Wilder-Smith, and Stefan Fischli

Abstract

Depuis nos recommandations publiees au FMS en 2016, de nouvelles connaissances, qui sont non seulement pertinentes pour les oncologues mais egalement pour les medecins de premier recours, sont disponibles.

Published

2019

33. Nebenwirkungen von onkologischen Immuntherapien

Author

Michael Christ, Justus E. Roos, Dominique Criblez, Stefan Fischli, Lukas Schmid, Urs Odermatt, Oliver Gautschi, Richard Kobza, Stefan Aebi, Joachim Diebold, Michael Gregor, Bernhard Schwizer, C. U. Brand, and Einar Wilder-Smith

Abstract

2016 stellten wir im SMF Empfehlungen zum Management der haufigsten Nebenwirkungen von Immuntherapien vor. Inzwischen gibt es neue Erkenntnisse, die nicht nur fur Onkologen, sondern auch fur Grundversorger relevant sind.

Published

2019

34. Abstract OT-26-02: Phase III open-label, multicenter, randomized trial of adjuvant palbociclib in combination with endocrine therapy versus endocrine therapy alone for patients with hormone receptor-positive / HER2-negative resected isolated locoregional recurrence of breast cancer - The POLAR Trial

Author

Noelia Martínez Jañez, Marija Balic, Uwe Güth, Heidi Roschitzki-Voser, Barbara Pistilli, Meritxell Bellet, Elisabetta Munzone, Stefan Aebi, and Meredith M. Regan

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, medicine.medical_treatment, HER2 negative, Endocrine therapy, Palbociclib, medicine.disease, law.invention, Breast cancer, Randomized controlled trial, Hormone receptor, law, Internal medicine, medicine, Open label, business, Adjuvant

Abstract

Background: Isolated local or regional recurrence (ILRR) of breast cancer (BC) after mastectomy or lumpectomy indicates a poor prognosis and patients with ILRR hold a substantial risk of developing subsequent distant metastasis. Limited randomized evidence supports the recommendation of systemic treatment for hormone receptor-positive (HR+) lLRR. Cyclin-dependent kinases 4 and 6 (CDK4/6) inhibitors, such as palbociclib, have shown activity and safety in the first-line treatment of metastatic HR+/HER2-negative BC. The POLAR hypothesis is based on the results of the CALOR trial (IBCSG Trial 27-02), which showed effectiveness of adjuvant chemotherapy among patients with resected HR-negative ILRR, but not for HR+ ILRR. Considering these findings and compelling evidence supporting the activity of the combination of CDK4/6 inhibitors and endocrine therapy (ET), we hypothesize that palbociclib in combination with ET may be effective as adjuvant therapy in patients with HR+/HER2-negative resected ILRR of BC. Trial design: POLAR is a phase III open-label, multicenter, randomized trial of adjuvant palbociclib in combination with standard ET versus standard ET alone for women and men with histologically confirmed HR+/HER2-negative resected ILRR of BC. Protocol treatment consists of palbociclib (125 mg/d orally for 21 days, followed by 7 days rest) for 3 years plus standard ET for at least 3 years (Arm A) or standard ET for at least 3 years (Arm B). Patients must be enrolled within 6 months of complete gross excision of the ILRR. Patients may have started standard ET prior to entry. Randomization (1:1) is stratified according to (1) gender and menopausal status; (2) planned ET (oral aromatase inhibitor or tamoxifen vs. fulvestrant). The primary endpoint, invasive disease-free survival (iDFS), will be compared between treatment groups using a stratified log-rank test. The sample size provides 80% power to detect a 50% reduction in hazard (HR=0.50) for palbociclib plus ET versus ET-alone, using a log-rank test with two-sided α=0.05 test with 66 iDFS events. The 3-year iDFS is assumed to be 76% on the basis of patients in the CALOR trial who had ER+ ILRRs. Accrual: The trial will recruit 400 patients from approximately 50 Centers in Austria, France, Hungary, Italy, Spain and Switzerland. The first patient was randomized in August 2019. Accrual as of mid-June 2020 was 25 patients. The POLAR trial (IBCSG 59-19 / BIG 18-02) is sponsored and coordinated by IBCSG with financial support from Pfizer. The trial is conducted under the BIG umbrella in collaboration with ABCSG, GEICAM, SOLTI, SAKK and Unicancer. NCT03820830 Citation Format: Elisabetta Munzone, Stefan Aebi, Noelia Martínez Jañez, Uwe Güth, Meritxell Bellet, Barbara Pistilli, Marija Balic, Heidi Roschitzki-Voser, Meredith M Regan. Phase III open-label, multicenter, randomized trial of adjuvant palbociclib in combination with endocrine therapy versus endocrine therapy alone for patients with hormone receptor-positive / HER2-negative resected isolated locoregional recurrence of breast cancer - The POLAR Trial [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr OT-26-02.

Published

2021

35. Intravascular large B‑cell lymphoma

Author

Manfred Kessler, Elisabeth J. Rushing, Daniela Weiler, Jeanne Godau, Karl Frontzek, Silvia Hofer, and Stefan Aebi

Subjects

Pathology, medicine.medical_specialty, Chemotherapy, Intravascular large B-cell lymphoma, business.industry, medicine.medical_treatment, Myelitis, Hematology, Disease, medicine.disease, Lymphoma, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, Oncology, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, Aphasia, medicine, Dementia, Radiology, medicine.symptom, business, Stroke

Abstract

Intravascular lymphoma (IVL), a rare, extranodal form of non-Hodgkin lymphoma (NHL), can cause infarcts by occluding small arteries of the brain. Owing to its heterogeneous clinical manifestations and unfavorable prognosis, the diagnosis is often made postmortem. Patients can present with a range of motor or sensory deficits, rapid cognitive impairment, aphasia or signs of myelitis, often with nonspecific radiographic findings.Timely recognition of a treatable disease is essential to prevent permanent neurocognitive defects. We present a case who could be treated successfully with chemotherapy.

Published

2016

36. The impact of ABCC11 polymorphisms on the risk of early-onset fluoropyrimidine toxicity

Author

N Wenger, Carlo R. Largiadèr, Tanja K. Froehlich, Stefan Aebi, Ursula Amstutz, Markus Joerger, and Seid Hamzic

Subjects

Adult, Male, Risk, 0301 basic medicine, Antimetabolites, Antineoplastic, medicine.medical_specialty, Adolescent, Pharmacology, Polymorphism, Single Nucleotide, Gastroenterology, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Leukocytes, Genetics, medicine, Dihydropyrimidine dehydrogenase, Humans, ABCC11, Aged, Aged, 80 and over, Leukopenia, biology, Cancer, Odds ratio, Middle Aged, medicine.disease, Pyrimidines, 030104 developmental biology, Fluorouracil, 030220 oncology & carcinogenesis, Toxicity, biology.protein, Molecular Medicine, ATP-Binding Cassette Transporters, Female, DPYD, medicine.symptom, medicine.drug

Abstract

A missense variant (c.1637C>T, T546M) in ABCC11 encoding the MRP8 (multidrug resistance protein 8), a transporter of 5-fluorodeoxyuridine monophosphate, has been associated with an increased risk of 5-fluorouracil-related severe leukopenia. To validate this association, we investigated the impact of the ABCC11 variants c.1637C>T, c.538G>A and c.395+1087C>T on the risk of early-onset fluoropyrimidine-related toxicity in 514 cancer patients. The ABCC11 variant c.1637C>T was strongly associated with severe leukopenia in patients carrying risk variants in DPYD, encoding the key fluoropyrimidine-metabolizing enzyme dihydropyrimidine dehydrogenase (odds ratio (OR): 71.0; 95% confidence interval (CI): 2.5-2004.8; Pc.1637C>T*DPYD=0.013). In contrast, in patients without DPYD risk variants, no association with leukopenia (OR: 0.95; 95% CI: 0.34-2.6) or overall fluoropyrimidine-related toxicity (OR: 1.02; 95% CI: 0.5-2.1) was observed. Our study thus suggests that c.1637C>T affects fluoropyrimidine toxicity to leukocytes particularly in patients with high drug exposure, for example, because of reduced fluoropyrimidine catabolism.

Published

2016

37. Männliches Mammakarzinom: Was ist anders?

Author

Philipp Niederberger, Susanne Bucher, and Stefan Aebi

Subjects

Oncology, medicine.medical_specialty, medicine.diagnostic_test, business.industry, medicine.medical_treatment, Estrogen receptor, General Medicine, medicine.disease, Metastatic breast cancer, Radiation therapy, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, 030220 oncology & carcinogenesis, Internal medicine, Male breast cancer, medicine, Adjuvant therapy, Mammography, 030212 general & internal medicine, business, Tamoxifen, medicine.drug

Abstract

Zusammenfassung. Brustkrebs ist beim Mann eine seltene Krankheit. Die Symptome sind ähnlich wie bei der Frau: Bei palpablem Tumor in der Brust, vergrösserten axillären Lymphknoten oder verdächtigen Hautveränderungen der Brust (Ulzeration, Sekretion, peau d'orange) empfehlen sich Mammografie, Mammasonografie mit Beurteilung der regionären Lymphknoten und präoperativer histologischer Bestätigung. Die Therapie des männlichen Mammakarzinoms erfolgt wie bei der Frau: Resektion gefolgt von Pharmakotherapie und Bestrahlung. Anders als bei Frauen kommt in der adjuvanten Therapie Tamoxifen und nicht ein Aromatasehemmer zum Einsatz. Die Behandlungsprinzipien in der metastasierten Situation gleichen dem Vorgehen bei Frauen.

Published

2016

38. Spotlight on pomalidomide: could less be more?

Author

Christoph Renner, Stefan Aebi, Christoph Driessen, Thomas Pabst, and Thilo Zander

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, 610 Medicine & health, Dexamethasone, Drug Administration Schedule, Drug Costs, 03 medical and health sciences, 0302 clinical medicine, Text mining, Adjuvants, Immunologic, Internal medicine, Humans, Medicine, Letter to the Editor, Survival analysis, Multiple myeloma, business.industry, Hematology, Pomalidomide, medicine.disease, Survival Analysis, Thalidomide, 030104 developmental biology, 030220 oncology & carcinogenesis, Immunology, Costs and Cost Analysis, Multiple Myeloma, business, medicine.drug

Published

2017

39. Evaluating the role of ENOSF1 and TYMS variants as predictors in fluoropyrimidine-related toxicities: An IPD meta-analysis

Author

Markus Joerger, Tanja K. Froehlich, Jan H.M. Schellens, Didier Meulendijks, Seid Hamzic, Carlo R. Largiadèr, Claire Palles, Xandra García-González, Luis A. López-Fernández, Ursula Amstutz, Stefan Aebi, Ian Thomlinson, and Dominic Kummer

Subjects

0301 basic medicine, Oncology, Antimetabolites, Antineoplastic, medicine.medical_specialty, Multivariate statistics, 610 Medicine & health, Capecitabine, 03 medical and health sciences, 0302 clinical medicine, Polymorphism (computer science), Neoplasms, Internal medicine, medicine, Humans, SNP, Allele, Hydro-Lyases, Pharmacology, business.industry, Haplotype, Cancer, Thymidylate Synthase, medicine.disease, 030104 developmental biology, Fluorouracil, 030220 oncology & carcinogenesis, Hand-Foot Syndrome, business, medicine.drug

Abstract

To assess the proposed associations of the c.742-227G>A (rs2612091) polymorphism within the Enolase Superfamily Member 1 gene (ENOSF1) and two variants in the adjacent Thymidylate Synthase gene (TYMS): the 5'VNTR 28bp-repeat (rs45445694) and 3'UTR 6bp-indel (rs11280056) with severe toxicity in fluoropyrimidine-treated cancer patients, we performed an individual patient data meta-analysis. Only studies investigating all three-abovementioned variants with fluoropyrimidine-related toxicities were considered for meta-analysis. Associations were tested individually for each study using multivariate regression. Meta-analysis was performed using a random-effects model. One-stage multivariate regressions including tests for independent SNP effects were applied to investigate individual effects of the variants. Multivariate haplotype regression analyses were performed on a pooled dataset to test multi-SNP effects. Of four studies including 2'067 patients, 1'912 were eligible for meta-analysis. All variants were exclusively associated with severe hand-foot-syndrome (HFS) (TYMS 2R: OR = 1.50, p = 0.0002; TYMS 6bp-ins: OR = 1.42 p = 0.0036; ENOSF1 c.742-227G: OR = 1.64 p A and the TYMS 28bp-repeat: each toxicity-associated allele increased the risk for severe HFS (OR = 1.32 per allele, p

Published

2020

40. Correction: Quality of life under extended continuous versus intermittent adjuvant letrozole in lymph node-positive, early breast cancer patients: the SOLE randomised phase 3 trial

Author

Jürg Bernhard, Vincenzo Di Lauro, Karin Ribi, Weixiu Luo, Patrick Neven, Prudence A. Francis, Aron Goldhirsch, Annelore Barbeaux, Thomas Ruhstaller, Stefan Aebi, Meredith M. Regan, Bettina Müller, Claudio Graiff, Per Karlsson, Olivia Pagani, Angelo Di Leo, Alan S. Coates, Theodoros Foukakis, Richard D. Gelber, Manuela Rabaglio, Marco Colleoni, Marie-Pascale Graas, Jacquie Chirgwin, Daniel A. Vorobiof, Laura Biganzoli, Rudolf Maibach, E Abdi, Henry L. Gomez, and Guy Jerusalem

Subjects

Cancer Research, medicine.medical_specialty, Sleep disorder, business.industry, Letrozole, Repeated measures design, medicine.disease, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Mood, Oncology, Breast Cancer Prevention Trial, Quality of life, 030220 oncology & carcinogenesis, Internal medicine, medicine, 610 Medicine & health, business, medicine.drug

Abstract

In the phase III SOLE trial, the extended use of intermittent versus continuous letrozole for 5 years did not improve disease-free survival in postmenopausal women with hormone receptor-positive breast cancer. Intermittent therapy with 3-month breaks may be beneficial for patients’ quality of life (QoL). In the SOLE QoL sub-study, 956 patients completed the Breast Cancer Prevention Trial (BCPT) symptom and further QoL scales up to 24 months after randomisation. Differences in change of QoL from baseline between the two administration schedules were tested at 12 and 24 months using repeated measures mixed-models. The primary outcome was change in hot flushes at 12 months. There was no difference in hot flushes at 12 months between the two schedules, but patients receiving intermittent letrozole reported significantly more improvement at 24 months. They also indicated less worsening in vaginal problems, musculoskeletal pain, sleep disturbance, physical well-being and mood at 12 months. Overall, 25–30% of patients reported a clinically relevant worsening in key symptoms and global QoL. Less symptom worsening was observed during the first year of extended treatment with the intermittent administration. For women experiencing an increased symptom burden of extended adjuvant endocrine therapy, an intermittent administration is a safe alternative. Clinical trial information: NCT00553410.

Published

2020

41. Quality of life under extended continuous versus intermittent adjuvant letrozole in lymph node-positive, early breast cancer patients: the SOLE randomised phase 3 trial

Author

Manuela Rabaglio, R. D. Gelber, Henry L. Gomez, Annelore Barbeaux, A. Goldhirsch, Daniel A. Vorobiof, V. Di Lauro, Thomas Ruhstaller, Claudio Graiff, Prudence A. Francis, A. S. Coates, Karin Ribi, Bettina Müller, Patrick Neven, Stefan Aebi, Theodoros Foukakis, Per Karlsson, Rudolf Maibach, M.A. Colleoni, O. Pagani, Meredith M. Regan, Laura Biganzoli, G. Jerusalem, Jacquie Chirgwin, Juerg Bernhard, E Abdi, Weixiu Luo, A. Di Leo, and Marie-Pascale Graas

Subjects

Oncology, Adult, Cancer Research, medicine.medical_specialty, Drug-Related Side Effects and Adverse Reactions, Phases of clinical research, Breast Neoplasms, Article, Disease-Free Survival, Drug Administration Schedule, law.invention, Breast cancer, Quality of life, Randomized controlled trial, law, Internal medicine, Human behaviour, medicine, Adjuvant therapy, Humans, 610 Medicine & health, Lymph node, Aged, Neoplasm Staging, business.industry, Letrozole, Cancer, Correction, Middle Aged, medicine.disease, SOLE Investigators, medicine.anatomical_structure, Chemotherapy, Adjuvant, Lymphatic Metastasis, Quality of Life, Female, Lymph Nodes, business, medicine.drug

Abstract

BACKGROUND: In the phase III SOLE trial, the extended use of intermittent versus continuous letrozole for 5 years did not improve disease-free survival in postmenopausal women with hormone receptor-positive breast cancer. Intermittent therapy with 3-month breaks may be beneficial for patients' quality of life (QoL). METHODS: In the SOLE QoL sub-study, 956 patients completed the Breast Cancer Prevention Trial (BCPT) symptom and further QoL scales up to 24 months after randomisation. Differences in change of QoL from baseline between the two administration schedules were tested at 12 and 24 months using repeated measures mixed-models. The primary outcome was change in hot flushes at 12 months. RESULTS: There was no difference in hot flushes at 12 months between the two schedules, but patients receiving intermittent letrozole reported significantly more improvement at 24 months. They also indicated less worsening in vaginal problems, musculoskeletal pain, sleep disturbance, physical well-being and mood at 12 months. Overall, 25-30% of patients reported a clinically relevant worsening in key symptoms and global QoL. CONCLUSION: Less symptom worsening was observed during the first year of extended treatment with the intermittent administration. For women experiencing an increased symptom burden of extended adjuvant endocrine therapy, an intermittent administration is a safe alternative. CLINICAL TRIAL INFORMATION: Clinical trial information: NCT00651456. ispartof: BRITISH JOURNAL OF CANCER vol:120 issue:10 pages:959-967 ispartof: location:England status: published

Published

2018

42. Characterization of male breast cancer: results of the EORTC 10085/TBCRC/BIG/NABCG International Male Breast Cancer Program

Author

B. Linderholm, John W.M. Martens, Joanna Vermeij, M Nowaczyk, Oliver Bogler, Sharon H. Giordano, Melissa Murray, C. Poncet, Kevin Punie, Cecilia Nilsson, Carolien P. Schröder, John M. S. Bartlett, Ingrid Hedenfalk, Lavinia P. Middleton, K Aalders, Fatima Cardoso, Kathryn J. Ruddy, Stefan Aebi, Isabel T. Rubio, E van Leeuwen-Stok, Theodora Goulioti, Peggy L. Porter, Aleksandra Peric, Catherine M. Kelly, Judith Fraser, C. J. van Asperen, Kim Benstead, L. Dal Lago, Leen Slaets, Eric P. Winer, Konstantinos Tryfonidis, Jane Bayani, Saskia Litière, Larissa A. Korde, Clifford A. Hudis, C.H.M. van Deurzen, Guided Treatment in Optimal Selected Cancer Patients (GUTS), Pathology, and Medical Oncology

Subjects

0301 basic medicine, Oncology, Male, medicine.medical_treatment, Lobular carcinoma, Estrogen receptor, consortium, Kaplan-Meier Estimate, male breast cancer, THERAPY, RECOMMENDATIONS, 0302 clinical medicine, Surveys and Questionnaires, Breast-conserving surgery, clinical and biological characteristics, medicine.diagnostic_test, Hematology, Middle Aged, retrospective analysis, ESTROGEN, 030220 oncology & carcinogenesis, Male breast cancer, medicine.drug, EXPRESSION, Adult, medicine.medical_specialty, KLINEFELTERS-SYNDROME, PATIENT, Breast Neoplasms, Male, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Internal medicine, LOBULAR CARCINOMA, Progesterone receptor, Biopsy, medicine, Biomarkers, Tumor, Humans, Aged, Proportional Hazards Models, Retrospective Studies, business.industry, MUTATIONS, Retrospective cohort study, Original Articles, medicine.disease, CONSENSUS GUIDELINES, BRCA2, 030104 developmental biology, business, Tamoxifen

Abstract

Background: Male breast cancer (BC) is rare, managed by extrapolation from female BC. The International Male BC Program aims to better characterize and manage this disease. We report the results of part I, a retrospective joint analysis of cases diagnosed during a 20-year period.Methods: Patients with follow-up and tumor samples, treated between 1990 and 2010, in 93 centers/9 countries. Samples were centrally analyzed in three laboratories (the United Kingdom, the Netherlands and the United States).Results: Of 1822 patients enrolled, 1483 were analyzed; 63.5% were diagnosed between 2001 and 2010, 57 (5.1%) had metastatic disease (M1). Median age at diagnosis: 68.4 years. Of 1054 M0 cases, 56.2% were node-negative (N0) and 48.5% had T1 tumors; 4% had breast conserving surgery (BCS), 18% sentinel lymph-node biopsy; half received adjuvant radiotherapy; 29.8% (neo) adjuvant chemotherapy and 76.8% adjuvant endocrine therapy (ET), mostly tamoxifen (88.4%). Per central pathology, for M0 tumors: 84.8% ductal invasive carcinomas, 51.5% grade 2; 99.3% estrogen receptor (ER)-positive; 81.9% progesterone receptor (PR)-positive; 96.9% androgen receptor (AR)-positive [ER, PR or AR Allred score >= 3]; 61.1% Ki67 expression low (Conclusions: Male BC is usually ER, PR and AR-positive, Luminal B-like/HER2-negative. Of note, 56% patients had T1 tumors but only 4% had BCS. ER was highly positive in> 90% of cases but only 77% received adjuvant ET. ER, PR and AR were associated with OS and RFS, whereas grade, Ki67 and IHC surrogates were not. Significant improvement in survival over time was observed.

Published

2018

43. Nivolumab for recurrent cutaneous squamous cell carcinoma: three cases

Author

Veronika, Blum, Beat, Müller, Silvia, Hofer, Esther, Pardo, Kristin, Zeidler, Joachim, Diebold, Klaus, Strobel, Christoph, Brand, Stefan, Aebi, and Oliver, Gautschi

Subjects

Aged, 80 and over, Male, Nivolumab, Skin Neoplasms, Programmed Cell Death 1 Receptor, Carcinoma, Squamous Cell, Antibodies, Monoclonal, Humans, Antineoplastic Agents, Female, Neoplasm Recurrence, Local, Switzerland, Aged

Abstract

Programmed cell death ligand 1 (PD-L1) is frequently expressed in cutaneous squamous cell cancer (CSCC) and preliminary data from an ongoing clinical trial suggest that programmed death receptor 1 (PD-1) checkpoint inhibitors may be useful to treat patients with metastatic non-melanoma skin cancer. To report a series of three patients with advanced CSCC treated with nivolumab, showing that commercially available PD-1 checkpoint inhibitors may be useful in non-melanoma skin cancer patients without access to a clinical trial. All patients had previous chemotherapy. All cancers were PD-1 ligand (PD-L1)-positive based on immunohistochemistry. Patients consented to off-label therapy with nivolumab, which is commercially available in Switzerland. Two patients had a partial tumour response, and have been receiving therapy for more than 12 months. One patient had stable disease after three months, and therapy is also ongoing. So far, no severe adverse effects have occurred. Our cases confirm previous reports demonstrating a clinical effect and tolerability of PD-1 checkpoint inhibitors for heavily pre-treated patients with metastatic CSCC. Commercially available PD-1 checkpoint inhibitors may be useful in these patients who should be considered for PD-1 checkpoint inhibitor therapy, preferentially within clinical trials.

Published

2018

44. Contributors

Author

Balkees Abderrahman, Stefan Aebi, Prasanna Alluri, Benjamin O. Anderson, Cletus A. Arciero, Raheela Ashfaq, Thomas Aversano, Jennifer Axilbund, Ebrahim Azizi, Rajesh Banderudrappagari, Andrea V. Barrio, Lawrence W. Bassett, Isabelle Bedrosian, Alyssa Berkowitz, Therese B. Bevers, Kirby I. Bland, Cristiano Boneti, Zeynep Bostanci, Ursa Brown-Glaberman, Adam Brufsky, Gwendolyn Bryant-Smith, Oren Cahlon, Benjamin C. Calhoun, Kristine E. Calhoun, Ryan J. Carr, Helena R. Chang, Steven L. Chen, Alice Chung, Maureen A. Chung, Hiram S. Cody, Edward M. Copeland, Ricardo Costa, Jorge I. de la Torre, Amy C. Degnim, Mary L. Disis, William D. Dupont, Melinda S. Epstein, Francisco J. Esteva, David M. Euhus, Suzanne Evans, Oluwadamilola M. Fayanju, Gary M. Freedman, Patrick Bryan Garvey, Abby Geletzke, Mary L. Gemignani, Armando E. Giuliano, Mehra Golshan, William J. Gradishar, Jill Granger, Caprice C. Greenberg, Lars J. Grimm, Stephen R. Grobmyer, Nora Hansen, Ramdane Harouaka, Eleanor E. Harris, Lynn C. Hartmann, Tina J. Hieken, Susan Higgins, Dennis Holmes, Kelly K. Hunt, E. Shelley Hwang, Reshma Jagsi, Sarika Jain, Bharti Jasra, Jacqueline S. Jeruss, Rafael E. Jimenez, Veronica Jones, V. Craig Jordan, Himanshu Joshi, Virginia Kaklamani, Nina J. Karlin, Meghan S. Karuturi, Rena B. Kass, Kenneth Kern, Seema A. Khan, Jennifer R. Klemp, V. Suzanne Klimberg, Soheila Korourian, Henry M. Kuerer, Asangi R. Kumarapeli, Priya Kumthekar, Maryann Kwa, Michael D. Lagios, Jeffrey Landercasper, Kate I. Lathrop, Gordon K. Lee, Stephanie Lee-Felker, A. Marilyn Leitch, D. Scott Lind, Charles L. Loprinzi, Anthony Lucci, Tahra Kaur Luther, Neil Majithia, Issam Makhoul, Melissa Anne Mallory, Anne T. Mancino, Sanjay Maraboyina, Aju Mathew, Damian McCartan, Susan A. McCloskey, Beryl McCormick, Karishma Mehra, Jane E. Mendez, Priya V. Mhatre, Michael D. Mix, Meena S. Moran, Molly Moravek, Leigh Neumayer, Samilia Obeng-Gyasi, Patience Odele, Maureen O'Donnell, Colleen M. O'Kelly Priddy, Ruth M. O'Regan, Sonal Oza, Holly J. Pederson, Angela Pennisi, Margot S. Peters, Sara B. Peters, Lindsay F. Petersen, Melissa Pilewskie, Raquel Prati, Michael F. Press, Erik Ramos, Amy E. Rivere, Arlan L. Rosenbloom, Kathryn J. Ruddy, Kilian E. Salerno, Melinda E. Sanders, Tara Sanft, Cesar A. Santa-Maria, Jennifer Sasaki, Nirav B. Savalia, Chirag Shah, Samman Shahpar, Yu Shyr, Melvin J. Silverstein, Jean F. Simpson, George W. Sledge, Karen Lisa Smith, Stephen M. Smith, George Somlo, Sasha E. Stanton, Vered Stearns, Matthew A. Steliga, Alison T. Stopeck, Toncred M. Styblo, Susie X. Sun, Melinda L. Telli, Amye J. Tevaarwerk, Parijatham S. Thomas, Nicholas D. Tingquist, Jacqueline Tsai, Stephanie A. Valente, Astrid Botty Van den Bruele, Luis O. Vasconez, Doctor Honoris Causa, Frank A. Vicini, Rebecca K. Viscusi, Daniel W. Visscher, Victor G. Vogel, Adrienne G. Waks, Irene L. Wapnir, Thomas Wells, Julia White, Max S. Wicha, Eric P. Winer, Kari B. Wisinski, Debra A. Wong, Teresa K. Woodruff, Eric J. Wright, Melissa Young, and Zachary T. Young

Published

2018

45. Axillary dissection versus no axillary dissection in patients with breast cancer and sentinel-node micrometastases (IBCSG 23-01): 10-year follow-up of a randomised, controlled, phase 3 trial

Author

Achim Fleischmann, Cindy Mak, Jane Hill, David Littlejohn, Andreas Veronesi, Holger Moch, Stefano Zurrida, L Perey, Nirmala Pathmanathan, Carlo Tondini, Giancarlo Pruneri, Viviana Galimberti, Christian Oehlschlegel, Christoph Rageth, Jack Hoffmann, Richard D. Gelber, John J. Collins, Angelo Recalcati, Marisa Donatella Magri, Andrée Rorive, Bruno Späti, Dimitri Sarlos, Zsuzsanna Varga, Rolf A. Stahel, Mattia Intra, Charlotte Lanng, P. Smart, L. Tan, Anna Cardillo, Francesco Coran, James French, Rudolf Maibach, Manuela Rabaglio, Marco Colleoni, Emilia Montagna, Elisabeth Saurenmann, Elisabeth Elder, Michael Knauer, Samuele Massarut, Mauro Arcicasa, Karin Ribi, Julie Craik, Theresa Zielinski, Wendy Jeanneret Sozzi, Sandro Morassut, Tiziana Rusca, Paul Chin, Elgene Lim, Frances M. Boyle, Richard West, Patrizia Dell'Orto, Umberto Veronesi, Marie-Christine Mathieu, Jean-Remi Garbay, Katrina Moore, Marisa Cristina Leonardi, Gregory Bruce Mann, Donatella Santini, Mario Roncadin, Joëlle Collignon, Michael D. Green, David Moon, Oreste Gentilini, Petere G. Gill, Stephen Allpress, Giulia Peruzzotti, Elga Majdic, Caitlin Mahoney, Karen N. Price, Craig Murphy, Lori Hayes, Melissa Bochner, Lynette Mann, Christoph Tausch, Otto Schiltknecht, Antonino Carbone, Aron Goldhirsch, Giuseppe Cancello, Anand Murugasu, John F. Forbes, Erica Piccoli, Luca Mazzucchelli, Alberto Gianatti, Lucien Zaman, Jose Manuel Cotrina, Per Karlsson, Janez Zgajnar, Diana Crivellari, Birgitte Bruun Rasmussen, Elisabetta Candiago, Manuela Sargenti, Robert Whitfield, Silvia Dellapasqua, R. Ghisini, Meredith M. Regan, Michael Müller, Tiziana Perin, M. Thorburn, Stamatina Fournarakou, Monika Bamert, Malcolm Buchanan, Allison Jones, Gerhard Ries, Andreas Ehrsam, Hugh Carmalt, István Láng, Jürg Bernhard, Guy Jerusalem, Manuela Lagrassa, S. Fiona Bonar, Mario Mileto, Jurij Lindtner, P. Jeal, Fereshte Farshidi, Bernard F. Cole, John Hoerby, James Kollias, Privato Fenaroli, Giovanni Mazzarol, Richard Dyer, Angelo Buonadonna, Heidi Roschitzki, Stefania Andrighetto, Robert Macindoe, Martin F. Fey, Ingrid Kössler, Olivia Pagani, Anita Hiltbrunner, Camelia Chifu, William Ross, Rachele Volpe, Linda Leidi, Barbara Ruepp, Giorgio Caccia, Philippe Delvenne, Susanne Gerred, Tara Scolese, Mario Taffurelli, Paola Baratella, Jean Francois Delaloye, Richard Harman, A. Michael Bilous, Ian G. Campbell, Franco Nolè, Maryse Fiche, Ute Lorenz, Susanne Roux, Roberto Orecchia, Mark Sywak, Aashit Shah, Assia Treboux, Laura Cattaneo, Martina Egli-Tupaj, Rosmarie Caduff, Paolo Veronesi, Linda Madigan, Elena Kralidis, Maj-Lis Moeller Talman, Roswitha Kammler, Michael Töpfer, Eva Juhasz, Peer Schousen, Michele Ghielmini, Snjezana Frkovic-Grazio, Hanne Galatius, Elisabeth Rippy, Sylvie Maweja, Lynette Blacher, Stefan Aebi, D.F. Preece, Gilles Berclaz, Daniel Wyss, D. F. Lindsay, Andreas Günthert, Frederick Mayall, Lucia Bronz, Paul McKenzie, Andrew J. Spillane, Giuseppe Viale, Sandra Lippert, Alberto Luini, Virginia Howard, Giuseppe Curigliano, Rainer Grobholz, Robert Millar, Julio Abugattas, Hans-Anton Lehr, Maria Emanuela Limonta, Monica Iorfida, Elisa Vicini, Helle Holtveg, Angelo Di Leo, Giuseppe Renne, Alan S. Coates, Ezio Candiani, Karolyn Scott, Mauro G. Mastropasqua, Paolo Tricomi, Thomas Gyr, Karen Briscoe, and Viviana Galimberti, Bernard F Cole, Giuseppe Viale, Paolo Veronesi, Elisa Vicini, Mattia Intra, Giovanni Mazzarol, Samuele Massarut, Janez Zgajnar, Mario Taffurelli, David Littlejohn, Michael Knauer, Carlo Tondini, Angelo Di Leo, Marco Colleoni, Meredith M Regan, Alan S Coates, Richard D Gelber, Aron Goldhirsch

Subjects

0301 basic medicine, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Population, Breast Neoplasms, Disease-Free Survival, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Risk Factors, Clinical endpoint, Medicine, Humans, education, Mastectomy, education.field_of_study, business.industry, Sentinel Lymph Node Biopsy, Hazard ratio, Sentinel node, medicine.disease, Breast cancer, axillary dissection, IBCSG 23-01, follow up, Surgery, Clinical trial, Axilla, 030104 developmental biology, medicine.anatomical_structure, Oncology, Neoplasm Micrometastasis, 030220 oncology & carcinogenesis, Lymphatic Metastasis, Disease Progression, Lymph Node Excision, Female, Sentinel Lymph Node, business

Abstract

Summary Background We previously reported the 5-year results of the phase 3 IBCSG 23-01 trial comparing disease-free survival in patients with breast cancer with one or more micrometastatic (≤2 mm) sentinel nodes randomly assigned to either axillary dissection or no axillary dissection. The results showed no difference in disease-free survival between the groups and showed non-inferiority of no axillary dissection relative to axillary dissection. The current analysis presents the results of the study after a median follow-up of 9·7 years (IQR 7·8–12·7). Methods In this multicentre, randomised, controlled, open-label, non-inferiority, phase 3 trial, participants were recruited from 27 hospitals and cancer centres in nine countries. Eligible women could be of any age with clinical, mammographic, ultrasonographic, or pathological diagnosis of breast cancer with largest lesion diameter of 5 cm or smaller, and one or more metastatic sentinel nodes, all of which were 2 mm or smaller and with no extracapsular extension. Patients were randomly assigned (1:1) before surgery (mastectomy or breast-conserving surgery) to no axillary dissection or axillary dissection using permuted blocks generated by a web-based congruence algorithm, with stratification by centre and menopausal status. The protocol-specified primary endpoint was disease-free survival, analysed in the intention-to-treat population (as randomly assigned). Safety was assessed in all randomly assigned patients who received their allocated treatment (as treated). We did a one-sided test for non-inferiority of no axillary dissection by comparing the observed hazard ratios (HRs) for disease-free survival with a margin of 1·25. This 10-year follow-up analysis was not prespecified in the trial's protocol and thus was not adjusted for multiple, sequential testing. This trial is registered with ClinicalTrials.gov, number NCT00072293. Findings Between April 1, 2001, and Feb 8, 2010, 6681 patients were screened and 934 randomly assigned to no axillary dissection (n=469) or axillary dissection (n=465). Three patients were ineligible and were excluded from the trial after randomisation. Disease-free survival at 10 years was 76·8% (95% CI 72·5–81·0) in the no axillary dissection group, compared with 74·9% (70·5–79·3) in the axillary dissection group (HR 0·85, 95% CI 0·65–1·11; log-rank p=0·24; p=0·0024 for non-inferiority). Long-term surgical complications included lymphoedema of any grade in 16 (4%) of 453 patients in the no axillary dissection group and 60 (13%) of 447 in the axillary dissection group, sensory neuropathy of any grade in 57 (13%) in the no axillary dissection group versus 85 (19%) in the axillary dissection group, and motor neuropathy of any grade (14 [3%] in the no axillary dissection group vs 40 [9%] in the axillary dissection group). One serious adverse event (postoperative infection and inflamed axilla requiring hospital admission) was attributed to axillary dissection; the event resolved without sequelae. Interpretation The findings of the IBCSG 23-01 trial after a median follow-up of 9·7 years (IQR 7·8–12·7) corroborate those obtained at 5 years and are consistent with those of the 10-year follow-up analysis of the Z0011 trial. Together, these findings support the current practice of not doing an axillary dissection when the tumour burden in the sentinel nodes is minimal or moderate in patients with early breast cancer. Funding International Breast Cancer Study Group.

Published

2018

46. Clinical importance of risk variants in the dihydropyrimidine dehydrogenase gene for the prediction of early-onset fluoropyrimidine toxicity

Author

Tanja K, Froehlich, Ursula, Amstutz, Stefan, Aebi, Markus, Joerger, and Carlo R, Largiadèr

Subjects

Adult, Aged, 80 and over, Male, Risk, Adolescent, Haplotypes, Humans, Female, Fluorouracil, Middle Aged, Polymorphism, Single Nucleotide, Dihydrouracil Dehydrogenase (NADP), Aged

Abstract

We investigated the clinical relevance of dihydropyrimidine dehydrogenase gene (DPYD) variants to predict severe early onset fluoropyrimidine (FP) toxicity in particular of a recently discovered haplotype hapB3 and a linked deep intronic splice site mutation c.1129 5923C>G. Selected regions of DPYD were sequenced in prospectively collected germline DNA of 500 patients receiving FP based chemotherapy. Associations of DPYD variants and haplotypes with hematologic gastrointestinal infectious and dermatologic toxicity in therapy cycles 1 2 and resulting FP dose interventions (dose reduction therapy delay or cessation) were analyzed accounting for clinical and demographic covariates. Fifteen additional cases with toxicity related therapy delay or cessation were retrospectively examined for risk variants. The association of c.1129 5923C>G/hapB3 (4.6\ carrier frequency) with severe toxicity was replicated in an independent prospective cohort. Overall c.1129 5923G/hapB3 carriers showed a relative risk of 3.74 (RR 95\ CI=2.30 6.09 p=2 x 10( 5)) for severe toxicity (grades 3 5). Of 31 risk variant carriers (c.1129 5923C>G/hapB3 c.1679T>G c.1905+1G>A or c.2846A>T) 11 (all with c.1129 5923C>G/hapB3) experienced severe toxicity (15\ of 72 cases RR=2.73 95\ CI=1.61 4.63 p=5 x 10( 6)) and 16 carriers (55\) required FP dose interventions. Seven of the 15 (47\) retrospective cases carried a risk variant. The c.1129 5923C>G/hapB3 variant is a major contributor to severe early onset FP toxicity in Caucasian patients. This variant may substantially improve the identification of patients at risk of FP toxicity compared to established DPYD risk variants (c.1905+1G>A c.1679T>G and c.2846A>T). Pre therapeutic DPYD testing may prevent 20 30\ of life threatening or lethal episodes of FP toxicity in Caucasian patients. What's New? Fluorouracil (5FU) is effective against a variety of cancers and is one of the most commonly prescribed chemotherapy drugs. But 5FU causes severe toxicity in some patients with their susceptibility determined largely by variations in the rate limiting enzyme dihydropyrimidine dehydrogenase (DPD) which catabolizes 5FU. This study shows that a relatively common haplotype hapB3 which is linked to an intronic splice site mutation (c.1129 5923C>G) in the DPD encoding gene DPYD is a major contributor to early onset severe fluoropyrimidine toxicity in Caucasian carriers. Inclusion of the c.1129 5923C>G variant in DPYD genetic testing could help prevent severe toxicity associated with fluoropyrimidine based therapies.

Published

2015

47. Dihydropyrimidinase and beta-ureidopropionase gene variation and severe fluoropyrimidine-related toxicity

Author

Tanja K. Froehlich, Ursula Amstutz, Stefan Aebi, Johanna Sistonen, Dominic Kummer, Markus Joerger, and Carlo R. Largiadèr

Subjects

Oncology, Adult, Male, medicine.medical_specialty, Antimetabolites, Antineoplastic, Adolescent, Drug-Related Side Effects and Adverse Reactions, Genotype, Biology, Bioinformatics, Amidohydrolases, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, Genetic variation, Genetics, medicine, Dihydropyrimidine dehydrogenase, Humans, Gene, 030304 developmental biology, Aged, Pharmacology, Aged, 80 and over, 0303 health sciences, Case-control study, Genetic Variation, Exons, Middle Aged, 3. Good health, Pyrimidines, 030220 oncology & carcinogenesis, Dihydropyrimidinase, Pharmacogenomics, Case-Control Studies, Toxicity, Molecular Medicine, Female, Fluorouracil

Abstract

Aims: To assess the association of DPYS and UPB1 genetic variation, encoding the catabolic enzymes downstream of dihydropyrimidine dehydrogenase, with early-onset toxicity from fluoropyrimidine-based chemotherapy. Patients & methods: The coding and exon-flanking regions of both genes were sequenced in a discovery subset (164 patients). Candidate variants were genotyped in the full cohort of 514 patients. Results & conclusions: Novel rare deleterious variants in DPYS (c.253C > T and c.1217G > A) were detected once each in toxicity cases and may explain the occurrence of severe toxicity in individual patients, and associations of common variants in DPYS (c.1–1T > C: padjusted = 0.003; OR = 2.53; 95% CI: 1.39–4.62, and c.265–58T > C: padjusted = 0.039; OR = 0.61; 95% CI: 0.38–0.97) with 5-fluorouracil toxicity were replicated.

Published

2015

48. Editorial Board / Contents / Imprint / Guidelines for Authors

Author

Antonello Calderoni, Seong-Jang Kim, Xiangdong Li, Lukas C. Heukamp, Salah-Eddin Al-Batran, Rudolf Morant, Yuan Guo, Uwe Pinkert, Stefan Aebi, Adrian Casty, Christoph Springfeld, Daniel Betticher, Arndt Vogel, Katharina König, R. R. Plentz, Chaoyang Cui, Carola Stadelmann, Martina Becker-Schiebe, Oliver Gautschi, Christa Baumann, Andreas Trojan, Christoph Mamot, Erica Pellicioli, Matthias Sperling, Franziska Aebersold-Keller, Wolfgang Hoffmann, Giannicola DʼAddario, Samuel Chang, Volker Kunzmann, Frank Kullmann, Reinhard Büttner, Jens T. Siveke, Guang Yang, Sonja Jehle-Schwertfeger, Joachim Diebold, Katharina Buser, Helmut Oettle, Claudius Irlé, and Hanno Riess

Subjects

Cancer Research, Medical education, Oncology, business.industry, Medicine, Hematology, Editorial board, business

Published

2015

49. Status quo in der Zweitlinientherapie des NSCLC und Ausblick in die Zukunft

Author

Jens T. Siveke, Christoph Mamot, Lukas C. Heukamp, Erica Pellicioli, Uwe Pinkert, Joachim Diebold, Salah-Eddin Al-Batran, Chaoyang Cui, Oliver Gautschi, Frank Kullmann, Hanno Riess, Giannicola DʼAddario, Antonello Calderoni, Carola Stadelmann, Daniel Betticher, Wolfgang Hoffmann, Yuan Guo, Reinhard Büttner, Christa Baumann, Helmut Oettle, Guang Yang, Franziska Aebersold-Keller, Stefan Aebi, Xiangdong Li, Claudius Irlé, R. R. Plentz, Arndt Vogel, Volker Kunzmann, Katharina Buser, Katharina König, Rudolf Morant, Andreas Trojan, Sonja Jehle-Schwertfeger, Christoph Springfeld, Samuel Chang, Adrian Casty, Seong-Jang Kim, Martina Becker-Schiebe, and Matthias Sperling

Subjects

Cancer Research, Oncology, Hematology

Published

2015

50. Retinoid receptors in ovarian cancer: expression and prognosis

Author

A. Kappeler, Stefan Aebi, P. C. Kaiser, and M. Körner

Subjects

endocrine system diseases, medicine.drug_class, Receptors, Retinoic Acid, Retinoic acid, Retinoid receptor, 610 Medicine & health, Retinoid X receptor, chemistry.chemical_compound, Ovarian carcinoma, medicine, Humans, Retinoid, RNA, Messenger, Aged, DNA Primers, Ovarian Neoplasms, Base Sequence, business.industry, Reverse Transcriptase Polymerase Chain Reaction, Hematology, Middle Aged, medicine.disease, Prognosis, Immunohistochemistry, Retinoic acid receptor, Oncology, chemistry, Nuclear receptor, Cancer research, 570 Life sciences, biology, Female, Ovarian cancer, business

Abstract

BACKGROUND Ovarian cancer is frequently lethal despite aggressive multimodal therapy, and new therapies are therefore needed. Retinoids are potential candidate drugs: they prevent the development of ovarian carcinoma and enhance the efficacy of cytotoxic drugs in ovarian cancer cells. At present, little is known about the retinoid receptor expression in ovarian cancer. PATIENTS AND METHODS The retinoid receptors comprise two classes, retinoic acid receptors (RARs) and retinoid X receptors (RXRs), each with three subclasses, alpha, beta and gamma. We investigated the expression of the subtypes RARalpha, RARgamma, RXRalpha and RXRbeta by immunohistochemistry in ovarian cancers of 80 patients, and assessed their prognostic significance. In addition, we quantified the expression of retinoid receptor mRNA using real-time PCR and correlated the results with clinical characteristics. RESULTS RARalpha and RXRbeta were highly expressed in a majority of ovarian cancers, particularly in advanced stages. High expression of RARalpha was an independent negative prognostic factor of survival in addition to FIGO stage, age and p53 accumulation. The mRNA expression of retinoid receptors did not correlate with clinical properties of the tumors. CONCLUSIONS Retinoic acid receptors are frequently and strongly expressed in epithelial ovarian cancer and may be indicators of an adverse prognosis. This study provides the molecular basis for the therapeutic use of retinoids in ovarian cancer.

Published

2017