Your search keyword '"Gluz O"' showing total 30 results

1. Nab-paclitaxel weekly versus dose-dense solvent-based paclitaxel followed by dose-dense epirubicin plus cyclophosphamide in high-risk HR+/HER2− early breast cancer: results from the neoadjuvant part of the WSG-ADAPT-HR+/HER2− trial.

Author

Gluz, O., Kuemmel, S., Nitz, U., Braun, M., Lüdtke-Heckenkamp, K., von Schumann, R., Darsow, M., Forstbauer, H., Potenberg, J., Uleer, C., Grischke, E.M., Aktas, B., Schumacher, C., zu Eulenburg, C., Kates, R., Jóźwiak, K., Graeser, M., Wuerstlein, R., Baehner, R., and Christgen, M.

Subjects

*HORMONE receptor positive breast cancer, *EPIDERMAL growth factor receptors, *CLINICAL trials, *BREAST cancer, *PACLITAXEL, *EPIRUBICIN

Abstract

In high-risk hormone receptor-positive/human epidermal growth factor receptor 2-negative (HR+/HER2−) early breast cancer (EBC), nanoparticle albumin-bound (nab)-paclitaxel showed promising efficacy versus solvent-based (sb)-paclitaxel in neoadjuvant trials; however, optimal patient and therapy selection remains a topic of ongoing research. Here, we investigate the potential of Oncotype DX® recurrence score (RS) and endocrine therapy (ET) response (low post-endocrine Ki67) for therapy selection. Within the WSG-ADAPT trial (NCT01779206), high-risk HR+/HER2− EBC patients were randomized to (neo)adjuvant 4× sb-paclitaxel 175 mg/m2 q2w or 8× nab-paclitaxel 125 mg/m2 q1w, followed by 4× epirubicin + cyclophosphamide (90 mg + 600 mg) q2w; inclusion criteria: (i) cN0-1, RS 12-25, and post-ET Ki67 >10%; (ii) cN0-1 with RS >25. Patients with cN2-3 or (G3, baseline Ki67 ≥40%, and tumor size >1 cm) were allowed to be included without RS and/or ET response testing. Associations of key factors with pathological complete response (pCR) (primary) and survival (secondary) endpoints were analyzed using statistical mediation and moderation models. Eight hundred and sixty-four patients received neoadjuvant nab-paclitaxel (n = 437) or sb-paclitaxel (n = 427); nab-paclitaxel was superior for pCR (20.8% versus 12.9%, P = 0.002). pCR was higher for RS >25 versus RS ≤25 (16.0% versus 8.4%, P = 0.021) and for ET non-response versus ET response (15.1% versus 6.0%, P = 0.027); no factors were predictive for the relative efficacy of nab-paclitaxel versus sb-paclitaxel. Patients with pCR had longer distant disease-free survival [dDFS; hazard ratio 0.42, 95% confidence interval (CI) 0.20-0.91, P = 0.024]. Despite favorable prognostic association of RS >25 versus RS ≤25 with pCR (odds ratio 3.11, 95% CI 1.71-5.63, P ≤ 0.001), higher RS was unfavorably associated with dDFS (hazard ratio 1.03, 95% CI 1.01-1.05, P = 0.010). In high-risk HR+/HER2− EBC, neoadjuvant nab-paclitaxel q1w appears superior to sb-paclitaxel q2w regarding pCR. Combining RS and ET response assessment appears to select patients with highest pCR rates. The disadvantage of higher RS for dDFS is reduced in patients with pCR. These are the first results from a large neoadjuvant randomized trial supporting the use of RS to help select patients for neoadjuvant chemotherapy in high-risk HR+/HER2− EBC. • 16-week neoadjuvant nab-paclitaxel induces higher pCR than sb-paclitaxel–epirubicin/cyclophosphamide in high-risk HR+/HER2− breast cancer. • First prospective phase III trial showed that higher RS is predictive for pCR. • Associations of higher RS and ET non-response with pCR are moderated by menopausal status (and/or ET agent used). • pCR mitigates the unfavorable impact of higher RS on dDFS. • Further trials should investigate therapy de-escalation in patients with RS >25, ET response, and lower clinical risk. [ABSTRACT FROM AUTHOR]

Published

2023

2. LBA17 Survival outcome of neoadjuvant endocrine therapy + trastuzumab and pertuzumab (ET+T+P) vs. de-escalated chemotherapy (CT)+T+P in hormone receptor positive (HR+)/HER2+ early breast cancer (EBC): WSG-TP-II trial.

Author

Gluz, O., Nitz, U.A., Christgen, M., Kummel, S., Holtschmidt, J., Schumacher, J., Hartkopf, A.D., Luedtke-Heckenkamp, K., Just, M., von Schumann, R., Polata, S., Schinköthe, T., Graeser-Mayer, M.K., Kates, R.E., Würstlein, R., Kreipe, H., and Harbeck, N.

Subjects

*HORMONE therapy, *HORMONE receptors, *NEOADJUVANT chemotherapy, *SURVIVAL rate, *BREAST cancer

Published

2024

3. 237MO TNBC-DX genomic test in early-stage triple-negative breast cancer treated with neoadjuvant taxane-based therapy without immunotherapy.

Author

Jimenez, M. Martin, Gluz, O., Villacampa, G., Lopez-Tarruella Cobo, S., Nitz, U.A., Cobo, S., Brasó-Maristany, F., Christgen, M., Gilarranz, Y. Jerez, Kummel, S., Conte, B., Diaz-Guardamino, I. Echavarria, Graeser-Mayer, M.K., Kreipe, H., Del Monte-Millan, M., Lopez, B. Herrero, Perou, C.M., Brunet, L. Pare, Prat, A., and Harbeck, N.

Subjects

*TRIPLE-negative breast cancer, *NEOADJUVANT chemotherapy, *IMMUNOTHERAPY

Published

2024

4. LBA14 Impact of age, recurrence score (RS) and ovarian function suppression (OFS) on endocrine response to short preoperative endocrine therapy (ET): Analysis of ADAPT and ADAPTcycle trials.

Author

Gluz, O., Nitz, U.A., Christgen, M., Kuemmel, S., Braun, M., Thill, M., Aktas, B., Wimberger, P., Luedtke-Heckenkamp, K., Zaiss, M., Warm, M., Schumacher, C., Schem, C., Graeser, M., Hartkopf, A.D., Kates, R.E., Eulenburg, C. zu, Schmid, P., Kreipe, H., and Harbeck, N.

Subjects

*HORMONE therapy, *AGE

Published

2022

5. De-escalation strategies in HER2-positive early breast cancer (EBC): final analysis of the WSG-ADAPT HER2+/HR— phase II trial: efficacy, safety, and predictive markers for 12 weeks of neoadjuvant dual blockade with trastuzumab and pertuzumab ± weekly paclitaxel

Author

Nitz, U. A., Gluz, O., Christgen, M., Grischke, E.-M., Augustin, D., Kuemmel, S., Braun, M., Potenberg, J., Kohls, A., Krauss, K., Stefek, A., Schumacher, C., Forstbauer, H., Reimer, T., Fischer, H., Liedtke, C., Wuerstlein, R., Schumacher, J., Kates, R., and Kreipe, H.

Subjects

*BREAST cancer, *TRASTUZUMAB, *PACLITAXEL, *CANCER chemotherapy, *TUMORS, *CANCER cells

Abstract

Background: Response rates in HER2-overexpressing EBC treated with neoadjuvant chemotherapy and trastuzumab (T) have been improved by addition of pertuzumab (P). The prospective, phase II, neoadjuvant WSG-ADAPT HER2+/HR— trial assessed whether patients with strong early response to dual blockade alone might achieve pathological complete response (pCR) comparable to that of patients receiving dual blockade and chemotherapy. Patients and methods: Female patients with HER2+/HR— EBC (M0) were randomized (5:2) to 12 weeks of T+P±weekly paclitaxel (pac) at 80 mg/m². Early response was defined as proliferation decrease ≥30% of Ki-67 (versus baseline) or low cellularity (<500 invasive tumor cells) in the 3-week biopsy. The trial was designed to test non-inferiority for pCR in early responding patients of the T+P arm versus all chemotherapy-treated patients. Results: From February 2014 to December 2015, 160 patients were screened, 92 were randomized to T+P and 42 to T+P+pac. Baseline characteristics were well balanced (median age 54 versus 51.5 years, cT2 51.1 versus 52.4%, cN0 54.3 versus 61.9%); 91.3% of patients completed T+P per protocol and 92.9% T+P+pac. The pCR rate in the T+P+pac arm was 90.5%, compared with 36.3% in the T+P arm as a whole. In the T+P arm, 24/92 were classified as non-responders, and their pCR rate was only 8.3% compared with 44.7% in responders (38/92) and 42.9% in patients with unclassified early response (30/92). No new safety signals were observed in the study population. Conclusion: Addition of taxane monotherapy to dual HER2 blockade in a 12-week neoadjuvant setting substantially increases pCR rates in HER2+/HR— EBC compared with dual blockade alone, even within early responders to dual blockade. Early nonresponse under dual blockade strongly predicts failure to achieve pCR. [ABSTRACT FROM AUTHOR]

Published

2017

6. Comparison of prognostic and predictive impact of genomic or central grade and immunohistochemical subtypes or IHC4 in HR+/HER2- early breast cancer: WSG-AGO EC-Doc Trial.

Author

Gluz, O., Liedtke, C., Huober, J., Peyro-Saint-Paul, H., Kates, R. E., Kreipe, H. H., Hartmann, A., Pelz, E., Erber, R., Mohrmann, S., Möbus, V., Augustin, D., Hoffmann, G., Thomssen, C., Jänicke, F., Kiechle, M., Wallwiener, D., Kuhn, W., Nitz, U., and Harbeck, N.

Subjects

*HORMONE receptor positive breast cancer, *BIOMARKERS, *EPIRUBICIN, *CANCER chemotherapy, *IMMUNOHISTOCHEMISTRY, *CANCER treatment, *THERAPEUTICS

Abstract

Introduction: Potential prognostic and predictive markers in early, intermediate-risk breast cancer (BC) include histological grade, Ki-67, genomic signatures, e.g. genomic grade index (GGI), and intrinsic subtypes. Their prognostic/ predictive impact in hormone receptor (HR: ER and/or PR) positive/HER2- BC is controversial. WSG-AGO EC-Doc demonstrated superior event-free survival (EFS) in patients with 1-3 positive lymph node receiving epirubicin/cyclophosphamide- docetaxel (EC-Doc) versus 5-fluoruracil/epirubicin/cyclophosphamide (FEC). Methods: In a representative trial subset, we quantify concordance among factors used for clinical chemotherapy indication. We investigate the impact of central histology (n = 772), immunohistochemistry for intrinsic subtyping and IHC4, and dichotomous (GG) or continuous (GGI) genomic grade (n = 472) on patient outcome and benefit from taxane chemotherapy, focusing on HR+/HER2- patients (n = 459). Results: Concordance of local grade (LG) with central (CG) or genomic grade was modest. In HR+/HER2- patients, low (GG-1: 16%), equivocal (GG-EQ: 17%), and high (GG-3: 67%) GG were associated with respective 5-year EFS of 100%, 93%, and 85%. GGI was prognostic for EFS within all LG subgroups and within CG3, whereas IHC4 was prognostic only in CG3 tumors. In unselected and HR+/HER2- patients, CG3 and luminal-A-like subtype entered the multivariate EFS model, but not IHC4 or GG. In the whole population, continuous GGI entered the model [hazard ratio (H.R.) of 75th versus 25th = 2.79; P = 0.01], displacing luminal-A-like subtype; within HR+/HER2- (H.R. = 5.36; P < 0.001), GGI was the only remaining prognostic factor. In multivariate interaction analysis (including central and genomic grade), luminal-Blike subtype [HR+ and (Ki-67 =20% or HER2+)] was predictive for benefit of EC-Doc versus FEC in unselected but not in HR+/HER2- patients. Conclusion: In the WSG-AGO EC-Doc trial for intermediate-risk BC, CG, intrinsic subtype (by IHC), and GG provide prognostic information. Continuous GGI (but not IHC4) adds prognostic information even when IHC subtype and CG are available. Finally, the high interobserver variability for histological grade and the still missing validation of Ki-67 preclude indicating or omitting adjuvant chemotherapy based on these single factors alone. [ABSTRACT FROM AUTHOR]

Published

2016

7. Final analysis of the prospective WSG-AGO EC-Doc versus FEC phase III trial in intermediate-risk (pN1) early breast cancer: efficacy and predictive value of Ki67 expression†.

Author

Nitz, U., Gluz, O., Huober, J., Kreipe, H. H., Kates, R. E., Hartmann, A., Erber, R., Scholz, M., Lisboa, B., Mohrmann, S., Möbus, V., Augustin, D., Hoffmann, G., Weiss, E., Böhmer, S., Kreienberg, R., Du Bois, A., Sattler, D., Thomssen, C., and Kiechle, M.

Subjects

*CLINICAL trials, *LONGITUDINAL method, *CYCLOPHOSPHAMIDE, *GENE expression, *BREAST cancer patients, *CANCER chemotherapy

Abstract

WSG EC-Doc is a prospective randomized trial comparing sequential taxanes versus taxane-free control involving more than 2000 early breast cancer patients at intermediate risk of recurrence (pN1). Addition of taxanes improves significantly event-free and overall survival rates. In hormone-sensitive disease only, patients with luminal B-like tumors as identified by high Ki-67 benefit from EC-Doc.Background Taxane-based adjuvant chemotherapy is standard in node-positive (N+) early breast cancer (BC). The magnitude of benefit in intermediate-risk N+ early BC is still unclear. WSG-AGO epiribicine and cyclophosphamide (EC)-Doc is a large trial evaluating modern taxane-based chemotherapy in patients with 1–3 positive lymph nodes (LNs) only. Patients and methods A total of 2011 BC patients (18–65 years, pN1) were entered into a randomized phase III trial comparing 4 × E90C600 q3w followed by 4 × docetaxel100 q3w (n = 1008) with the current standard: 6 × F500E100C500 q3w (n = 828) or C600M40F600 d1, 8× q4w (n = 175). Primary end point was event-free survival (EFS); secondary end points were overall survival (OS), toxicity, translational research, and quality of life. Central tumor bank samples were evaluable in a representative collective (n = 772; 40%). Ki-67 was assessed centrally in hormone receptor-positive disease as a surrogate marker for the distinction of luminal A/B-like tumors. Results Baseline characteristics were well balanced between study arms in both main study and central tumor bank subset. At 59-month median follow-up, superior efficacy of EC-Doc [versus FEC (a combination of 5-fluorouracil, epirubicin, and cyclophosphamide)] was seen in EFS and OS: 5-year EFS: 89.8% versus 87.3% (P = 0.038); 5-year OS: 94.5% versus 92.8% (P = 0.034); both tests one-tailed. EC-Doc caused more toxicity. In hormone receptor-positive (HR)+ disease, only high-Ki-67 tumors (≥20%) derived significant benefit from taxane-based therapy: hazard ratio = 0.39 (95% CI 0.18–0.82) for EC-Doc versus FEC (test for interaction; P = 0.01). Conclusion EC-Doc significantly improved EFS and OS versus FEC in intermediate-risk BC (1–3 LNs) within all subgroups as defined by local pathology. In HR+ disease, patients with luminal A-like tumors may be potentially over-treated by taxane-based chemotherapy. Clinical Trial number ClinicalTrials.gov, NCT02115204. [ABSTRACT FROM AUTHOR]

Published

2014

8. Final results from the prospective phase III WSG-ARA trial: impact of adjuvant darbepoetin alfa on event-free survival in early breast cancer†.

Author

Nitz, U., Gluz, O., Zuna, I., Oberhoff, C., Reimer, T., Schumacher, C., Hackmann, J., Warm, M., Uleer, C., Runde, V., Dünnebacke, J., Belzl, N., Augustin, D., Kates, R. E., and Harbeck, N.

Subjects

*ADJUVANT treatment of cancer, *DARBEPOETIN alfa, *BREAST cancer treatment, *CANCER chemotherapy, *ANEMIA, *RANDOMIZED controlled trials, *HEALTH outcome assessment

Abstract

WSG-ARA plus is a prospective phase III trial in node positive early breast cancer randomizing 1234 patients to standard adjuvant chemotherapy with or without darbepoetin (DA). Adjuvant DA treatment does not impact on EFS or OS in a routine adjuvant setting.Background WSG-ARA plus trial evaluated the effect of adjuvant darbepoetin alfa (DA) on outcome in node positive primary breast cancer (BC). Patients and methods One thousand two hundred thirty-four patients were randomized to chemotherapy either with DA (DA+; n = 615) or without DA (DA−; n = 619). DA (500 µg q3w) was started at hemoglobin (Hb) levels <13.0 g/dl (<12 g/dl after DA label amendment) and stopped at Hb levels ≥14.0 g/dl (12 g/dl after label amendment). Primary efficacy end point was event-free survival (EFS); secondary end points were toxicity, quality of life (QoL) and overall survival (OS). Results Venous thrombosis (DA+: 3.0%, DA−: 1.0%; P = 0.013) was significantly higher for DA+, but not pulmonary embolism (0.3% in both arms). Median Hb levels were stable in DA+ (12.6 g/dl) and decreased in DA− (11.7 g/dl). Hb levels >15 g/dl were reported in 0.8% of cycles. QoL parameters did not significantly differ between arms. At 39 months, DA had no significant impact on EFS (DA+: 89.3%, DA−: 87.5%; Plog-rank = 0.55) or OS (DA+: 95.5%, DA−: 95.4%; Plog-rank = 0.77). Conclusions DA treatment did not impact EFS or OS in routine adjuvant BC treatment. [ABSTRACT FROM AUTHOR]

Published

2014

9. Triple-negative breast cancer—current status and future directions.

Author

Gluz, O., Liedtke, C., Gottschalk, N., Pusztai, L., Nitz, U., and Harbeck, N.

Subjects

*TRIPLE-negative breast cancer, *CANCER patients, *ESTROGEN, *PROGESTERONE receptors, *EPIDERMAL growth factor, *DRUG therapy

Abstract

Triple-negative breast cancer (TNBC) is defined by a lack of expression of both estrogen and progesterone receptor as well as human epidermal growth factor receptor 2. It is characterized by distinct molecular, histological and clinical features including a particularly unfavorable prognosis despite increased sensitivity to standard cytotoxic chemotherapy regimens. TNBC is highly though not completely concordant with various definitions of basal-like breast cancer (BLBC) defined by high-throughput gene expression analyses. The lack in complete concordance may in part be explained by both BLBC and TNBC comprising entities that in themselves are heterogeneous. Numerous efforts are currently being undertaken to improve prognosis for patients with TNBC. They comprise both optimization of choice and scheduling of common cytotoxic agents (i.e. addition of platinum salts or dose intensification strategies) and introduction of novel agents (i.e. poly-ADP-ribose-polymerase-1 inhibitors, agents targeting the epidermal growth factor receptor, multityrosine kinase inhibitors or antiangiogenic agents). [ABSTRACT FROM PUBLISHER]

Published

2009

10. Corrigendum to "De-escalation strategies in HER2-positive early breast cancer (EBC): final analysis of the WSG-ADAPT HER2+/HR− phase II trial: efficacy, safety, and predictive markers for 12weeks of neoadjuvant dual blockade with trastuzumab and pertuzumab ± weekly paclitaxel": [Annals of Oncology 28 (2017) 2768-2772]

Author

Nitz, U.A., Gluz, O., Christgen, M., Grischke, E.-M., Augustin, D., Kuemmel, S., Braun, M., Potenberg, J., Kohls, A., Krauss, K., Stefek, A., Schumacher, C., Forstbauer, H., Reimer, T., Fischer, H., Liedtke, C., Wuerstlein, R., Schumacher, J., Kates, R., and Kreipe, H.

Subjects

*HER2 positive breast cancer, *TRASTUZUMAB

Published

2022

11. LBA2 Impact of RNA expression signatures and tumour infiltrating lymphocytes (TILs) for pathological complete response (pCR) and survival after 12 week de-escalated neoadjuvant pertuzumab + trastuzumab ± paclitaxel in the WSG-HER2+/HR- ADAPT trial.

Author

Graeser, M., Gluz, O., Biehl, C., Ulbrich-Gebauer, D., Palatty, J., Christgen, M., Kuemmel, S., Grischke, E-M., Augustin, D., Braun, M., Potenberg, J., Wuerstlein, R., Eulenburg, C., Kates, R., Kolberg-Liedtke, C., Feuerhake, F., Kreipe, H., Nitz, U., and Harbeck, N.

Subjects

*NEOADJUVANT chemotherapy, *BREAST cancer treatment, *TREATMENT effectiveness

Published

2021

12. LBA13Prognostic impact of anthracyclines and immune/proliferation markers in TNBC according to pCR after de-escalated neoadjuvant chemotherapy with 12 weeks of nab-paclitaxel/carboplatin or gemcitabine: Survival results of WSG-ADAPT-TN phase II trial.

Author

Gluz, O, Nitz, U, Liedtke, C, Christgen, M, Grischke, E-M, Forstbauer, H, Braun, M, Warm, M, Hackmann, J, and Uleer, C

Subjects

*CANCER chemotherapy, *TRIPLE-negative breast cancer

Published

2018

13. P213 - Five-year results of the prospective Phase III WSG PlanB trial confirm prognostic impact of 21-Gene Recurrence Score in high-risk HR+/HER2− early breast cancer (EBC) patients with 1-3 involved lymph nodes.

Author

Gluz, O., Nitz, U., Christgen, M., Kates, R., Clemens, M., Nuding, B., Shak, S., Würstlein, R., Kreipe, H., and Harbeck, N.

Subjects

BREAST cancer treatment, CANCER chemotherapy, CLINICAL trials, CANCER relapse, EPIDEMIOLOGY

Published

2017

14. P255 - Impact of MammaPrint and BluePrint on early breast cancer treatment decisions: WSG PRIMe study results.

Author

Wuerstlein, R., Grischke, E.M., Gluz, O., Kates, R., Persoon, M., Thill, M., Hasmueller, S., Knauer, M., Pusch, R., and Harbeck, N.

Subjects

BREAST cancer treatment, MEDICAL decision making, TREATMENT effectiveness, CLINICAL trials, CANCER relapse

Published

2017

15. P226 - Chemotherapy (CT) decision in node-positive (N+), ER+, early breast cancer (EBC) after new ASCO Guideline – evidence for the 21-gene Recurrence Score (RS) assay.

Author

Mamounas, E.P., Goldstein, L.J., Penault-Llorca, F., Roché, H., Gluz, O., Harbeck, N., Nitz, U., O’shaughnessy, J., and Albain, K.S.

Subjects

HORMONE receptor positive breast cancer, CANCER chemotherapy, BREAST cancer diagnosis, CANCER relapse, CLINICAL trials, CANCER treatment

Published

2017

16. P231 Luminal subtypes vs. early Ki-67 response and Oncotype DX® in early breast cancer: WSG-ADAPT study.

Author

Gluz, O., Nitz, U., Christgen, M., Kreipe, H., Kates, R.E., Kuemmel, S., Braun, M., Schumacher, C., Wuerstlein, R., and Harbeck, N.

Subjects

BREAST cancer patients, BREAST cancer, CANCER prevention, BREAST cancer treatment, BREAST cancer diagnosis, BREAST cancer surgery, CARCINOGENS, CANCER chemotherapy

Published

2015

17. Significantly longer time to deterioration of quality of life due to CANKADO PRO-React eHealth support in HR+ HER2− metastatic breast cancer patients receiving palbociclib and endocrine therapy: primary outcome analysis of the multicenter randomized AGO-B WSG PreCycle trial

Author

Harbeck, N., Fasching, P.A., Wuerstlein, R., Degenhardt, T., Lüftner, D., Kates, R.E., Schumacher, J., Räth, P., Hoffmann, O., Lorenz, R., Decker, T., Reinisch, M., Göhler, T., Staib, P., Gluz, O., Schinköthe, T., and Schmidt, M.

Subjects

*HORMONE receptor positive breast cancer, *METASTATIC breast cancer, *HORMONE therapy, *EPIDERMAL growth factor receptors, *PATIENT participation, *CANCER patients

Abstract

The multicenter, randomized, phase IV, intergroup AGO-B WSG PreCycle trial (NCT03220178) evaluated the impact of CANKADO-based electronic patient-reported outcome (ePRO) assessment on quality of life (QoL) in hormone receptor-positive, human epidermal growth factor receptor 2-negative locally advanced or metastatic breast cancer (MBC) patients receiving palbociclib and an aromatase inhibitor or palbociclib + fulvestrant. CANKADO PRO-React, a European Union-registered medical device, is an interactive autonomous application reacting to patient self-reported observations. Between 2017 and 2021, 499 patients (median age 59 years) from 71 centers were randomized (2 : 1, stratified by therapy line) between an active version of CANKADO PRO-React (CANKADO-active arm) and a version with limited functionality (CANKADO-inform arm). A total of 412 patients (271 CANKADO-active; 141 CANKADO-inform) were available for analysis of the primary endpoint, time to deterioration (TTD) of QoL [10-point drop on the Functional Assessment of Cancer Therapy—General (FACT-G) score], using an Aalen–Johansen estimator for cumulative incidence function of TTD DQoL (QoL deterioration) with 95% pointwise confidence intervals (CIs). Secondary endpoints included progression-free survival (PFS), overall survival (OS), and DQoL. In all patients [intention-to-treat (ITT)-ePRO], cumulative incidence of DQoL was significantly more favorable (lower) in the CANKADO-active arm (hazard ratio 0.698, 95% CI 0.506-0.963). Among first-line patients (n = 295), the corresponding hazard ratio was 0.716 (0.484-1.060; P = 0.09), and in second-line patients (n = 117) it was 0.661 (0.374-1.168; P = 0.2). Absolute patient numbers declined in later visits; FACT-G completion rates were 80% and higher until about visit 30. Mean FACT-G scores showed a steady decline from baseline and an offset in favor of CANKADO-active. No significant differences in clinical outcome were observed between arms: median PFS (ITT population) was 21.4 (95% CI 19.4-23.7) (CANKADO-active) and 18.7 (15.1-23.5) months (CANKADO-inform); median OS was not reached (CANKADO-active) and 42.6 months (CANKADO-inform). PreCycle is the first multicenter randomized eHealth trial demonstrating a significant benefit for MBC patients receiving oral tumor therapy when using an interactive autonomous patient empowerment application. • PreCycle evaluated the impact of an autonomous symptom monitoring application on TTD of QoL. • Primary endpoint was TTD of QoL in HR+/HER2- MBC treated with endocrine therapy + palbociclib. • Deterioration of QoL was significantly delayed with interactive CANKADO PRO-React-based ePRO assessment. [ABSTRACT FROM AUTHOR]

Published

2023

18. PP 30 Prospective comparison of Recurrence Score, uPA/PAI-1, central grade and molecular subtyping in early breast cancer: first results from the WSG-Plan B trial (interim analysis)

Author

Wuerstlein, R., Gluz, O., Kreipe, H., Kates, R., Degenhardt, T., Liedtke, C., Shak, S., Nitz, U., and Harbeck, N.

Published

2011

19. P178 Prospective comparison of uPA/PAI-1, Ki-67 based molecular classification, Recurrence Score and clinical–pathological characteristics in hormone-receptor (HR) positive primary breast cancer: Pilot phase of the randomized WSG PlanB trial.

Author

Liedtke, C., Gluz, O., Kreipe, H., Degenhardt, T., Kates, R., Baehner, R., Clemens, M., Wuerstlein, R., Nitz, U., and Harbeck, N.

Published

2011

20. P90 Tandem versus single high dose chemotherapy (HDC)with haematopoietic stem cell support in patients with chemosensitive metastatic breast cancer (MBC): outcome parameters - results from a randomised multicenter phase III trial.

Author

Mohrmann, S., Kroeger, N., Frick, M., Schuett, G., Metzner, B., Ko, Y., Berdel, E., Gluz, O., Nitz, U., and Zander, A.

Published

2005

21. P75 Current status and results of the second toxicityanalysis of a WSG/AGO-Mamma Intergroup Phase III trial AM02 “Ec->Doc” for patients with primary breast cancer and 1-3 positive axillary lymph nodes.

Author

Schuett, G.J., Gluz, O., Mohrmann, S., Kuhn, W., Huober, J., Borntr ger, J., buss, V.M., Harbeck, N., Bergmann, T., and Nitz, U.

Published

2005

22. 1LBA - Differential impact of prognostic parameters in hormone receptor-positive lobular early breast cancer in the WSG PlanB trial.

Author

Christgen, M., Harbeck, N., Gluz, O., Raap, M., Christgen, H., Clemens, M., Malter, W., Nuding, B., Aktas, B., Kuemmel, S., Reimer, T., Stefek, A., Krabisch, P., Just, M., Graeser, M., Baehner, R., Wuerstlein, R., Nitz, U., Kates, R., and Kreipe, H.

Subjects

*CONFERENCES & conventions, *HORMONE receptor positive breast cancer

Published

2020

23. 208P ARB: Phase II window of opportunity study of preoperative treatment with enzalutamide in ER+ve and TNBC.

Author

Schmid, P., Gomez-Pardo, P., Wheatley, D., Roy, P., Krabisch, P., Thill, M., Ledwidge, S., Thompson, A., Macaskill, E.J., Viehstädt, N., Purushotham, A., Gluz, O., Stefek, A., Ackerman, C., Prendergast, A., Mousa, K., Jones, L., Viale, G., Cortés, J., and Kümmel, S.

Subjects

*THERAPEUTICS

Published

2021

24. 123MO BARBICAN: A randomized, phase II study to determine the contribution of ipatasertib to neoadjuvant chemotherapy plus atezolizumab in women with triple-negative breast cancer.

Author

Schmid, P., Bofill, F.J. Salvador, Bermejo, B., Phillips, M., Wheatley, D., Neus, F., Schem, C., Stradella, A., Mele, M., Salgado, A. Cortes, Quiroga, V., Torres, A. Antón, Cussac, A. Llombart, Zamora, E., Viale, G., Kuemmel, S., Prendergast, A., Mousa, K., Gluz, O., and Cortés, J.

Subjects

*TRIPLE-negative breast cancer, *BREAST cancer, *ATEZOLIZUMAB, *NEOADJUVANT chemotherapy

Published

2021

25. 311P Pooled-analysis of prospective observational studies evaluated the effectiveness and safety of bevacizumab and paclitaxel as the first-line chemotherapy for HER2-negative metastatic breast cancer.

Author

Yamashiro, H., Yamamoto, Y., Schneeweiss, A., Müller, V., Gluz, O., Klare, P., Aktas, B., Magdolna, D., Büdi, L., Pikó, B., Mangel, L., Toi, M., Morita, S., and Ohno, S.

Subjects

*METASTATIC breast cancer, *BEVACIZUMAB, *PACLITAXEL, *SCIENTIFIC observation, *CANCER chemotherapy

Published

2020

26. 172P Gene expression in early breast cancer (EBC) patients (pts) with relapse despite pathologic complete response (pCR): An intra- and interindividual (matched control) analysis.

Author

Bruzas, S., Kümmel, S., Harbeck, N., Schmid, P., Cortés, J., Seiberling, C., Chiari, O., Harrach, H., Ataseven, B., Dyson, M., Traut, E., Theuerkauf, I., Gebauer, D., Gluz, O., and Reinisch, M.

Subjects

*BREAST cancer, *GENE expression

Published

2020

27. 164MO Impaired Ki67 response towards neoadjuvant endocrine therapy in luminal breast cancer is associated with mutations conferring endocrine resistance: WSG-ADAPT HR+/HER2- translational results.

Author

Grote, I., Bartels, S., Kandt, L., Bollmann, L., Christgen, H., Gronewold, M., Gluz, O., Nitz, U., Kümmel, S., Braun, M., Aktas, B., Grischke, E-M., Schumacher, C., Lüdtke-Heckenkamp, K., Kates, R., Wuerstlein, R., Gräser, M., Harbeck, N., Christgen, M., and Kreipe, H.

Subjects

*BREAST cancer, *HORMONE therapy, *METASTATIC breast cancer, *HORMONE receptor positive breast cancer, *ENTEROENDOCRINE cells

Published

2020

28. 206P Protroca: A non-interventional study on prophylaxis of chemotherapy induced neutropenia using lipegfilgrastim in non-selected breast cancer patients.

Author

Wuerstlein, R, Harbeck, N, Grischke, E-M, Forstmeyer, D, Schumann, R von, Krabisch, P, Nitz, U, Gluz, O, Kates, R E, and Graeser, M

Subjects

*BREAST cancer patients, *CANCER chemotherapy, *MEDICAL sciences, *WOMEN'S hospitals, *CANCER

Published

2019

29. 260 Primary Tumor in Breast Cancer and Its Phenotype in Positive Lymph Nodes and Later Disease Recurrence (metastatic Breast Cancer): Results of the PRIMET-trial (WSG/DETECT)

Author

Wuerstlein, R., Freudenberger, M., Wildenburg, L., Ortmann, M., Liedtke, C., Gluz, O., Kates, R., Fehm, T., Nitz, U., and Harbeck, N.

Published

2012

30. 5177 POSTER Correlation Between PARP-1 Expression and ln-vitro Chemotherapy Sensitivity in Patients With Breast Cancer

Author

Liedtke, C., Packeisen, J., Denkert, C., Gluz, O., Tio, J., Kiesel, L., Vogt, U., Müller, B., Hess, K.R., and Bürger, H.

Published

2011