Comprehensive Analysis of Spatial, Temporal and Molecular Patterns of Ribociclib Efficacy and Resistance in Advanced Breast Cancer Patients (CAPTOR-BC)

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ClinicalTrials.gov Identifier: NCT05452213

Recruitment Status : Recruiting

First Posted : July 11, 2022

Last Update Posted : April 18, 2023

See Contacts and Locations

View this study on the modernized ClinicalTrials.gov

Sponsor:

Collaborators:

AGO Breast Study Group e.V.

Novartis Pharmaceuticals

Information provided by (Responsible Party):

Institut fuer Frauengesundheit

Study Description

Brief Summary:

This is a single-arm, open-label phase IV study of patients with advanced HR+/HER2- breast cancer who are treated first line with ribociclib and standard of care endocrine treatment according to SmPC.

Condition or disease	Intervention/treatment	Phase
Breast Cancer Breast Neoplasms Breast Neoplasm Female Breast Cancer Female HER2-negative Breast Cancer Hormone Receptor-positive Breast Cancer Advanced Breast Cancer	Drug: Ribociclib	Phase 4

Detailed Description:

This is a prospective, multicenter, phase IV, one-arm, open-label clinical trial investigating patients treated with ribociclib and standard of care endocrine therapy for hormone receptor positive (HR+) / human epidermal growth factor receptor negative (HER2-) advanced breast cancer in the first therapy line. Patients eligible for this trial will receive on-label ribociclib according to Summary of Product Characteristics (SmPC) and as well as the specified inclusion/exclusion criteria.

The survival rates for progression-free survival (PFS) and overall survival (OS) at month 12 are the co-primary objectives. Quality of life and toxicity are secondary objectives. Additionally, there is a comprehensive biomarker discovery and validation program included into the study.

A total of 1000 patients are planned to be enrolled into this trial in 75 trial sites in Germany.

Biomarkers will be evaluated before, during and after treatment or at progression. A comprehensive biospecimens sampling will be done to enable translational research projects and evaluation of potential biomarkers within circulation tumor desoxyribonucleic acid (ctDNA), circulating tumor ribonucleic acid (ctRNA), formaldehyde-fixed paraffin-embedded tissue (FFPE) tissue, Serum, Plasma and circulating immune cells

Study Design

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Study Type :	Interventional (Clinical Trial)
Estimated Enrollment :	1000 participants
Allocation:	N/A
Intervention Model:	Single Group Assignment
Intervention Model Description:	One-arm, open-label
Masking:	None (Open Label)
Primary Purpose:	Treatment
Official Title:	CAPTOR-BC: Comprehensive Analysis of Spatial, Temporal and Molecular Patterns of Ribociclib Efficacy and Resistance in Advanced Breast Cancer Patients
Actual Study Start Date :	October 12, 2022
Estimated Primary Completion Date :	October 2024
Estimated Study Completion Date :	October 2026

Resource links provided by the National Library of Medicine

MedlinePlus Genetics related topics: Breast cancer

MedlinePlus related topics: Breast Cancer

Drug Information available for: Ribociclib

U.S. FDA Resources

Arms and Interventions

Arm	Intervention/treatment
Experimental: Ribociclib	Drug: Ribociclib All patients will receive ribociclib in combination with standard endocrine therapy according to the current SmPC and local in-house standard. Ribociclib will be administered once daily for 21 consecutive days followed by 7 days off treatment (28-day cycle). The daily dose is 600 mg/day. Ribociclib and standard of care endocrine treatment will be prescribed and administered according to investigator's discretion.

Arm

Intervention/treatment

Experimental: Ribociclib

Drug: Ribociclib

All patients will receive ribociclib in combination with standard endocrine therapy according to the current SmPC and local in-house standard.

Ribociclib will be administered once daily for 21 consecutive days followed by 7 days off treatment (28-day cycle). The daily dose is 600 mg/day.

Ribociclib and standard of care endocrine treatment will be prescribed and administered according to investigator's discretion.

Outcome Measures

Primary Outcome Measures :

12-month PFS rate [ Time Frame: 12 months ]
The rate for progression-free survival at month 12 will be calculated.
12-month OS rate [ Time Frame: 12 months ]
The rate for overall survival at month 12 will be calculated.

Secondary Outcome Measures :

24-month PFS rate [ Time Frame: 24 months ]
The rate for progression-free survival at month 24 will be calculated.
24-month OS rate [ Time Frame: 24 months ]
The rate for overall survival at month 24 will be calculated.
36-month PFS rate [ Time Frame: 36 months ]
The rate for progression-free survival at month 36 will be calculated.
36-month OS rate [ Time Frame: 36 months ]
The rate for overall survival at month 36 will be calculated.
Median progression-free survival [ Time Frame: From date of enrollment until first documented progression or date of death from any cause or regular end of study (up to 24 months) whichever is first. ]
Median progression-free survival will be estimated if achieved at the end of study
Median overall survival [ Time Frame: From date of enrollment until date of death from any cause or regular end of study (up to 24 months) whichever is first. ]
Median overall survival will be estimated if achieved at the end of study
Health related quality of life (FACT-G) [ Time Frame: Collected before start of trial treatment, at 3 months and every 6 months afterwards until end of study up to 24 months ]
Health related quality of life as assessed by FACT-G questionnaire (Functional Assessment of Cancer Therapy - General) Min 0, Max 108, The higher the score, the better the QoL.
Health related quality of life (FACT-B) [ Time Frame: Collected before start of trial treatment, at 3 months and every 6 months afterwards until end of study up to 24 months ]
Health related quality of life as assessed by FACT-B questionnaire (Functional Assessment of Cancer Therapy - Breast Cancer) Min 0, Max 148, The higher the score, the better the QoL.
Number of participants with treatment-related adverse events as assessed by CTCAE v5.0 [ Time Frame: All adverse events will be recorded from signing informed consent through 30 days following cessation of treatment or until the last study visit ]
The safety endpoints for the study will include rate of adverse events (AE), serious adverse events (SAEs) and fatal SAEs, causality and outcome of AE/SAEs, rate of treatment discontinuations and reasons, Changes in vital signs, laboratory values etc. Grading of AE/SAEs will be based on NCI CTCAE v5.0.

Other Outcome Measures:

Correlation of genome wide genetic biomarkers with progression-free survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide genetic biomarkers with overall survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide genetic biomarkers with quality of life [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide genetic biomarkers with ribociclib side effects [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide gene expression biomarkers with progression-free survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide gene expression biomarkers with overall survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide gene expression biomarkers with quality of life [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide gene expression biomarkers with ribociclib side effects [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Genome wide genetic biomarkers will be assessed by whole genome sequencing and/ or panel sequencing from blood samples.
Correlation of genome wide tumor mutational patterns assessed from formalin-fixed paraffin embedded tumor material with progression-free survival [ Time Frame: Measured from biomaterial collected at baseline and at the time of tumor progression ]
Tumor DNA will be either isolated from FFPE tissue (primary tumor or metastasis) or from Plasma samples (STRECK cfDNA Tube). DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from formalin-fixed paraffin embedded tumor material with overall survival [ Time Frame: Measured from biomaterial collected at baseline and at the time of tumor progression ]
Tumor DNA will be either isolated from FFPE tissue (primary tumor or metastasis) or from Plasma samples (STRECK cfDNA Tube). DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from formalin-fixed paraffin embedded tumor material with quality of life [ Time Frame: Measured from biomaterial collected at baseline and at the time of tumor progression ]
Tumor DNA will be either isolated from FFPE tissue (primary tumor or metastasis) or from Plasma samples (STRECK cfDNA Tube). DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from formalin-fixed paraffin embedded tumor material with ribociclib side effects [ Time Frame: Measured from biomaterial collected at baseline and at the time of tumor progression ]
Tumor DNA will be either isolated from FFPE tissue (primary tumor or metastasis) or from Plasma samples (STRECK cfDNA Tube). DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from ctDNA biomarkers with progression-free survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from ctDNA biomarkers with overall survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from ctDNA biomarkers with quality of life [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of genome wide tumor mutational patterns assessed from ctDNA biomarkers with ribociclib side effects [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of changes in the genome wide tumor mutational patterns assessed from ctDNA biomarkers with progression-free survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of changes in the genome wide tumor mutational patterns assessed from ctDNA biomarkers with overall survival [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of changes in the genome wide tumor mutational patterns assessed from ctDNA biomarkers with quality of life [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.
Correlation of changes in the genome wide tumor mutational patterns assessed from ctDNA biomarkers with ribociclib side effects [ Time Frame: Measured from biomaterial collected at baseline, 2 weeks, 3 months, 6 months, 12 months, 18 months or at the end of treatment in case treatment is stopped irregularly. ]
Germline DNA will be isolated from one EDTA blood samples obtained within the study. DNA will be analyzed by whole genome sequencing and/or panel sequencing.

Eligibility Criteria

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Ages Eligible for Study:	18 Years and older (Adult, Older Adult)
Sexes Eligible for Study:	Female
Accepts Healthy Volunteers:	No

Criteria

Inclusion Criteria:

Indication for treatment with ribociclib in combination with endocrine therapy in the locally advanced or 1st line metastatic therapy setting according to SmPC. (Previous treatment with cycline dependent kinase 4/6 (CDK4/6) inhibitors is allowed in the adjuvant setting)
Written informed consent prior to beginning of trial specific procedures
Subject must be female and aged ≥ 18 years on the day of signing informed consent
Locally advanced or metastatic breast cancer not amenable to curative treatment
Patient has HER2-negative breast cancer confirmed by local laboratory defined as a negative in situ hybridization test or an immunohistochemistry (IHC) status of 0 or 1+. If IHC is 2+, a negative in situ hybridization (FISH, CISH, or SISH) test is required to confirm the HER2-negative status (based on the most recently analyzed tissue sample tested by a local laboratory
Histologically confirmed estrogen receptor (ER) positive and/ or progesterone receptor (PgR) positive breast cancer determined by core biopsy according to local in-house standard.
corrected QT (QTcF) interval < 450 ms
Adequate organ function amenable for treatment with ribociclib as assessed by local laboratory
Women of childbearing potential must have a negative urine or serum pregnancy test within 72 h prior to study entry and be willing to use highly effective method of contraception for course of the trial through 21 days after the last dose of trial treatment.
Patient must be willing and able to comply with scheduled visits, treatment plans, laboratory tests, and other trial procedures.

Exclusion Criteria:

Concurrent participation in a study with an investigational agent/device or within 14 days of study entry or 5 half-lives of the respective investigational agent/device, whichever is longer
Patients who are not treated for advanced HR+, HER2- breast cancer in the first line therapy setting.
Patient not eligible for treatment with ribociclib according to SmPC or investigator's discretion
Patients who are pregnant or lactating.
Patients with existing or patients who are at significant risk of developing corrected QT interval (QTc) prolongation. This includes
- patients with long QT syndrome
- uncontrolled or significant cardiac disease, including recent myocardial infarction, congestive heart failure, unstable angina and bradyarrhythmia
- electrolyte abnormalities
Patients with known hypersensitivity to the active substance of ribociclib, soya, peanut or any other of the excipients of ribociclib.
Patients with active systemic infections (for example, bacterial infection requiring intravenous antibiotics at time of initiating study treatment, fungal infection, or detectable viral infection requiring systemic therapy) or viral load (such as known human immunodeficiency virus positivity or with known active hepatitis B or C, for example, hepatitis B surface antigen positive).
Patients with serious preexisting medical condition(s) that, in the judgment of the investigator, would preclude participation in this study (such as severe renal impairment, interstitial lung disease, severe dyspnea at rest or requiring oxygen therapy, history of major surgical resection involving the stomach or small bowel, or preexisting Crohn's disease or ulcerative colitis or a preexisting chronic condition resulting in clinically significant diarrhea).
Patient who do not agree to collection of biospecimens samples (blood, stool, tissue)

Contacts and Locations

Information from the National Library of Medicine

To learn more about this study, you or your doctor may contact the study research staff using the contact information provided by the sponsor.

Please refer to this study by its ClinicalTrials.gov identifier (NCT number): NCT05452213

Contacts

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Contact: CAPTOR Study Manager	09131 9278638	captor@ifg-erlangen.de

Locations

Show 52 study locations

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Germany
Department of Gynecology and Obstetrics, Erlangen University Hospital	Recruiting
Erlangen, Bavaria, Germany, 91054
Contact: Peter A Fasching, MD, Prof. +49 9131 8543470 peter.fasching@uk-erlangen.de
Department of Gynecology and Obstetrics, University Medicine Mainz	Recruiting
Mainz, Hesse, Germany, 55131
Contact: Marcus Schmidt, MD, Prof. +49 6131 176884 marcus.schmidt@unimedizin-mainz.de
Department for Gynecology and Obstetrics, Marienhospital Bottrop gGmbH	Recruiting
Bottrop, North Rhine-Westphalia, Germany, 46236
Contact: Hans-Christian Kolberg, MD +49 2041 1061601 hans-christian.kolberg@mhb-bottrop.de
Klinikum St Marien Amberg	Recruiting
Amberg, Germany, 92224
Contact: Tanja H Haunzenberger, MD +499621381381 haunzenberger.tanja@klinikum-amberg.de
Onkologie Aschaffenburg, Hämato-Onkologische Schwerpunktpraxis am Klinikum Aschaffenburg	Recruiting
Aschaffenburg, Germany, 63739
Contact: Manfred Welslau, MD manfred.welslau@klinikum-ab-alz.de
Klinik für Hämatologie und Onkologie, Uniklinik Augsburg	Not yet recruiting
Augsburg, Germany, 86156
Contact: Frank Jordan, MD Frank.Jordan@uk-augsburg.de
University Hospital Augsburg	Recruiting
Augsburg, Germany, 86156
Contact: Nina Ditsch, MD, Prof. +498214002208 nina.ditsch@uk-augsburg.de
Frauenklinik des Klinikums Bamberg	Not yet recruiting
Bamberg, Germany, 96049
Contact: Denise Wrobel, MD studienzentrale@sozialstiftung-bamberg.de
MediOnko GbR	Not yet recruiting
Berlin, Germany, 10367
Contact: Gülten Oskay-Özcelik, MD studienoskay@medionko.de
HELIOS Klinikum Berlin-Buch	Not yet recruiting
Berlin, Germany, 13125
Contact: Michael Untch, MD michael.untch@helios-gesundheit.de
Zentrum für ambulante Hämatologie und Onkologie (ZAHO) an der Robert-Janker-Klinik	Not yet recruiting
Bonn, Germany, 53129
Contact: Martin Esser, MD messer@zaho-rheinland.de
Klinik für Gynäkologie, Gynäkoonkologie und Senologie Klinikum Bremen-Mitte	Not yet recruiting
Bremen, Germany, 28205
Contact: Mustafa Aydogdu, MD studien_kbm_gyn@gesundheitnord.de
Klinikum Chemnitz gGmbH, Klinik für Frauenheilkunde und Geburtshilfe	Not yet recruiting
Chemnitz, Germany, 09116
Contact: Petra Krabisch, MD p.krabisch@skc.de
Kliniken Der Stadt Köln gGmbH	Recruiting
Cologne, Germany, 51067
Contact: Myriam EM Vincent +4922189076700 vincentm@kliniken-koeln.de
Carl-Thiem-Klinikum Cottbus	Recruiting
Cottbus, Germany, 03048
Contact: Nikola Bangemann, MD N.Bangemann@ctk.de
Staedtisches Klinikum Dessau, Gynecology and Obstetrics	Recruiting
Dessau, Germany, 06847
Contact: Hermann Voß, MD +493405014310 hermann.voss@klinikum-dessau.de
Universitäts-Frauenklinik Carl Gustav Carus Universität Dresden	Not yet recruiting
Dresden, Germany, 01307
Contact: Pauline Wimberger, MD pauline.wimberger@uniklinikum-dresden.de
Universitaetsklinikum Duesseldorf AöR	Recruiting
Duesseldorf, Germany, 40225
Contact: Tanja Fehm, MD, Prof. +492118117501 direktion.frauenklinik@med.uni-duesseldorf.de
Universitaetsklinikum Essen AöR, Gynecology and Obstetrics	Not yet recruiting
Essen, Germany, 45147
Contact: Oliver Hoffmann, MD +492017232575 oliver.hoffmann@uk-essen.de
Klinikum Esslingen GmbH	Not yet recruiting
Esslingen, Germany, 73730
Contact: Alexander Hein, MD a.hein.cto@klinikum-esslingen.de
Agaplesion Frankfurter Diakonie Kliniken gGmbH, Gynecology and Obstetrics	Not yet recruiting
Frankfurt Am Main, Germany, 60431
Contact: Marc AM Thill, MD, Prof. +496995332228 marc.thill@agaplesion.de
Universitäts-Frauenklinik Frankfurt	Not yet recruiting
Frankfurt am Main, Germany, 60596
Contact: Christine Solbach, MD Christine.Solbach@kgu.de
Universitäts-Frauenklinik Freiburg	Not yet recruiting
Freiburg, Germany, 79106
Contact: Ingolf Juhasz-Böss, MD ingolf.juhasz-boess@uniklinik-freiburg.de
Medizinisches Versorgungszentrum Onkologie Georgsmarienhütte und Bramsche	Recruiting
Georgsmarienhütte, Germany, 49124
Contact: Kerstin Lüdtke-Heckenkamp, MD kerstin.luedtke-heckenkamp@niels-stensen-kliniken.de
Universitäts-Frauenklinik Hamburg-Eppendorf	Not yet recruiting
Hamburg, Germany, 20246
Contact: Volkmar Müller, MD v.mueller@uke.de
Mammazentrum Hamburg am Krankenhaus Jerusalem	Not yet recruiting
Hamburg, Germany, 20357
Contact: Christian Schem, MD schem@mammazentrum-hamburg.de
Nationales Centrum für Tumorerkrankungen, Universitätsklinikum Heidelberg Abteilung für Gynäkologie und Geburtshilfe	Recruiting
Heidelberg, Germany, 69120
Contact: Andreas Schneeweiss, MD Andreas.Schneeweiss@med.uni-heidelberg.de
Frauenklinik, SLK-Kliniken Heilbronn GmbH	Recruiting
Heilbronn, Germany, 74078
Contact: Nikolaus De Gregorio, MD nikolaus.degregorio@slk-kliniken.de
Staedtisches Klinikum Karlsruhe gGmbH, Gynecology and Obstetrics	Recruiting
Karlsruhe, Germany, 76133
Contact: Gariele Kaltenecker, MD +4972197462406 gabriele.kaltenecker@klinikum-karlsruhe.de
University Medical Centre Schleswig-Holstein, Gynecology and Obstetrics	Recruiting
Kiel, Germany, 24105
Contact: Marion van Mackelenbergh, MD +4943150021410 marion.vanmackelenbergh@uksh.de
ZAGO-Zentrum für ambulante gynäkologische Onkologie	Recruiting
Krefeld, Germany, 47805
Contact: Gunther M Rogmans, MD +492151322969 rogmans.gunther@gmail.com
Klinikum Kulmbach	Recruiting
Kulmbach, Germany, 95326
Contact: Benno Lex, MD +499221981901 benno.lex@klinikum-kulmbach.de
VK&K Studienzentrum Landshut am Lakumed Klinikum Landshut-Achdorf	Not yet recruiting
Landshut, Germany, 84036
Contact: Ursula Vehling-Kaiser, MD dr.vk@vehling-kaiser.de
Praxis Dr. Müller MVM GmbH, Studienzentrum UnterEms	Not yet recruiting
Leer, Germany, 26789
Contact: Lothar Müller, MD lothar.mueller@onkologie-ue.de
Universitäts-Frauenklinik Leipzig	Not yet recruiting
Leipzig, Germany, 04103
Contact: Bahriye Aktas, MD Bahriye.Aktas@medizin.uni-leipzig.de
Hämatologie Onkologie Gemeinschaftspraxis Pasing	Recruiting
Munich, Germany, 81241
Contact: Matthias Zingerle, MD zingerle@onkologie-pasing.de
Ev. Krankenhaus Bethesda Mönchengladbach	Not yet recruiting
Mönchengladbach, Germany, 41061
Contact: Iris Scheffen, MD iris.scheffen@wsg-online.com
MVZ Nordhausen gGmbH	Recruiting
Nordhausen, Germany, 99734
Contact: Andrea Grafe, MD andrea.grafe@shk-ndh.de
Klinikum Nürnberg	Not yet recruiting
Nuremberg, Germany, 90419
Contact: Christine Zeder-Göß, MD +499113983843 christine.zeder-goess@klinikum-nuernberg.de
Frauenklinik, Medius Klinik Nürtingen	Recruiting
Nürtingen, Germany, 72622
Contact: Elke Faust, MD e.faust@medius-kliniken.de
Gemeinschaftspraxis für Hämatologie und Onkologie GbR	Recruiting
Ravensburg, Germany, 88212
Contact: Thomas Decker, MD thomas.decker@onkonet.eu
Frauenklinik, Diakoniekrankenhaus Rotenburg	Recruiting
Rotenburg, Germany, 27356
Contact: Tobias Hesse, MD hesse@diako-online.de
Leopoldina Krankenhaus der Stadt Schweinfurt gGmbH	Recruiting
Schweinfurt, Germany, 97422
Contact: Michael Weigel, MD mweigel@leopoldina.de
Schwerpunktpraxis für Hämatologie, Onkologie und Magen-Darm Diagnostik	Recruiting
Singen, Germany, 78224
Contact: Thomas Fietz, MD studie@onkologie-bodensee.de
Onkologische Schwerpunktpraxis Speyer	Recruiting
Speyer, Germany, 61346
Contact: Gregor Bolz, MD g.bolz@onkologie-speyer.de
Klinikum Stuttgart	Not yet recruiting
Stuttgart, Germany, 70174
Contact: Ulrich Karck, MD u.karck@klinikum-stuttgart.de
Onkologie Rheinsieg, Praxisnetzwerk Hämatologie und internistische Onkologie	Not yet recruiting
Troisdorf, Germany, 53840
Contact: Ernst Rodermann, MD rodermann@onkologie-rheinsieg.de
Universitaetsklinikum Tuebingen	Recruiting
Tuebingen, Germany, 72076
Contact: Eva-Maria Grischke, MD, Prof. +4970712982211 eva-maria.grischke@med.uni-tuebingen.de
Universitäts-Frauenklinik Ulm	Not yet recruiting
Ulm, Germany, 89075
Contact: Brigitte Rack, MD Studienzentrale.UFK@uniklinik-ulm.de
MVZ Nordoberpfalz	Not yet recruiting
Weiden, Germany, 92637
Contact: Robert Funck, MD robert.funck@mvz-weiden.de
Medizinische Studiengesellschaft Nord-West GmbH	Recruiting
Westerstede, Germany, 26655
Contact: Jan Janssen, MD
Rems-Murr Kliniken Winnenden	Recruiting
Winnenden, Germany, 71364
Contact: Hans-Joachim Strittmatter, MD ans-joachim.strittmatter@rems-murr-kliniken.de

Sponsors and Collaborators

Institut fuer Frauengesundheit

AGO Breast Study Group e.V.

Novartis Pharmaceuticals

Investigators

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Study Chair:	Peter A. Fasching, MD, Prof.	Department of Gynecology and Obstetrics, Erlangen University Hospital
Study Chair:	Tanja Fehm, MD, Prof.	Department of Gynecology/Obstetrics \|University Hospital Düsseldorf, Germany
Study Chair:	Andreas Schneeweiss, MD, Prof.	National Center for Tumor Diseases (NCT) \| Heidelberg University Hospital and German Cancer Research Center

More Information

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Responsible Party:	Institut fuer Frauengesundheit
ClinicalTrials.gov Identifier:	NCT05452213
Other Study ID Numbers:	IFG-01-2022
First Posted:	July 11, 2022 Key Record Dates
Last Update Posted:	April 18, 2023
Last Verified:	April 2023
Individual Participant Data (IPD) Sharing Statement:
Plan to Share IPD:	No

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Studies a U.S. FDA-regulated Drug Product:	No
Studies a U.S. FDA-regulated Device Product:	No

Additional relevant MeSH terms:

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Breast Neoplasms Neoplasms Neoplasms by Site Breast Diseases Skin Diseases

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