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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT00798070
Other study ID # PANTHER SBG2004-1
Secondary ID 2007-002061-12IS
Status Active, not recruiting
Phase Phase 3
First received
Last updated
Start date February 2007
Est. completion date January 2022

Study information

Verified date September 2020
Source Karolinska University Hospital
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is an adjuvant, open, prospective, randomized study to compare:

A. Individually tailored and two weekly dosed epirubicin + cyclophosphamide followed by a three weeks break followed by biweekly and tailored docetaxel (dtEC→dtT) given every second week, to

B. Fixed dosed and three weekly epirubicin, cyclophosphamide and 5-fluorouracil, followed by fixed dosed and three weekly docetaxel (FEC→T).

Patients with primary node-positive or high risk lymph node negative breast cancer will be eligible for the study.

The primary objective of the phase 3 study is to compare breast cancer relapse-free survival (BCRFS) between the dtEC→dtT and FE100C→T. To detect a five-year BCRFS difference of 0.710 to 0.790 about 1000 patients per arm will be needed. They will be recruited during four years and followed another two years for breast cancer events.

Secondary objectives are to compare

1. Distant disease-free survival (DDFS)

2. Event-free survival and

3. Overall survival

4. Health-related quality of life and toxicity analyses according to CTC

5. Outcome in relation to tumour biological factors and polymorphism patterns

1. RFS in relation to the Sorlie classes using immunohistochemical markers and/or gene expression profiling comparing A vs B arm

2. RFS with receptor positive disease (analyzed in the local laboratories as described in the CRFs and also analyzed as continuous variables) in the comparison between the A- and B- arms.

3. RFS with high and low proliferation, respectively, (analyzed in the local laboratories as described in the CRFs and also analyzed as a continuous variable, or centrally analyzed), in the comparison between the A- and B-arms.

4. RFS in relation to HER-2/neu status (analyzed in the local laboratories as described in the CRFs) in the primary cancers in the comparison between the A- and B-arms and analyzed whether trastuzumab was given in sequence or concurrently.

5. RFS analyzed in relation to other molecular markers (e.g. gene expression profiling/ sequencing) in the primary cancers and SNPs signatures in normal DNA (related to toxicities for EC/FEC and docetaxel components, respectively, and given dose levels and outcome in relation to these factors and in relation QoL) to outcome per arm.

6. RFS analyzed in relation to tumour associated lymphocytes and Y-box binding protein in the comparison between the A- and B-arms.

Tumour tissue will be obtained and stored for studies of prognostication and therapy prediction.

Last patient randomized was September 2011.


Description:

Are described under the heading "Outcome measures"


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 2017
Est. completion date January 2022
Est. primary completion date April 2016
Accepts healthy volunteers No
Gender Female
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

- Histological proven invasive primary breast cancer, with at least 5 (recommended 10) removed axillary lymph nodes OR negative sentinel node biopsy performed for the node negative cohort. Interval between definitive surgery that includes axillary lymph node dissection and registration must be less than 60 days. Paraffin block from the primary tumour must be retained (not mandatory for Austrian sites). Frozen tumour tissue is strongly recommended to be stored.

- Receptor negative or positive tumours with 1 or more positive axillary lymph nodes (more than 0.2 mm) OR axillary node negative breast cancers if the primary tumour is larger than 20 mm and receptor negative (Er and Pgr with no receptor content) and being Elston grade III. In Germany high risk node negative breast cancer patients are not eligible until labelling for docetaxel includes node-negative disease.

- A primary breast cancer patient being 35 years or younger considered suitable for adjuvant chemotherapy (may be receptor negative or positive, HER-2/neu negative or positive, with or without axillary lymph node metastases).

- Macroscopically and microscopically free margins after radical surgery (no cancer cells at borders of resection).

- No proven distant metastases (negative chest/pulmonary X-ray, bone scintigram (when clinical signs of skeletal metastases or elevated ALP) supplemented with normal conventional X-ray of hot spots, normal liver function test and haematological function tests; when abnormal values, CT or ultrasound of the liver, patient can be included if no metastases are demonstrated.

- Female age 18-65.

- Ambulant patients (ECOG 1 or less).

- No major cardiovascular morbidity NYHA I or II. (Appendix 3).

- Written informed consent according to the local ethics committee requirements.

- Patients of childbearing potential should have a negative pregnancy test within seven days of registration. (In Austria, pregnancy tests have to be repeated monthly during the treatment phase).

Exclusion Criteria:

- Previous neo-adjuvant treatment.

- Non-radical surgery (histopathological positive margins).

- Proven distant metastases.

- Pregnancy or lactation.

- Other serious medical condition.

- Previous or concurrent malignancies at other sites, except basal cell carcinoma and/or squamous cell carcinoma in situ of the skin or cervix. Patients with previous breast cancer (invasive and/or ductal carcinoma in situ) in the other breast without loco-regional (large lung volumes) radiotherapy, without objective findings for relapse, with > 5 years since diagnosis can be included.

- Abnormal laboratory values precluding the possibility to safely deliver the used cytotoxic agents in the study.

- Hypersensitivity to drugs formulated in polysorbate 80.

- Peripheral neuropathy grade =2.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
dtEC?dtT
Individually tailored and two weekly dosed epirubicin (start dose 90mg/m2) + cyclophosphamide (start dose 600mg/m2) followed by a three weeks break followed by biweekly and tailored docetaxel (start dose 75mg/m2) given every second week. If toxicity measured by CTC-NCI criteria are grade 2 or less (except haematological toxicity) it will be possible to escalate doses
FEC?T
Fixed dosed and three weekly epirubicin (100mg/m2), cyclophosphamide (500mg/m2) and 5-fluorouracil (500mg/m2), followed by fixed dosed and three weekly docetaxel (100mg/m2), no dose escalations.

Locations

Country Name City State
Austria MUG - Med. Univ.-Klinik Graz Graz
Austria MUI - Univ. Klinik f. Frauenheilkunde, Innsbruck Innsbruck
Austria LKH Leoben Leoben
Austria AKH Linz Linz
Austria KH BHS Linz Linz
Austria LKH Rankweil Rankweil
Austria LKH Salzburg / PMU Salzburg
Austria KH BHB St. Veit/Glan St. Veit/Glan
Austria Klinikum Wels - Grieskirchen GmbH Wels
Austria Brustzentrum Hanusch-KH Wien
Germany Marienhospital Aachen
Germany Klinikum am Bruderwald Bamberg
Germany Klinikum Bayreuth Bayreuth
Germany HELIOS Klinikum Berlin
Germany Klinikum Bietigheim Bietigheim
Germany Klinikum Sindelfingen-Böblingen Boblingen
Germany Johanniter Krankenhaus Bonn
Germany Universitätsfrauenklinik Bonn
Germany Krankenhaus Celle Celle
Germany Klinikum Deggendorf Deggendorf
Germany Diakonissen Krankenhaus Dresden
Germany Gemeinschaftspraxis Dresden
Germany Krankenhaus St. Joseph-Stift Dresden
Germany Praxis Dr. Adhami Erkelenz
Germany Klinikum der J. W. Goethe Universität Frankfurt am Main
Germany Klinikum Frankfurt Höchst GmbH Frankfurt am Main
Germany Onkologische Gemeinschaftspraxis Frankfurt am Main
Germany Kreiskrankenhaus Freudenstadt
Germany Klinikum Fulda Fulda
Germany Onkologische Schwerpunktpraxis Goslar
Germany Krankenhaus St. Elisabeth und St. Barbara Halle
Germany Universitätsfrauenklinik Halle
Germany Klinikum Hameln Hameln
Germany Henriettenstiftung Hannover
Germany Medizinische Hochschule Hannover
Germany Universität Heidelberg Heidelberg
Germany Klinikum Heilbronn Heilbronn
Germany Gemienschaftspraxis Hildesheim
Germany Universitätsfrauenklinik Homburg
Germany St. Vincentius Kliniken Karlsruhe
Germany Städtisches Klinikum Karlsruhe
Germany Elisabeth Krankenhaus Kassel
Germany Klinikum Kempten Kempten
Germany St. Elisabeth-KKH Köln
Germany St. Vincenz Krankenhaus Limburg
Germany Onkologische Tagesklinik Lohsa
Germany Klinikum Ludwigsburg Ludwigsburg
Germany Ev. Krankenhaus Ludwigsfelde
Germany St. Vincenz und Elisabeth-Hospital Mainz
Germany Universitätsfrauenklinik Mainz
Germany Universitätsfrauenklinik Mannheim
Germany Klinikum Fichtelgebirge Marktredwitz
Germany Onkologische Praxis Memmingen
Germany Gemeinschaftspraxis Münster Münster
Germany Praxis am Klinikum Neumarkt Neumarkt
Germany Onkologische Praxis Pinneberg
Germany Klinikum am Steinenberg Reutlingen
Germany Klinikum Rheinfelden Rheinfelden
Germany Klinikum Schwerin Schwerin
Germany Gesellschaft für onkologische Studien Troisdorf
Germany Universitätsfrauenklinik Tübingen
Germany Klinikum Tuttlingen Tuttlingen
Germany Universitätsfrauenklinik Ulm
Germany Klinikum Villingen-Schwenningen Villingen
Germany Klinikum Weiden Weiden
Germany Klinikum Weinheim Weinheim
Germany Asklepios Paulinen Klinik Wiesbaden
Germany St. Josefs-Hospital Wiesbaden
Germany Stadtkrankenhaus Worms
Sweden Central Hospital Gävle
Sweden Sahlgrenska University Hospital Göteborg
Sweden Central Hospital Karlstad
Sweden Linköping University Hospital Linköping
Sweden Lund University Hospital Lund
Sweden Malmö General University Hospital Malmö
Sweden Örebro University Hospital Örebro
Sweden Karolinska University Hospital, Dept of Oncology Stockholm
Sweden Central Hospital Sundsvall
Sweden Norrlands University Hospital Umeå
Sweden Uppsala Academic Hospital Uppsala

Sponsors (4)

Lead Sponsor Collaborator
Karolinska University Hospital Austrian Breast & Colorectal Cancer Study Group, German Breast Group, Swedish Breast Cancer Group

Countries where clinical trial is conducted

Austria,  Germany,  Sweden, 

References & Publications (2)

Bergh J. Oral presentation, ASCO Annual Meeting 2016.

Foukakis T, von Minckwitz G, Bengtsson NO, Brandberg Y, Wallberg B, Fornander T, Mlineritsch B, Schmatloch S, Singer CF, Steger G, Egle D, Karlsson E, Carlsson L, Loibl S, Untch M, Hellström M, Johansson H, Anderson H, Malmström P, Gnant M, Greil R, Möbus — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Breast cancer relapse-free survival Breast cancer recurrence free survival is defined as time from randomization to the first of the events; local-, regional- or distant breast cancer recurrence or death due to breast cancer or last date of follow-up if no event has occurred. This was defined already in the phase 2 protocol (1 Sept 2004). 2 years
Secondary Distant disease-free survival Distant disease free survival is defined as time from randomization to the first of distant metastases or death due to breast cancer. 2 years
Secondary Event-free survival Event-free survival is defined as time from randomization to the first of the events breast cancer recurrence (any type), contra-lateral breast cancer, other malignancy or any cause of death. 2 years
Secondary Overall survival Overall survival is defined as time from randomization to any death. 2 years
Secondary Health-related quality of life and toxicity analyses according to CTC 2 years
Secondary Outcome in relation to tumour biological factors and polymorphism patterns Comparing arm A vs B regarding:
RFS in relation to the Sorlie classes using immunohistochemical markers and/or gene expression profiling comparing A vs B arm;
RFS with receptor positive disease in the comparison between the A- and B arms;
RFS with high and low proliferation, respectively, in the comparison between the A- and B-arms.;
RFS in relation to HER-2/neu status in the primary cancers in the comparison between the A- and B-arms and analyzed whether trastuzumab was given in sequence or concurrently;
RFS analyzed in relation to other molecular markers in the primary cancers and SNPs signatures in normal DNA to outcome per arm;
RFS analyzed in relation to tumour associated lymphocytes and Y-box binding protein in the comparison between the A- and B-arms.
Description of a to e are more detailed in the protocol, shortened here due to space limitation.
2 years
Secondary BCRFS in arm A in relation to given dose levels Breast cancer relapse free survival 2 years
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