Reducing chemotherapy use in clinically high-risk, genomically low-risk pN0 and pN1 early breast cancer patients: five-year data from the prospective, randomised phase 3 West German Study Group (WSG) PlanB trial

Ulrike Nitz; Oleg Gluz; Matthias Christgen; Ronald Kates; Michael Clemens; Wolfram Malter; Benno Nuding; Bahriye Aktas; Sherko Küemmel; Toralf Reimer; Andrea Stefek; Fatemeh Lorenz-Salehi; Petra Krabisch; Marianne Just; Doris Augustin; Cornelia Liedtke; Calvin Chao; Steven Shak; Rachel Wuerstlein; Hans Kreipe; Nadia Harbeck

doi:10.1007/s10549-017-4358-6

Reducing chemotherapy use in clinically high-risk, genomically low-risk pN0 and pN1 early breast cancer patients: five-year data from the prospective, randomised phase 3 West German Study Group (WSG) PlanB trial

Ulrike Nitz(Deutsches Archäologisches Institut, Zentrale), Oleg Gluz(Bethesda Hospital), Matthias Christgen(Medizinische Hochschule Hannover), Ronald Kates(Deutsches Archäologisches Institut, Zentrale), Michael Clemens(Klinikum Mutterhaus der Borromäerinnen), Wolfram Malter, Benno Nuding(Federal Highway and Transport Research Institute), Bahriye Aktas(Essen University Hospital), Sherko Küemmel(Kliniken Essen-Mitte), Toralf Reimer(Klinikum Südstadt Rostock), Andrea Stefek(Die Johanniter), Fatemeh Lorenz-Salehi(Helios Dr. Horst Schmidt Kliniken Wiesbaden), Petra Krabisch(Klinikum Chemnitz), Marianne Just(Klinikum Bielefeld), Doris Augustin, Cornelia Liedtke(Deutsches Archäologisches Institut, Zentrale), Calvin Chao(Genomic Health (United States)), Steven Shak(Genomic Health (United States)), Rachel Wuerstlein(Deutsches Archäologisches Institut, Zentrale), Hans Kreipe(Medizinische Hochschule Hannover), Nadia Harbeck(Deutsches Archäologisches Institut, Zentrale)

Breast Cancer Research and Treatment

June 29, 2017

10.1007/s10549-017-4358-6

Cited by 189Open Access

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Abstract

BACKGROUND: (RS) to define a genomically low-risk subset of clinically high-risk pN0-1 early breast cancer (EBC) patients for treatment with adjuvant endocrine therapy (ET) alone. Here, we report five-year data evaluating the prognostic value of RS, Ki-67, and other traditional clinicopathological parameters. METHODS: A central tumour bank was prospectively established within PlanB. Following an early amendment, hormone receptor (HR)+ , pN0-1 RS ≤ 11 patients were recommended to omit chemotherapy. Patients with RS ≥ 12, pN2-3, or HR-negative/HER2-negative disease were randomised to anthracycline-containing or anthracycline-free chemotherapy. Primary endpoint: disease-free survival (DFS). PlanB Clinicaltrials.gov identifier: NCT01049425. FINDINGS: From 2009 to 2011, PlanB enrolled 3198 patients (central tumour bank, n = 3073) with the median age of 56 years, 41.1% pN+, and 32.5% grade 3 EBC. Chemotherapy was omitted in 348/404 (86.1%) eligible RS ≤ 11 patients. After 55 months of median follow-up, five-year DFS in ET-treated RS ≤ 11 patients was 94% (in both pN0 and pN1) versus 94% (RS 12-25) and 84% (RS > 25) in chemotherapy-treated patients (p < 0.001); five-year overall survival (OS) was 99 versus 97% and 93%, respectively (p < 0.001). Nodal status, central/local grade, tumour size, continuous Ki-67, progesterone receptor (PR), IHC4, and RS were univariate prognostic factors for DFS. In a multivariate analysis including all univariate prognostic markers, only pN2-3, central and local grade 3, tumour size >2 cm, and RS, but not IHC4 or Ki-67 were independent adverse factors. If RS was excluded, IHC4 or both Ki-67 and PR entered the model. The impact of RS was particularly pronounced in patients with intermediate Ki-67 (>10%, <40%) tumours. INTERPRETATION: The excellent five-year outcomes in clinically high-risk, genomically low-risk (RS ≤ 11) pN0-1 patients without adjuvant chemotherapy support using RS with standardised pathology for treatment decisions in HR+ HER2-negative EBC. Ki-67 has the potential to support patient selection for genomic testing.

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