Poster lunch

1454 - 70-gene signature, an encouraging prognostic tool to guide adjuvant therapy in Early Breast Cancer. (87P)

Date

18 Nov 2017

Session

Poster lunch

Presenters

Alberto Cunquero Tomas

Citation

Annals of Oncology (2017) 28 (suppl_10): x16-x24. 10.1093/annonc/mdx655

Authors

A. Cunquero Tomas¹, C. Avila Andrade², A.B. Fernandez Diaz², M. Meri Abad², I. Shaheen³, L. Condori Farfan², A. Rodriguez Huaman², V. Sforza¹, F.D.A. Aparisi Aparisi¹, M.J. Safont Aguilera², A. Blasco Cordellat², M. Gil Raga¹, C. Caballero Diaz¹, A. Berrocal², M.C. Godes Sanz de Bremond¹, A. Pérez⁴, V. Iranzo Gonzalez-Cruz², C. Camps Herrero²

Author affiliations

¹ Medical Oncology, Consorcio Hospital General Universitario Valencia, 46014 - Valencia/ES
² Medical Oncology, General University Hospital of Valencia, 46014 - VALENCIA/ES
³ Medical Oncology, Hospital General Universitario Valencia, 46018 - Valencia/ES
⁴ Pathology, Consorcio Hospital General Universitario Valencia, 46014 - Valencia/ES

Resources

Abstract 1454

Background

Prognosis of early breast cancer (EBC) after surgery seems to be tied to both clinical and molecular features. Based on this, the addition of adjuvant chemotherapy (ACT) in ER+ HER2-, moderately differentiated, low ER expression or moderate tumor burden EBC is made, assuming a predictive role of these features in ACT benefit. There are patients who, based on these data, could abstain ACT without an increase in the risk of early relapse or decrease in survival. It is in these patients that molecular platforms, either 70-gene (Mammaprint®) or 21-gene (OncotypeDx®) signatures, combined with clinical features, would help decision making, sparing toxicities to these patients.

Methods

We analyzed 89 of 850 first visits (2014/17) with ER+ HER2- EBC,

Results

Mean 57 year-old patients at diagnosis, 60% postmenopausal. 53% Luminal B, all Luminal type by Blueprint®. 79% T1 and 16% N1mic. Bad prognosis encouraging ACT in 57% and 33% of patients based on clinical and statistical characteristics, respectively. 36% ACT indication on molecular basis, 25% of reduction of ACT indication. In subgroup analysis, 55% of high-risk patients according to clinical criteria were low-risk Mammaprint, with 33% who went from low to high risk of relapse. This implies a 20% decrease in chemotherapy treatments. In addition, 2 or more clinical risk factors may predict a high-risk result in the 70-gene signature assay, with likeliness of poor prognosis and ACT potential benefit. With a median follow-up of 15 months, no relapses have been noticed.

Conclusions

Prognosis based on clinically significant reduction of the indication of ACT (around 25%) without affecting the rate of relapse has been noticed, with data suggesting prediction of gene-signature assay results according to the number of clinical risk factor present. A longer follow-up time and a larger number of patients are needed to confirm these results.

Clinical trial identification

Legal entity responsible for the study

Consorcio Hospital General Universitario Valencia

Funding

None

Disclosure

All authors have declared no conflicts of interest.