Ensemble‐based classification using microRNA expression identifies a breast cancer patient subgroup with an ultralow long‐term risk of metastases

Author:

Block Ines1ORCID,Burton Mark123,Sørensen Kristina P.1,Larsen Martin J.12,Do Thi T. N.12,Bak Martin45,Cold Søren6,Thomassen Mads123,Tan Qihua237,Kruse Torben A.123ORCID

Affiliation:

1. Department of Clinical Genetics Odense University Hospital Odense Denmark

2. Human Genetics, Department of Clinical Research University of Southern Denmark Odense Denmark

3. Clinical Genome Center University of Southern Denmark and Region of Southern Denmark Odense Denmark

4. Department of Pathology Odense University Hospital Odense Denmark

5. Department of Pathology Hospital of Southwest Jutland Esbjerg Denmark

6. Department of Oncology Odense University Hospital Odense Denmark

7. Epidemiology, Department of Public Health University of Southern Denmark Odense Denmark

Abstract

AbstractBackgroundCurrent clinical markers overestimate the recurrence risk in many lymph node negative (LNN) breast cancer (BC) patients such that a majority of these low‐risk patients unnecessarily receive systemic treatments. We tested if differential microRNA expression in primary tumors allows reliable identification of indolent LNN BC patients to provide an improved classification tool for overtreatment reduction in this patient group.MethodsWe collected freshly frozen primary tumors of 80 LNN BC patients with recurrence and 80 recurrence‐free patients (mean follow‐up: 20.9 years). The study comprises solely systemically untreated patients to exclude that administered treatments confound the metastasis status. Samples were pairwise matched for clinical‐pathological characteristics to minimize dependence of current markers. Patients were classified into risk‐subgroups according to the differential microRNA expression of their tumors via classification model building with cross‐validation using seven classification methods and a voting scheme. The methodology was validated using available data of two independent cohorts (n = 123, n = 339).ResultsOf the 80 indolent patients (who would all likely receive systemic treatments today) our ultralow‐risk classifier correctly identified 37 while keeping a sensitivity of 100% in the recurrence group. Multivariable logistic regression analysis confirmed independence of voting results from current clinical markers. Application of the method in two validation cohorts confirmed successful classification of ultralow‐risk BC patients with significantly prolonged recurrence‐free survival.ConclusionProfiles of differential microRNAs expression can identify LNN BC patients who could spare systemic treatments demanded by currently applied classifications. However, further validation studies are required for clinical implementation of the applied methodology.

Funder

Syddansk Universitet

Kræftens Bekæmpelse

Dansk Kræftforsknings Fond

Natur og Univers, Det Frie Forskningsråd

Lundbeck Foundation

Frimodt-Heineke Fonden

Breast Friends

Fonden til Lægevidenskabens Fremme

Harboefonden

Publisher

Wiley

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