Molecular Profiling of the Residual Disease of Triple-negative Breast Cancers After Neoadjuvant Chemotherapy Identifies Actionable Therapeutic Targets

Overview

Journal Cancer Discov

Specialty Oncology

Date 2013 Dec 21

PMID 24356096

Citations 287

Authors

Justin M Balko

Jennifer M Giltnane

Kai Wang

Luis J Schwarz

Christian D Young

Rebecca S Cook

Phillip Owens

Melinda E Sanders

Maria G Kuba

Violeta Sanchez

Richard Kurupi

Preston D Moore

Joseph A Pinto

Franco D Doimi

Henry Gomez

Dai Horiuchi

Andrei Goga

Brian D Lehmann

Joshua A Bauer

Jennifer A Pietenpol

Jeffrey S Ross

Gary A Palmer

Roman Yelensky

Maureen Cronin

Vincent A Miller

Phillip J Stephens

Carlos L Arteaga

Affiliations

Soon will be listed here.

Abstract

Unlabelled: Neoadjuvant chemotherapy (NAC) induces a pathologic complete response (pCR) in approximately 30% of patients with triple-negative breast cancers (TNBC). In patients lacking a pCR, NAC selects a subpopulation of chemotherapy-resistant tumor cells. To understand the molecular underpinnings driving treatment-resistant TNBCs, we performed comprehensive molecular analyses on the residual disease of 74 clinically defined TNBCs after NAC, including next-generation sequencing (NGS) on 20 matched pretreatment biopsies. Combined NGS and digital RNA expression analysis identified diverse molecular lesions and pathway activation in drug-resistant tumor cells. Ninety percent of the tumors contained a genetic alteration potentially treatable with a currently available targeted therapy. Thus, profiling residual TNBCs after NAC identifies targetable molecular lesions in the chemotherapy-resistant component of the tumor, which may mirror micrometastases destined to recur clinically. These data can guide biomarker-driven adjuvant studies targeting these micrometastases to improve the outcome of patients with TNBC who do not respond completely to NAC.

Significance: This study demonstrates the spectrum of genomic alterations present in residual TNBC after NAC. Because TNBCs that do not achieve a CR after NAC are likely to recur as metastatic disease at variable times after surgery, these alterations may guide the selection of targeted therapies immediately after mastectomy before these metastases become evident.

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