Clonal Hematopoiesis in Young Women Treated for Breast Cancer

Author:

Gibson Christopher J.123ORCID,Fell Geoffrey4ORCID,Sella Tal15ORCID,Sperling Adam S.1236ORCID,Snow Craig17ORCID,Rosenberg Shoshana M.8ORCID,Kirkner Greg17ORCID,Patel Ashka9ORCID,Dillon Deborah9ORCID,Bick Alexander G.10ORCID,Neuberg Donna4ORCID,Partridge Ann H.137ORCID,Miller Peter G.2311ORCID

Affiliation:

1. 1Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts.

2. 2Broad Institute of Harvard and MIT, Cambridge, Massachusetts.

3. 3Harvard Medical School, Boston, Massachusetts.

4. 4Department of Data Sciences, Dana-Farber Cancer Institute, Boston, Massachusetts.

5. 5Department of Oncology, Sheba Medical Center, Israel.

6. 6Division of Hematology, Department of Medicine, Brigham and Women's Hospital, Boston, Massachusetts.

7. 7Breast Oncology Program, Dana-Farber Brigham Cancer Center, Boston, Massachusetts.

8. 8Weill Cornell Medicine, New York, New York.

9. 9Department of Pathology, Brigham and Women's Hospital, Boston, Massachusetts.

10. 10Division of Genetic Medicine, Department of Medicine, Vanderbilt University Medical Center, Nashville, Tennessee.

11. 11Center for Cancer Research and Center for Regenerative Medicine, Massachusetts General Hospital, Boston, Massachusetts.

Abstract

Abstract Purpose: Young women treated for breast cancer with cytotoxic therapies are at risk for clonal hematopoiesis of indeterminate potential (CHIP), a condition in which blood cells carrying a somatic mutation associated with hematologic malignancy comprise at least 4% of the total blood system. CHIP has primarily been studied in older patient cohorts with limited clinical phenotyping. Experimental Design: We performed targeted sequencing on longitudinal blood samples to characterize the clonal hematopoietic landscape of 878 women treated for breast cancer enrolled in the prospective Young Women's Breast Cancer Study. Results: We identified somatic driver mutations in 252 study subjects (28.7%), but only 24 (2.7%) had clones large enough to meet criteria for CHIP. The most commonly mutated genes were DNMT3A and TET2, similar to mutations observed in noncancer cohorts. At 9-year median follow-up, we found no association between the presence of a somatic blood mutation (regardless of clone size) and adverse breast cancer (distant relapse-free survival) or non–breast cancer-related outcomes in this cohort. A subset of paired blood samples obtained over 4 years showed no evidence of mutant clonal expansion, regardless of genotype. Finally, we identified a subset of patients with likely germline mutations in genes known to contribute to inherited cancer risk, such as TP53 and ATM. Conclusions: Our data show that for young women with early-stage breast cancer, CHIP is uncommon after cytotoxic exposure, is unlikely to contribute to adverse outcomes over the decade-long follow-up and may not require additional monitoring if discovered incidentally.

Funder

V Foundation for Cancer Research

National Institutes of Health

NIH Office of the Director

Edward P. Evans Foundation

Burroughs Wellcome Fund

Pew Charitable Trusts

Alexander and Margaret Stewart Trust

Publisher

American Association for Cancer Research (AACR)

Subject

Cancer Research,Oncology

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