Exome sequencing reveals frequent deleterious germline variants in cancer susceptibility genes in women with invasive breast cancer undergoing neoadjuvant chemotherapy

被引:0
作者
Marissa S. Ellingson
Steven N. Hart
Krishna R. Kalari
Vera Suman
Kimberly A. Schahl
Travis J. Dockter
Sara J. Felten
Jason P. Sinnwell
Kevin J. Thompson
Xiaojia Tang
Peter T. Vedell
Poulami Barman
Hugues Sicotte
Jeanette E. Eckel-Passow
Donald W. Northfelt
Richard J. Gray
Sarah A. McLaughlin
Alvaro Moreno-Aspitia
James N. Ingle
Ann M. Moyer
Daniel W. Visscher
Katie Jones
Amy Conners
Michelle McDonough
Eric D. Wieben
Liewei Wang
Richard Weinshilboum
Judy C. Boughey
Matthew P. Goetz
机构
[1] Mayo Clinic,Center for Individualized Medicine
[2] Mayo Clinic,Department of Health Sciences Research
[3] Mayo Clinic,Hematology/Oncology
[4] Mayo Clinic,Department of Surgery
[5] Mayo Clinic,Department of Surgery
[6] Mayo Clinic,Hematology/Oncology
[7] Mayo Clinic,Department of Laboratory Medicine and Pathology
[8] Mayo Clinic,Department of Radiology
[9] Mayo Clinic,Department of Radiology
[10] Mayo Clinic,Biochemistry
[11] Mayo Clinic,Department of Molecular Pharmacology & Experimental Therapeutics
[12] Mayo Clinic,Department of Surgery
[13] Mayo Clinic,Medical Oncology
来源
Breast Cancer Research and Treatment | 2015年 / 153卷
关键词
Breast cancer; Neoadjuvant chemotherapy; High-risk breast cancer; Return of results; Exome sequencing; Germline mutation/pathogenic germline variant;
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摘要
When sequencing blood and tumor samples to identify targetable somatic variants for cancer therapy, clinically relevant germline variants may be uncovered. We evaluated the prevalence of deleterious germline variants in cancer susceptibility genes in women with breast cancer referred for neoadjuvant chemotherapy and returned clinically actionable results to patients. Exome sequencing was performed on blood samples from women with invasive breast cancer referred for neoadjuvant chemotherapy. Germline variants within 142 hereditary cancer susceptibility genes were filtered and reviewed for pathogenicity. Return of results was offered to patients with deleterious variants in actionable genes if they were not aware of their result through clinical testing. 124 patients were enrolled (median age 51) with the following subtypes: triple negative (n = 43, 34.7 %), HER2+ (n = 37, 29.8 %), luminal B (n = 31, 25 %), and luminal A (n = 13, 10.5 %). Twenty-eight deleterious variants were identified in 26/124 (21.0 %) patients in the following genes: ATM (n = 3), BLM (n = 1), BRCA1 (n = 4), BRCA2 (n = 8), CHEK2 (n = 2), FANCA (n = 1), FANCI (n = 1), FANCL (n = 1), FANCM (n = 1), FH (n = 1), MLH3 (n = 1), MUTYH (n = 2), PALB2 (n = 1), and WRN (n = 1). 121/124 (97.6 %) patients consented to return of research results. Thirteen (10.5 %) had actionable variants, including four that were returned to patients and led to changes in medical management. Deleterious variants in cancer susceptibility genes are highly prevalent in patients with invasive breast cancer referred for neoadjuvant chemotherapy undergoing exome sequencing. Detection of these variants impacts medical management.
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页码:435 / 443
页数:8
相关论文
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