Acquired mutations and transcriptional remodeling in long-term estrogen-deprived locoregional breast cancer recurrences

Endocrine therapy resistance is a hallmark of advanced estrogen receptor (ER)-positive breast cancer. In this study, we aimed to determine acquired genomic changes in endocrine-resistant disease. We performed DNA/RNA hybrid-capture sequencing on 12 locoregional recurrences after long-term estrogen d...

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Bibliographic Details
Published in:Breast cancer research : BCR 2021-01, Vol.23 (1), p.1-14, Article 1
Main Authors: Priedigkeit, Nolan, Ding, Kai, Horne, William, Kolls, Jay K, Du, Tian, Lucas, Peter C, Blohmer, Jens-Uwe, Denkert, Carsten, Machleidt, Anna, Ingold-Heppner, Barbara, Oesterreich, Steffi, Lee, Adrian V
Format: Article
Language:English
Subjects:
Biomarkers, Tumor
Blacklisting
Breast cancer
Breast Neoplasms - etiology
Breast Neoplasms - metabolism
Breast Neoplasms - pathology
Breast Neoplasms - therapy
Computational Biology - methods
Copy number
Deoxyribonucleic acid
Diseases
DNA
DNA Copy Number Variations
DNA sequencing
Endocrine therapy
Estimates
Estrogen receptor
Estrogen Receptor alpha - metabolism
Estrogen receptors
Estrogens
Estrogens - metabolism
Female
Fibroblast growth factor receptor 4
FosB protein
FOXO1 protein
Gene expression
Gene Expression Profiling
Gene Expression Regulation, Neoplastic
Genes
Genetic aspects
Genetic transcription
Humans
Locoregional recurrence
Metastasis
Mutation
p53 Protein
Patients
Pax3 protein
Phenols
Recurrence
Relapse
RNA
RNA-seq
Therapy resistance
Transcription
Transcriptome
Tumor proteins
Tumors
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Summary:Endocrine therapy resistance is a hallmark of advanced estrogen receptor (ER)-positive breast cancer. In this study, we aimed to determine acquired genomic changes in endocrine-resistant disease. We performed DNA/RNA hybrid-capture sequencing on 12 locoregional recurrences after long-term estrogen deprivation and identified acquired genomic changes versus each tumor's matched primary. Despite being up to 7 years removed from the primary lesion, most recurrences harbored similar intrinsic transcriptional and copy number profiles. Only two genes, AKAP9 and KMT2C, were found to have single nucleotide variant (SNV) enrichments in more than one recurrence. Enriched mutations in single cases included SNVs within transcriptional regulators such as ARID1A, TP53, FOXO1, BRD1, NCOA1, and NCOR2 with one local recurrence gaining three PIK3CA mutations. In contrast to DNA-level changes, we discovered recurrent outlier mRNA expression alterations were common-including outlier gains in TP63 (n = 5 cases [42%]), NTRK3 (n = 5 [42%]), NTRK2 (n = 4 [33%]), PAX3 (n = 4 [33%]), FGFR4 (n = 3 [25%]), and TERT (n = 3 [25%]). Recurrent losses involved ESR1 (n = 5 [42%]), RELN (n = 5 [42%]), SFRP4 (n = 4 [33%]), and FOSB (n = 4 [33%]). ESR1-depleted recurrences harbored shared transcriptional remodeling events including upregulation of PROM1 and other basal cancer markers. Taken together, this study defines acquired genomic changes in long-term, estrogen-deprived disease; highlights the importance of longitudinal RNA profiling; and identifies a common ESR1-depleted endocrine-resistant breast cancer subtype with basal-like transcriptional reprogramming.
ISSN:1465-542X
1465-5411
1465-542X
DOI:10.1186/s13058-020-01379-3