Literature DB >> 29263308

Mutational profiles of breast cancer metastases from a rapid autopsy series reveal multiple evolutionary trajectories.

Bracha Erlanger Avigdor1, Ashley Cimino-Mathews1,2, Angelo M DeMarzo1,2, Jessica L Hicks1,2, James Shin1,2, Saraswati Sukumar1, John Fetting1, Pedram Argani1,2, Ben H Park1,3, Sarah J Wheelan1,4,5.   

Abstract

Heterogeneity within and among tumors in a metastatic cancer patient is a well-established phenomenon that may confound treatment and accurate prognosis. Here, we used whole-exome sequencing to survey metastatic breast cancer tumors from 5 patients in a rapid autopsy program to construct the origin and genetic development of metastases. Metastases were obtained from 5 breast cancer patients using a rapid autopsy protocol and subjected to whole-exome sequencing. Metastases were evaluated for sharing of somatic mutations, correlation of copy number variation and loss of heterozygosity, and genetic similarity scores. Pathological features of the patients' disease were assessed by immunohistochemical analyses. Our data support a monoclonal origin of metastasis in 3 cases, but in 2 cases, metastases arose from at least 2 distinct subclones in the primary tumor. In the latter 2 cases, the primary tumor presented with mixed histologic and pathologic features, suggesting early divergent evolution within the primary tumor with maintenance of metastatic capability in multiple lineages. We used genetic and histopathological evidence to demonstrate that metastases can be derived from a single or multiple independent clones within a primary tumor. This underscores the complexity of breast cancer clonal evolution and has implications for how best to determine and implement therapies for early- and late-stage disease.

Entities:  

Keywords:  Genetic variation; Genetics

Mesh:

Substances:

Year:  2017        PMID: 29263308      PMCID: PMC5752302          DOI: 10.1172/jci.insight.96896

Source DB:  PubMed          Journal:  JCI Insight        ISSN: 2379-3708


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