AI Article Synopsis
- Breast cancer brain metastases are challenging to treat, with chemotherapy being ineffective and limited treatment options leading to poor patient outcomes.
- This study investigates gene copy number variation (CNV) in 10 metastatic brain tumors from breast cancer patients using array comparative genomic hybridization (aCGH), identifying significant cancer gene aberrations in all specimens.
- The findings suggest that original breast cancer oncogenic signals persist in metastatic tumors, supporting the need for genomic-based diagnostics and the development of new treatment strategies.
Article Abstract
Breast cancer brain metastases remain a significant clinical problem. Chemotherapy is ineffective and a lack of treatment options result in poor patient outcomes. Targeted therapeutics have proven to be highly effective in primary breast cancer, but lack of molecular genomic characterization of metastatic brain tumors is hindering the development of new treatment regimens. Here we contribute to fill this void by reporting on gene copy number variation (CNV) in 10 breast cancer metastatic brain tumors, assayed by array comparative genomic hybridization (aCGH). Results were compared to a list of cancer genes verified by others to influence cancer. Cancer gene aberrations were identified in all specimens and pathway-level analysis was applied to aggregate data, which identified stem cell pluripotency pathway enrichment and highlighted recurring, significant amplification of SOX2, PIK3CA, NTRK1, GNAS, CTNNB1, and FGFR1. For a subset of the metastatic brain tumor samples (n = 4) we compared patient-matched primary breast cancer specimens. The results of our CGH analysis and validation by alternative methods indicate that oncogenic signals driving growth of metastatic tumors exist in the original cancer. This report contributes support for more rapid development of new treatments of metastatic brain tumors, the use of genomic-based diagnostic tools and repurposed drug treatments.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4546491 | PMC |
| http://dx.doi.org/10.18632/oncotarget.3786 | DOI Listing |
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