In vitro model for DNA double‐strand break repair analysis in breast cancer reveals cell type–specific associations with age and prognosis

6533b854fe1ef96bd12aec71

RESEARCH PRODUCT

In vitro model for DNA double‐strand break repair analysis in breast cancer reveals cell type–specific associations with age and prognosis

Julia Kaufmann Miriam Deniz Marlen Keimling Michaela Ihle Andreea Stahl Lisa Wiesmüller T Gundelach Stephanie Hampp Wolfgang Janni Isabell Hoffmann

subject

Adult 0301 basic medicine Pathology medicine.medical_specialty Epithelial-Mesenchymal Transition DNA Repair DNA repair Cell Breast Neoplasms Biology medicine.disease_cause Biochemistry 03 medical and health sciences 0302 clinical medicine Breast cancer Cell Line Tumor Genetics medicine Humans DNA Breaks Double-Stranded Genetic Predisposition to Disease Breast Epithelial–mesenchymal transition Homologous Recombination Molecular Biology Aged Aged 80 and over Adenosine Diphosphate Ribose Mutation Age Factors Middle Aged DNA repair protein XRCC4 Prognosis medicine.disease Double Strand Break Repair 030104 developmental biology medicine.anatomical_structure 030220 oncology & carcinogenesis Mutation Cancer research Female Homologous recombination Biotechnology

description

Dysfunction of homologous recombination is a common denominator of changes associated with breast cancer-predisposing mutations. In our previous work, we identified a functional signature in peripheral blood lymphocytes from women who were predisposed that indicated a shift from homologous recombination to alternative, error-prone DNA double-strand break (DSB) repair pathways. To capture both hereditary and nonhereditary factors, we newly established a protocol for isolation and ex vivo analysis of epithelial cells, epithelial-mesenchymal transition cells (EMTs), and fibroblasts from breast cancer specimens (147 patients). By applying a fluorescence-based test system, we analyzed the error-prone DSB repair pathway microhomology-mediated end joining in these tumor-derived cell types and peripheral blood lymphocytes. In parallel, we investigated DNA lesion processing by quantitative immunofluorescence microscopy of histone H2AX phosphorylated on Ser139 focus after radiomimetic treatment. Our study reveals elevated histone H2AX phosphorylated on Ser139 damage removal in epithelial cells, not EMTs, and poly(ADP-ribose)polymerase inhibitor sensitivities, which suggested a DSB repair pathway shift with increasing patient age. Of interest, we found elevated microhomology-mediated end joining in EMTs, not epithelial cells, from patients who received a treatment recommendation of adjuvant chemotherapy, that is, those with high-risk tumors. Our discoveries of altered DSB repair activities in cells may serve as a method to further classify breast cancer to predict responsiveness to adjuvant chemotherapy and/or therapeutics that target DSB repair-dysfunctional tumors.-Deniz, M., Kaufmann, J., Stahl, A., Gundelach, T., Janni, W., Hoffmann, I., Keimling, M., Hampp, S., Ihle, M., Wiesmüller, L. In vitro model for DNA double-strand break repair analysis in breast cancer reveals cell type-specific associations with age and prognosis.

year	journal	country	edition	language
2016-03-17	The FASEB Journal

https://doi.org/10.1096/fj.201600453r