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Evidence for accelerated aging in mammary epithelia of women carrying germline BRCA1 or BRCA2 mutations

Sundus Shalabi, Masaru Miyano, Rosalyn W. Sayaman, Jennifer C. Lopez, Tiina Jokela, Michael E. Todhunter, Stefan Hinz, James C. Garbe, Martha R. Stampfer, Kai Kessenbrock, Victoria L. Seewaldt, Mark A. LaBarge

2021Nature Aging89 citationsDOIOpen Access PDF

Abstract

Abstract During aging in the human mammary gland, luminal epithelial cells lose lineage fidelity by expressing markers normally expressed in myoepithelial cells. We hypothesize that loss of lineage fidelity is a general manifestation of epithelia that are susceptible to cancer initiation. In the present study, we show that histologically normal breast tissue from younger women who are susceptible to breast cancer, as a result of harboring a germline mutation in BRCA1 , BRCA2 or PALB2 genes, exhibits hallmarks of accelerated aging. These include proportionately increased luminal epithelial cells that acquired myoepithelial markers, decreased proportions of myoepithelial cells and a basal differentiation bias or failure of differentiation of cKit + progenitors. High-risk luminal and myoepithelial cells are transcriptionally enriched for genes of the opposite lineage, inflammatory- and cancer-related pathways. We have identified breast-aging hallmarks that reflect a convergent biology of cancer susceptibility, regardless of the specific underlying genetic or age-dependent risk or the associated breast cancer subtype.

Topics & Concepts

Myoepithelial cellBiologyBreast cancerGermlineLineage (genetic)Mammary glandGermline mutationSomatic cellCancer researchCancerMutationGeneGeneticsImmunologyImmunohistochemistryBRCA gene mutations in cancerCancer Cells and MetastasisGenomics and Chromatin Dynamics
Evidence for accelerated aging in mammary epithelia of women carrying germline BRCA1 or BRCA2 mutations | Litcius