A single-cell atlas enables mapping of homeostatic cellular shifts in the adult human breast

Austin D. Reed(Wellcome/MRC Cambridge Stem Cell Institute), Sara Pensa(Wellcome/MRC Cambridge Stem Cell Institute), Adi Steif(University of Cambridge), Jack Stenning(Wellcome/MRC Cambridge Stem Cell Institute), Daniel J. Kunz(European Bioinformatics Institute), Linsey J. Porter(Wellcome/MRC Cambridge Stem Cell Institute), Kui Hua(University of Cambridge), Peng He(European Bioinformatics Institute), Alecia‐Jane Twigger(Wellcome/MRC Cambridge Stem Cell Institute), Abigail J. Q. Siu(Wellcome/MRC Cambridge Stem Cell Institute), Katarzyna Kania(University of Cambridge), Rachel Barrow‐McGee(Queen Mary University of London), Iain Goulding(Queen Mary University of London), Jennifer J. Gomm(Queen Mary University of London), Valerie Speirs(University of Aberdeen), Julia Jones(Queen Mary University of London), John C. Marioni(European Bioinformatics Institute), Walid T. Khaled(Wellcome/MRC Cambridge Stem Cell Institute)
Nature Genetics
March 28, 2024
Cited by 96Open Access
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Abstract

Here we use single-cell RNA sequencing to compile a human breast cell atlas assembled from 55 donors that had undergone reduction mammoplasties or risk reduction mastectomies. From more than 800,000 cells we identified 41 cell subclusters across the epithelial, immune and stromal compartments. The contribution of these different clusters varied according to the natural history of the tissue. Age, parity and germline mutations, known to modulate the risk of developing breast cancer, affected the homeostatic cellular state of the breast in different ways. We found that immune cells from BRCA1 or BRCA2 carriers had a distinct gene expression signature indicative of potential immune exhaustion, which was validated by immunohistochemistry. This suggests that immune-escape mechanisms could manifest in non-cancerous tissues very early during tumor initiation. This atlas is a rich resource that can be used to inform novel approaches for early detection and prevention of breast cancer.


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