| Literature DB >> 35617956 |
G Kenneth Gray1, Carman Man-Chung Li1, Jennifer M Rosenbluth2, Laura M Selfors1, Nomeda Girnius3, Jia-Ren Lin4, Ron C J Schackmann1, Walter L Goh1, Kaitlin Moore1, Hana K Shapiro1, Shaolin Mei4, Kurt D'Andrea5, Katherine L Nathanson5, Peter K Sorger4, Sandro Santagata6, Aviv Regev7, Judy E Garber8, Deborah A Dillon9, Joan S Brugge10.
Abstract
The breast is a dynamic organ whose response to physiological and pathophysiological conditions alters its disease susceptibility, yet the specific effects of these clinical variables on cell state remain poorly annotated. We present a unified, high-resolution breast atlas by integrating single-cell RNA-seq, mass cytometry, and cyclic immunofluorescence, encompassing a myriad of states. We define cell subtypes within the alveolar, hormone-sensing, and basal epithelial lineages, delineating associations of several subtypes with cancer risk factors, including age, parity, and BRCA2 germline mutation. Of particular interest is a subset of alveolar cells termed basal-luminal (BL) cells, which exhibit poor transcriptional lineage fidelity, accumulate with age, and carry a gene signature associated with basal-like breast cancer. We further utilize a medium-depletion approach to identify molecular factors regulating cell-subtype proportion in organoids. Together, these data are a rich resource to elucidate diverse mammary cell states.Entities:
Keywords: BRCA1; BRCA2; CyTOF mass cytometry; aging; breast cancer; cell state plasticity; mammary biology; multi-omic single-cell atlas; multiplexed tissue staining; organoids; scRNA-Seq
Mesh:
Year: 2022 PMID: 35617956 PMCID: PMC9202341 DOI: 10.1016/j.devcel.2022.05.003
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 13.417