Differential chromatin accessibility and transcriptional dynamics define breast cancer subtypes and their lineages

Michael D. Iglesia; Reyka G. Jayasinghe; Siqi Chen; Nadezhda V. Terekhanova; John M. Herndon; Erik Storrs; Alla Y. Karpova; Daniel Cui Zhou; Nataly Naser Al Deen; Andrew Shinkle; Rita Jui-Hsien Lu; Wagma Caravan; Andrew Houston; Yanyan Zhao; Kazuhito Sato; Preet Lal; Cherease Street; Fernanda Martins Rodrigues; Austin N. Southard-Smith; André Luiz N. Targino da Costa; Houxiang Zhu; Chia-Kuei Mo; Lisa Crowson; Robert S. Fulton; Matthew A. Wyczalkowski; Catrina C. Fronick; Lucinda A. Fulton; Hua Sun; Sherri R. Davies; Elizabeth L. Appelbaum; Sara E. Chasnoff; Madelyn Carmody; Candace Brooks; Ruiyang Liu; Michael C. Wendl; Clara Oh; Diane E. Bender; Carlos Cruchaga; Oscar Harari; Andrea Bredemeyer; Kory J. Lavine; Ron Bose; Julie A. Margenthaler; Jason M. Held; Samuel Achilefu; Foluso O. Ademuyiwa; Rebecca Aft; X. Cynthia; Graham A. Colditz; Tao Ju; Stephen T. Oh; James A. J. Fitzpatrick; E. Shelley Hwang; Kooresh I. Shoghi; Milan G. Chheda; Deborah V. Novack; Feng Chen; Ryan C. Fields; William E. Gillanders; Li Ding

doi:10.1038/s43018-024-00773-6

Differential chromatin accessibility and transcriptional dynamics define breast cancer subtypes and their lineages

Michael D. Iglesia(James S. McDonnell Foundation), Reyka G. Jayasinghe(James S. McDonnell Foundation), Siqi Chen(James S. McDonnell Foundation), Nadezhda V. Terekhanova(James S. McDonnell Foundation), John M. Herndon(Washington University in St. Louis), Erik Storrs(James S. McDonnell Foundation), Alla Y. Karpova(James S. McDonnell Foundation), Daniel Cui Zhou(James S. McDonnell Foundation), Nataly Naser Al Deen(James S. McDonnell Foundation), Andrew Shinkle(James S. McDonnell Foundation), Rita Jui-Hsien Lu(James S. McDonnell Foundation), Wagma Caravan(James S. McDonnell Foundation), Andrew Houston(James S. McDonnell Foundation), Yanyan Zhao(James S. McDonnell Foundation), Kazuhito Sato(James S. McDonnell Foundation), Preet Lal(Washington University in St. Louis), Cherease Street(Washington University in St. Louis), Fernanda Martins Rodrigues(James S. McDonnell Foundation), Austin N. Southard-Smith(James S. McDonnell Foundation), André Luiz N. Targino da Costa(James S. McDonnell Foundation), Houxiang Zhu(James S. McDonnell Foundation), Chia-Kuei Mo(James S. McDonnell Foundation), Lisa Crowson(James S. McDonnell Foundation), Robert S. Fulton(James S. McDonnell Foundation), Matthew A. Wyczalkowski(James S. McDonnell Foundation), Catrina C. Fronick(James S. McDonnell Foundation), Lucinda A. Fulton(James S. McDonnell Foundation), Hua Sun(James S. McDonnell Foundation), Sherri R. Davies(Washington University in St. Louis), Elizabeth L. Appelbaum(James S. McDonnell Foundation), Sara E. Chasnoff(Washington University in St. Louis), Madelyn Carmody(Washington University in St. Louis), Candace Brooks(Washington University in St. Louis), Ruiyang Liu(James S. McDonnell Foundation), Michael C. Wendl(James S. McDonnell Foundation), Clara Oh(James S. McDonnell Foundation), Diane E. Bender(Washington University in St. Louis), Carlos Cruchaga(Washington University in St. Louis), Oscar Harari(Washington University in St. Louis), Andrea Bredemeyer(Washington University in St. Louis), Kory J. Lavine(Washington University in St. Louis), Ron Bose(Washington University in St. Louis), Julie A. Margenthaler(Washington University in St. Louis), Jason M. Held(Washington University in St. Louis), Samuel Achilefu(Washington University in St. Louis), Foluso O. Ademuyiwa(Washington University in St. Louis), Rebecca Aft(Washington University in St. Louis), X. Cynthia(Washington University in St. Louis), Graham A. Colditz(Washington University in St. Louis), Tao Ju(Washington University in St. Louis), Stephen T. Oh(Washington University in St. Louis), James A. J. Fitzpatrick(Washington University in St. Louis), E. Shelley Hwang(Duke Medical Center), Kooresh I. Shoghi(Washington University in St. Louis), Milan G. Chheda(Washington University in St. Louis), Deborah V. Novack(Washington University in St. Louis), Feng Chen(Washington University in St. Louis), Ryan C. Fields(Washington University in St. Louis), William E. Gillanders(Washington University in St. Louis), Li Ding(James S. McDonnell Foundation)

Nature Cancer

October 30, 2024

10.1038/s43018-024-00773-6

Cited by 26Open Access

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Abstract

Abstract Breast cancer (BC) is defined by distinct molecular subtypes with different cells of origin. The transcriptional networks that characterize the subtype-specific tumor-normal lineages are not established. In this work, we applied bulk, single-cell and single-nucleus multi-omic techniques as well as spatial transcriptomics and multiplex imaging on 61 samples from 37 patients with BC to show characteristic links in gene expression and chromatin accessibility between BC subtypes and their putative cells of origin. Regulatory network analysis of transcription factors underscored the importance of BHLHE40 in luminal BC and luminal mature cells and KLF5 in basal-like tumors and luminal progenitor cells. Furthermore, we identify key genes defining the basal-like ( SOX6 and KCNQ3 ) and luminal A/B ( FAM155A and LRP1B ) lineages. Exhausted CTLA4-expressing CD8 + T cells were enriched in basal-like BC, suggesting an altered means of immune dysfunction. These findings demonstrate analysis of paired transcription and chromatin accessibility at the single-cell level is a powerful tool for investigating cancer lineage and highlight transcriptional networks that define basal and luminal BC lineages.

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