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이세민

Lee, Semin
Computational Biology Lab.
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Spatial and genomic profiling of residual breast cancer after neoadjuvant chemotherapy unveil divergent fates for each breast cancer subtype

Author(s)
Seo, Eun SeopPark, SabinCho, Eun YoonLee, Jeong EonJung, Hae HyunHyeon, JiyeonAn, SepilKim, Seok WonShin, JunghoonAhn, Jin SeokPark, Yeon HeeIm, Young-HyuckKim, HoonLee, SeminPark, Woong-YangKim, Ji-Yeon
Issued Date
2025-06
DOI
10.1016/j.xcrm.2025.102164
URI
https://scholarworks.unist.ac.kr/handle/201301/87420
Citation
CELL REPORTS MEDICINE, v.6, no.6, pp.102164
Abstract
Residual cancer burden (RCB) is a strong prognostic marker after neoadjuvant chemotherapy (NAC) in breast cancer (BC), yet some BCs defy their predicted outcomes. Using single-cell spatial transcriptomics and genomic profiling, we investigate mechanisms underlying divergent fates of BCs with high RCB across subtypes. In triple-negative BC (TNBC), CXCL9+ macrophage-CD8+ T cell interactions via chemokines and interferon-gamma signaling promote favorable outcomes, while SPP1+ macrophage-cancer cell interactions driven by hypoxia signaling correlate with poor prognosis. In non-TNBC, the extent of basal-like cancer cells and their proximity to scarce immune cells are linked to prognosis. Additionally, tumor-intrinsic features- such as homologous recombination deficiency in hormone receptor (HR)-positive cancers and structural variations, including extrachromosomal ERBB2 DNA in human epidermal growth factor receptor 2 (HER2)-positive cancers-predict worse outcomes. This study highlights distinct genomic and microenvironmental strategies governing BC subtype-specific fates after NAC.
Publisher
CELL PRESS
ISSN
2666-3791
Keyword
SIGNATURESNETWORKATLASHULLSINGLE-CELLLYMPHOCYTES

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