Single-cell transcriptomics of the myeloid milieu reveals an angiogenic niche in triple-negative breast cancer

Yechan Choi; Minkyu Shim; Suhn Hyung Kim; Duk Ki Kim; Juhee Jeong; Jinyoung Byeon; Giyong Jang; Ji Yeon Kim; Paul Robson; Charles Lee; Han Byoel Lee; Keehoon Jung

doi:10.1038/s12276-025-01571-5

Single-cell transcriptomics of the myeloid milieu reveals an angiogenic niche in triple-negative breast cancer

Yechan Choi
, Minkyu Shim
, Suhn Hyung Kim
, Duk Ki Kim
, Juhee Jeong
, Jinyoung Byeon
, Giyong Jang
, Ji Yeon Kim
, Paul Robson
, Charles Lee
, Han Byoel Lee
, Keehoon Jung

Department of Internal Medicine

Seoul National University
Ewha Womans University
Jackson Laboratory

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Intratumoral myeloid cells are highly heterogeneous in terms of development and function and are pivotal for forming and regulating the tumor microenvironment. However, the myeloid milieu in triple-negative breast cancer (TNBC) remains poorly understood. Here, to elucidate this myeloid milieu, we integrated in-house and public single-cell RNA sequencing data. We detected diverse neutrophil and mononuclear-phagocyte subtypes and delineated their developmental trajectories and functions. Of particular interest were the VEGFA^hi neutrophil and SPP1^hi macrophage subtypes, which displayed protumoral functions, including angiogenesis. Spatial transcriptomics revealed that they colocalized with epithelial cancer cells and APLN^hi endothelial tip cells in a hypoxic region forming an angiogenic niche. Moreover, patients with SPP1^hi macrophage-enriched TNBC showed poor prognosis, which worsened in patients who also displayed abundant VEGFA^hi neutrophils. These subtypes were also conserved in multiple murine TNBC models. This comprehensive analysis of the myeloid population in TNBC thus reveals a previously undercharacterized interaction between VEGFA^hi neutrophils and SPP1^hi macrophages, elucidating their contributions in the formation of an angiogenic niche.

Original language	English
Pages (from-to)	2487-2504
Number of pages	18
Journal	Experimental and Molecular Medicine
Volume	57
Issue number	11
DOIs	https://doi.org/10.1038/s12276-025-01571-5
State	Published - Nov 2025

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title = "Single-cell transcriptomics of the myeloid milieu reveals an angiogenic niche in triple-negative breast cancer",

abstract = "Intratumoral myeloid cells are highly heterogeneous in terms of development and function and are pivotal for forming and regulating the tumor microenvironment. However, the myeloid milieu in triple-negative breast cancer (TNBC) remains poorly understood. Here, to elucidate this myeloid milieu, we integrated in-house and public single-cell RNA sequencing data. We detected diverse neutrophil and mononuclear-phagocyte subtypes and delineated their developmental trajectories and functions. Of particular interest were the VEGFAhi neutrophil and SPP1hi macrophage subtypes, which displayed protumoral functions, including angiogenesis. Spatial transcriptomics revealed that they colocalized with epithelial cancer cells and APLNhi endothelial tip cells in a hypoxic region forming an angiogenic niche. Moreover, patients with SPP1hi macrophage-enriched TNBC showed poor prognosis, which worsened in patients who also displayed abundant VEGFAhi neutrophils. These subtypes were also conserved in multiple murine TNBC models. This comprehensive analysis of the myeloid population in TNBC thus reveals a previously undercharacterized interaction between VEGFAhi neutrophils and SPP1hi macrophages, elucidating their contributions in the formation of an angiogenic niche.",

author = "Yechan Choi and Minkyu Shim and Kim, \{Suhn Hyung\} and Kim, \{Duk Ki\} and Juhee Jeong and Jinyoung Byeon and Giyong Jang and Kim, \{Ji Yeon\} and Paul Robson and Charles Lee and Lee, \{Han Byoel\} and Keehoon Jung",

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doi = "10.1038/s12276-025-01571-5",

language = "English",

volume = "57",

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T1 - Single-cell transcriptomics of the myeloid milieu reveals an angiogenic niche in triple-negative breast cancer

AU - Choi, Yechan

AU - Shim, Minkyu

AU - Kim, Suhn Hyung

AU - Kim, Duk Ki

AU - Jeong, Juhee

AU - Byeon, Jinyoung

AU - Jang, Giyong

AU - Kim, Ji Yeon

AU - Robson, Paul

AU - Lee, Charles

AU - Lee, Han Byoel

AU - Jung, Keehoon

PY - 2025/11

Y1 - 2025/11

N2 - Intratumoral myeloid cells are highly heterogeneous in terms of development and function and are pivotal for forming and regulating the tumor microenvironment. However, the myeloid milieu in triple-negative breast cancer (TNBC) remains poorly understood. Here, to elucidate this myeloid milieu, we integrated in-house and public single-cell RNA sequencing data. We detected diverse neutrophil and mononuclear-phagocyte subtypes and delineated their developmental trajectories and functions. Of particular interest were the VEGFAhi neutrophil and SPP1hi macrophage subtypes, which displayed protumoral functions, including angiogenesis. Spatial transcriptomics revealed that they colocalized with epithelial cancer cells and APLNhi endothelial tip cells in a hypoxic region forming an angiogenic niche. Moreover, patients with SPP1hi macrophage-enriched TNBC showed poor prognosis, which worsened in patients who also displayed abundant VEGFAhi neutrophils. These subtypes were also conserved in multiple murine TNBC models. This comprehensive analysis of the myeloid population in TNBC thus reveals a previously undercharacterized interaction between VEGFAhi neutrophils and SPP1hi macrophages, elucidating their contributions in the formation of an angiogenic niche.

AB - Intratumoral myeloid cells are highly heterogeneous in terms of development and function and are pivotal for forming and regulating the tumor microenvironment. However, the myeloid milieu in triple-negative breast cancer (TNBC) remains poorly understood. Here, to elucidate this myeloid milieu, we integrated in-house and public single-cell RNA sequencing data. We detected diverse neutrophil and mononuclear-phagocyte subtypes and delineated their developmental trajectories and functions. Of particular interest were the VEGFAhi neutrophil and SPP1hi macrophage subtypes, which displayed protumoral functions, including angiogenesis. Spatial transcriptomics revealed that they colocalized with epithelial cancer cells and APLNhi endothelial tip cells in a hypoxic region forming an angiogenic niche. Moreover, patients with SPP1hi macrophage-enriched TNBC showed poor prognosis, which worsened in patients who also displayed abundant VEGFAhi neutrophils. These subtypes were also conserved in multiple murine TNBC models. This comprehensive analysis of the myeloid population in TNBC thus reveals a previously undercharacterized interaction between VEGFAhi neutrophils and SPP1hi macrophages, elucidating their contributions in the formation of an angiogenic niche.

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DO - 10.1038/s12276-025-01571-5

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SN - 1226-3613

VL - 57

SP - 2487

EP - 2504

JO - Experimental and Molecular Medicine

JF - Experimental and Molecular Medicine

IS - 11

ER -

Single-cell transcriptomics of the myeloid milieu reveals an angiogenic niche in triple-negative breast cancer

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