An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis

Ian W. Folkert; William A. Molina Arocho; Tsun Ki Jerrick To; Samir Devalaraja; Irene S. Molina; Jason Shoush; Hesham Mohei; Li Zhai; Md Naushad Akhtar; Veena Kochat; Emre Arslan; Alexander J. Lazar; Khalida Wani; William P. Israel; Zhan Zhang; Venkata S. Chaluvadi; Robert J. Norgard; Ying Liu; Ashley M. Fuller; Mai T. Dang; Robert E. Roses; Giorgos C. Karakousis; John T. Miura; Douglas L. Fraker; T. S.Karin Eisinger-Mathason; M. Celeste Simon; Kristy Weber; Kai Tan; Yi Fan; Kunal Rai; Malay Haldar

doi:10.1084/jem.20230420

An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis

Ian W. Folkert, William A. Molina Arocho, Tsun Ki Jerrick To, Samir Devalaraja, Irene S. Molina, Jason Shoush, Hesham Mohei, Li Zhai, Md Naushad Akhtar, Veena Kochat, Emre Arslan, Alexander J. Lazar, Khalida Wani, William P. Israel, Zhan Zhang, Venkata S. Chaluvadi, Robert J. Norgard, Ying Liu, Ashley M. Fuller, Mai T. DangRobert E. Roses, Giorgos C. Karakousis, John T. Miura, Douglas L. Fraker, T. S.Karin Eisinger-Mathason, M. Celeste Simon, Kristy Weber, Kai Tan, Yi Fan, Kunal Rai, Malay Haldar

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Abstract

We define a subset of macrophages in the tumor microenvironment characterized by high intracellular iron and enrichment of heme and iron metabolism genes. These iron-rich tumor-associated macrophages (iTAMs) supported angiogenesis and immunosuppression in the tumor microenvironment and were conserved between mice and humans. iTAMs comprise two additional subsets based on gene expression profile and location—perivascular (pviTAM) and stromal (stiTAM). We identified the endothelin receptor type B (Ednrb) as a specific marker of iTAMs and found myeloid-specific deletion of Ednrb to reduce tumor growth and vascular density. Further studies identified the transcription factor Bach1 as a repressor of the iTAM transcriptional program, including Ednrb expression. Heme is a known inhibitor of Bach1, and, correspondingly, heme exposure induced Ednrb and iTAM signature genes in macrophages. Thus, iTAMs are a distinct macrophage subset regulated by the transcription factor Bach1 and characterized by Ednrb-mediated immunosuppressive and angiogenic functions.

Original language	English
Article number	e20230420
Journal	Journal of Experimental Medicine
Volume	221
Issue number	10
DOIs	https://doi.org/10.1084/jem.20230420
State	Published - 2024

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Folkert, I. W., Molina Arocho, W. A., To, T. K. J., Devalaraja, S., Molina, I. S., Shoush, J., Mohei, H., Zhai, L., Akhtar, M. N., Kochat, V., Arslan, E., Lazar, A. J., Wani, K., Israel, W. P., Zhang, Z., Chaluvadi, V. S., Norgard, R. J., Liu, Y., Fuller, A. M., ... Haldar, M. (2024). An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis. Journal of Experimental Medicine, 221(10), Article e20230420. https://doi.org/10.1084/jem.20230420

@article{9cb67490def0429d895339879bcc88ae,

title = "An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis",

abstract = "We define a subset of macrophages in the tumor microenvironment characterized by high intracellular iron and enrichment of heme and iron metabolism genes. These iron-rich tumor-associated macrophages (iTAMs) supported angiogenesis and immunosuppression in the tumor microenvironment and were conserved between mice and humans. iTAMs comprise two additional subsets based on gene expression profile and location—perivascular (pviTAM) and stromal (stiTAM). We identified the endothelin receptor type B (Ednrb) as a specific marker of iTAMs and found myeloid-specific deletion of Ednrb to reduce tumor growth and vascular density. Further studies identified the transcription factor Bach1 as a repressor of the iTAM transcriptional program, including Ednrb expression. Heme is a known inhibitor of Bach1, and, correspondingly, heme exposure induced Ednrb and iTAM signature genes in macrophages. Thus, iTAMs are a distinct macrophage subset regulated by the transcription factor Bach1 and characterized by Ednrb-mediated immunosuppressive and angiogenic functions.",

author = "Folkert, {Ian W.} and {Molina Arocho}, {William A.} and To, {Tsun Ki Jerrick} and Samir Devalaraja and Molina, {Irene S.} and Jason Shoush and Hesham Mohei and Li Zhai and Akhtar, {Md Naushad} and Veena Kochat and Emre Arslan and Lazar, {Alexander J.} and Khalida Wani and Israel, {William P.} and Zhan Zhang and Chaluvadi, {Venkata S.} and Norgard, {Robert J.} and Ying Liu and Fuller, {Ashley M.} and Dang, {Mai T.} and Roses, {Robert E.} and Karakousis, {Giorgos C.} and Miura, {John T.} and Fraker, {Douglas L.} and Eisinger-Mathason, {T. S.Karin} and Simon, {M. Celeste} and Kristy Weber and Kai Tan and Yi Fan and Kunal Rai and Malay Haldar",

note = "Publisher Copyright: {\textcopyright} 2024 Folkert et al.",

year = "2024",

doi = "10.1084/jem.20230420",

language = "English",

volume = "221",

journal = "Journal of Experimental Medicine",

issn = "0022-1007",

number = "10",

}

Folkert, IW, Molina Arocho, WA, To, TKJ, Devalaraja, S, Molina, IS, Shoush, J, Mohei, H, Zhai, L, Akhtar, MN, Kochat, V, Arslan, E, Lazar, AJ, Wani, K, Israel, WP, Zhang, Z, Chaluvadi, VS, Norgard, RJ, Liu, Y, Fuller, AM, Dang, MT, Roses, RE, Karakousis, GC, Miura, JT, Fraker, DL, Eisinger-Mathason, TSK, Simon, MC, Weber, K, Tan, K, Fan, Y, Rai, K & Haldar, M 2024, 'An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis', Journal of Experimental Medicine, vol. 221, no. 10, e20230420. https://doi.org/10.1084/jem.20230420

TY - JOUR

T1 - An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis

AU - Folkert, Ian W.

AU - Molina Arocho, William A.

AU - To, Tsun Ki Jerrick

AU - Devalaraja, Samir

AU - Molina, Irene S.

AU - Shoush, Jason

AU - Mohei, Hesham

AU - Zhai, Li

AU - Akhtar, Md Naushad

AU - Kochat, Veena

AU - Arslan, Emre

AU - Lazar, Alexander J.

AU - Wani, Khalida

AU - Israel, William P.

AU - Zhang, Zhan

AU - Chaluvadi, Venkata S.

AU - Norgard, Robert J.

AU - Liu, Ying

AU - Fuller, Ashley M.

AU - Dang, Mai T.

AU - Roses, Robert E.

AU - Karakousis, Giorgos C.

AU - Miura, John T.

AU - Fraker, Douglas L.

AU - Eisinger-Mathason, T. S.Karin

AU - Simon, M. Celeste

AU - Weber, Kristy

AU - Tan, Kai

AU - Fan, Yi

AU - Rai, Kunal

AU - Haldar, Malay

PY - 2024

Y1 - 2024

N2 - We define a subset of macrophages in the tumor microenvironment characterized by high intracellular iron and enrichment of heme and iron metabolism genes. These iron-rich tumor-associated macrophages (iTAMs) supported angiogenesis and immunosuppression in the tumor microenvironment and were conserved between mice and humans. iTAMs comprise two additional subsets based on gene expression profile and location—perivascular (pviTAM) and stromal (stiTAM). We identified the endothelin receptor type B (Ednrb) as a specific marker of iTAMs and found myeloid-specific deletion of Ednrb to reduce tumor growth and vascular density. Further studies identified the transcription factor Bach1 as a repressor of the iTAM transcriptional program, including Ednrb expression. Heme is a known inhibitor of Bach1, and, correspondingly, heme exposure induced Ednrb and iTAM signature genes in macrophages. Thus, iTAMs are a distinct macrophage subset regulated by the transcription factor Bach1 and characterized by Ednrb-mediated immunosuppressive and angiogenic functions.

AB - We define a subset of macrophages in the tumor microenvironment characterized by high intracellular iron and enrichment of heme and iron metabolism genes. These iron-rich tumor-associated macrophages (iTAMs) supported angiogenesis and immunosuppression in the tumor microenvironment and were conserved between mice and humans. iTAMs comprise two additional subsets based on gene expression profile and location—perivascular (pviTAM) and stromal (stiTAM). We identified the endothelin receptor type B (Ednrb) as a specific marker of iTAMs and found myeloid-specific deletion of Ednrb to reduce tumor growth and vascular density. Further studies identified the transcription factor Bach1 as a repressor of the iTAM transcriptional program, including Ednrb expression. Heme is a known inhibitor of Bach1, and, correspondingly, heme exposure induced Ednrb and iTAM signature genes in macrophages. Thus, iTAMs are a distinct macrophage subset regulated by the transcription factor Bach1 and characterized by Ednrb-mediated immunosuppressive and angiogenic functions.

UR - http://www.scopus.com/inward/record.url?scp=85205336604&partnerID=8YFLogxK

U2 - 10.1084/jem.20230420

DO - 10.1084/jem.20230420

M3 - Article

C2 - 39347789

AN - SCOPUS:85205336604

SN - 0022-1007

VL - 221

JO - Journal of Experimental Medicine

JF - Journal of Experimental Medicine

IS - 10

M1 - e20230420

ER -

An iron-rich subset of macrophages promotes tumor growth through a Bach1-Ednrb axis

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