Interferon-gamma is quintessential for NOS2 and COX2 expression in ER- breast tumors that lead to poor outcome

Robert Y.S. Cheng; Lisa A. Ridnour; Adelaide L. Wink; Ana L. Gonzalez; Elise L. Femino; Helene Rittscher; Veena Somasundaram; William F. Heinz; Leandro Coutinho; M. Cristina Rangel; Elijah F. Edmondson; Donna Butcher; Robert J. Kinders; Xiaoxian Li; Stephen T.C. Wong; Daniel W. McVicar; Stephen K. Anderson; Milind Pore; Stephen M. Hewitt; Timothy R. Billiar; Sharon A. Glynn; Jenny C. Chang; Stephen J. Lockett; Stefan Ambs; David A. Wink

doi:10.1038/s41419-023-05834-9

Interferon-gamma is quintessential for NOS2 and COX2 expression in ER^- breast tumors that lead to poor outcome

Robert Y.S. Cheng
, Lisa A. Ridnour
, Adelaide L. Wink
, Ana L. Gonzalez
, Elise L. Femino
, Helene Rittscher
, Veena Somasundaram
, William F. Heinz
, Leandro Coutinho
, M. Cristina Rangel
, Elijah F. Edmondson
, Donna Butcher
, Robert J. Kinders
, Xiaoxian Li
, Stephen T.C. Wong
, Daniel W. McVicar
, Stephen K. Anderson
, Milind Pore
, Stephen M. Hewitt
, Timothy R. Billiar

Sharon A. Glynn, Jenny C. Chang, Stephen J. Lockett, Stefan Ambs, David A. Wink

Pathology

Basic Research Laboratory
Cancer Research Technology Program
University of São Paulo
Emory University School of Medicine
Houston Methodist Hospital
National Cancer Institute (NCI)
University of Pittsburgh Medical Center

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

10 Citations (Scopus)

Abstract

A strong correlation between NOS2 and COX2 tumor expression and poor clinical outcomes in ER breast cancer has been established. However, the mechanisms of tumor induction of these enzymes are unclear. Analysis of The Cancer Genome Atlas (TCGA) revealed correlations between NOS2 and COX2 expression and Th1 cytokines. Herein, single-cell RNAseq analysis of TNBC cells shows potent NOS2 and COX2 induction by IFNγ combined with IL1β or TNFα. Given that IFNγ is secreted by cytolytic lymphocytes, which improve clinical outcomes, this role of IFNγ presents a dichotomy. To explore this conundrum, tumor NOS2, COX2, and CD8⁺ T cells were spatially analyzed in aggressive ER–, TNBC, and HER2 + breast tumors. High expression and clustering of NOS2-expressing tumor cells occurred at the tumor/stroma interface in the presence of stroma-restricted CD8⁺ T cells. High expression and clustering of COX2-expressing tumor cells extended into immune desert regions in the tumor core where CD8⁺ T cell penetration was limited or absent. Moreover, high NOS2-expressing tumor cells were proximal to areas with increased satellitosis, suggestive of cell clusters with a higher metastatic potential. Further in vitro experiments revealed that IFNγ + IL1β/TNFα increased the elongation and migration of treated tumor cells. This spatial analysis of the tumor microenvironment provides important insight into distinct neighborhoods where stroma-restricted CD8⁺ T cells exist proximal to NOS2-expressing tumor niches that could have increased metastatic potential.

Original language	English
Article number	319
Journal	Cell Death and Disease
Volume	14
Issue number	5
DOIs	https://doi.org/10.1038/s41419-023-05834-9
Publication status	Published - 11 May 2023

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This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

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10.1038/s41419-023-05834-9

Cite this

Cheng, R. Y. S., Ridnour, L. A., Wink, A. L., Gonzalez, A. L., Femino, E. L., Rittscher, H., Somasundaram, V., Heinz, W. F., Coutinho, L., Rangel, M. C., Edmondson, E. F., Butcher, D., Kinders, R. J., Li, X., Wong, S. T. C., McVicar, D. W., Anderson, S. K., Pore, M., Hewitt, S. M., ... Wink, D. A. (2023). Interferon-gamma is quintessential for NOS2 and COX2 expression in ER^- breast tumors that lead to poor outcome. Cell Death and Disease, 14(5), Article 319. https://doi.org/10.1038/s41419-023-05834-9

@article{f930a491149f422ca653b3515c40b262,

title = "Interferon-gamma is quintessential for NOS2 and COX2 expression in ER- breast tumors that lead to poor outcome",

abstract = "A strong correlation between NOS2 and COX2 tumor expression and poor clinical outcomes in ER breast cancer has been established. However, the mechanisms of tumor induction of these enzymes are unclear. Analysis of The Cancer Genome Atlas (TCGA) revealed correlations between NOS2 and COX2 expression and Th1 cytokines. Herein, single-cell RNAseq analysis of TNBC cells shows potent NOS2 and COX2 induction by IFNγ combined with IL1β or TNFα. Given that IFNγ is secreted by cytolytic lymphocytes, which improve clinical outcomes, this role of IFNγ presents a dichotomy. To explore this conundrum, tumor NOS2, COX2, and CD8+ T cells were spatially analyzed in aggressive ER–, TNBC, and HER2 + breast tumors. High expression and clustering of NOS2-expressing tumor cells occurred at the tumor/stroma interface in the presence of stroma-restricted CD8+ T cells. High expression and clustering of COX2-expressing tumor cells extended into immune desert regions in the tumor core where CD8+ T cell penetration was limited or absent. Moreover, high NOS2-expressing tumor cells were proximal to areas with increased satellitosis, suggestive of cell clusters with a higher metastatic potential. Further in vitro experiments revealed that IFNγ + IL1β/TNFα increased the elongation and migration of treated tumor cells. This spatial analysis of the tumor microenvironment provides important insight into distinct neighborhoods where stroma-restricted CD8+ T cells exist proximal to NOS2-expressing tumor niches that could have increased metastatic potential.",

author = "Cheng, \{Robert Y.S.\} and Ridnour, \{Lisa A.\} and Wink, \{Adelaide L.\} and Gonzalez, \{Ana L.\} and Femino, \{Elise L.\} and Helene Rittscher and Veena Somasundaram and Heinz, \{William F.\} and Leandro Coutinho and Rangel, \{M. Cristina\} and Edmondson, \{Elijah F.\} and Donna Butcher and Kinders, \{Robert J.\} and Xiaoxian Li and Wong, \{Stephen T.C.\} and McVicar, \{Daniel W.\} and Anderson, \{Stephen K.\} and Milind Pore and Hewitt, \{Stephen M.\} and Billiar, \{Timothy R.\} and Glynn, \{Sharon A.\} and Chang, \{Jenny C.\} and Lockett, \{Stephen J.\} and Stefan Ambs and Wink, \{David A.\}",

note = "Publisher Copyright: {\textcopyright} 2023, This is a U.S. Government work and not under copyright protection in the US; foreign copyright protection may apply.",

year = "2023",

month = may,

day = "11",

doi = "10.1038/s41419-023-05834-9",

language = "English",

volume = "14",

journal = "Cell Death and Disease",

issn = "2041-4889",

publisher = "Springer Nature",

number = "5",

}

Cheng, RYS, Ridnour, LA, Wink, AL, Gonzalez, AL, Femino, EL, Rittscher, H, Somasundaram, V, Heinz, WF, Coutinho, L, Rangel, MC, Edmondson, EF, Butcher, D, Kinders, RJ, Li, X, Wong, STC, McVicar, DW, Anderson, SK, Pore, M, Hewitt, SM, Billiar, TR, Glynn, SA, Chang, JC, Lockett, SJ, Ambs, S & Wink, DA 2023, 'Interferon-gamma is quintessential for NOS2 and COX2 expression in ER^- breast tumors that lead to poor outcome', Cell Death and Disease, vol. 14, no. 5, 319. https://doi.org/10.1038/s41419-023-05834-9

TY - JOUR

T1 - Interferon-gamma is quintessential for NOS2 and COX2 expression in ER- breast tumors that lead to poor outcome

AU - Cheng, Robert Y.S.

AU - Ridnour, Lisa A.

AU - Wink, Adelaide L.

AU - Gonzalez, Ana L.

AU - Femino, Elise L.

AU - Rittscher, Helene

AU - Somasundaram, Veena

AU - Heinz, William F.

AU - Coutinho, Leandro

AU - Rangel, M. Cristina

AU - Edmondson, Elijah F.

AU - Butcher, Donna

AU - Kinders, Robert J.

AU - Li, Xiaoxian

AU - Wong, Stephen T.C.

AU - McVicar, Daniel W.

AU - Anderson, Stephen K.

AU - Pore, Milind

AU - Hewitt, Stephen M.

AU - Billiar, Timothy R.

AU - Glynn, Sharon A.

AU - Chang, Jenny C.

AU - Lockett, Stephen J.

AU - Ambs, Stefan

AU - Wink, David A.

PY - 2023/5/11

Y1 - 2023/5/11

N2 - A strong correlation between NOS2 and COX2 tumor expression and poor clinical outcomes in ER breast cancer has been established. However, the mechanisms of tumor induction of these enzymes are unclear. Analysis of The Cancer Genome Atlas (TCGA) revealed correlations between NOS2 and COX2 expression and Th1 cytokines. Herein, single-cell RNAseq analysis of TNBC cells shows potent NOS2 and COX2 induction by IFNγ combined with IL1β or TNFα. Given that IFNγ is secreted by cytolytic lymphocytes, which improve clinical outcomes, this role of IFNγ presents a dichotomy. To explore this conundrum, tumor NOS2, COX2, and CD8+ T cells were spatially analyzed in aggressive ER–, TNBC, and HER2 + breast tumors. High expression and clustering of NOS2-expressing tumor cells occurred at the tumor/stroma interface in the presence of stroma-restricted CD8+ T cells. High expression and clustering of COX2-expressing tumor cells extended into immune desert regions in the tumor core where CD8+ T cell penetration was limited or absent. Moreover, high NOS2-expressing tumor cells were proximal to areas with increased satellitosis, suggestive of cell clusters with a higher metastatic potential. Further in vitro experiments revealed that IFNγ + IL1β/TNFα increased the elongation and migration of treated tumor cells. This spatial analysis of the tumor microenvironment provides important insight into distinct neighborhoods where stroma-restricted CD8+ T cells exist proximal to NOS2-expressing tumor niches that could have increased metastatic potential.

AB - A strong correlation between NOS2 and COX2 tumor expression and poor clinical outcomes in ER breast cancer has been established. However, the mechanisms of tumor induction of these enzymes are unclear. Analysis of The Cancer Genome Atlas (TCGA) revealed correlations between NOS2 and COX2 expression and Th1 cytokines. Herein, single-cell RNAseq analysis of TNBC cells shows potent NOS2 and COX2 induction by IFNγ combined with IL1β or TNFα. Given that IFNγ is secreted by cytolytic lymphocytes, which improve clinical outcomes, this role of IFNγ presents a dichotomy. To explore this conundrum, tumor NOS2, COX2, and CD8+ T cells were spatially analyzed in aggressive ER–, TNBC, and HER2 + breast tumors. High expression and clustering of NOS2-expressing tumor cells occurred at the tumor/stroma interface in the presence of stroma-restricted CD8+ T cells. High expression and clustering of COX2-expressing tumor cells extended into immune desert regions in the tumor core where CD8+ T cell penetration was limited or absent. Moreover, high NOS2-expressing tumor cells were proximal to areas with increased satellitosis, suggestive of cell clusters with a higher metastatic potential. Further in vitro experiments revealed that IFNγ + IL1β/TNFα increased the elongation and migration of treated tumor cells. This spatial analysis of the tumor microenvironment provides important insight into distinct neighborhoods where stroma-restricted CD8+ T cells exist proximal to NOS2-expressing tumor niches that could have increased metastatic potential.

UR - https://www.scopus.com/pages/publications/85159184764

UR - https://europepmc.org/articles/PMC10175544

U2 - 10.1038/s41419-023-05834-9

DO - 10.1038/s41419-023-05834-9

M3 - Article

C2 - 37169743

AN - SCOPUS:85159184764

SN - 2041-4889

VL - 14

JO - Cell Death and Disease

JF - Cell Death and Disease

IS - 5

M1 - 319

ER -

Interferon-gamma is quintessential for NOS2 and COX2 expression in ER^- breast tumors that lead to poor outcome

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