Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas

The reciprocal relationship between malignant T cells and lymphoma-associated macrophages (LAM) within the tumor microenvironment (TME) is unique, as LAMs are well poised to provide ligands for antigen, costimulatory, and cytokine receptors that promote T-cell lymphoma growth. Conversely, malignant...

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Autores principales: Gao, Xin, Kady, Nermin, Wang, Chenguang, Abdelrahman, Suhaib, Gann, Peter, Sverdlov, Maria, Wolfe, Ashley, Brown, Noah, Reneau, John, Robida, Aaron M., Murga-Zamalloa, Carlos, Wilcox, Ryan A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10035520/
https://www.ncbi.nlm.nih.gov/pubmed/36970721
http://dx.doi.org/10.1158/2767-9764.CRC-22-0336
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author Gao, Xin
Kady, Nermin
Wang, Chenguang
Abdelrahman, Suhaib
Gann, Peter
Sverdlov, Maria
Wolfe, Ashley
Brown, Noah
Reneau, John
Robida, Aaron M.
Murga-Zamalloa, Carlos
Wilcox, Ryan A.
author_facet Gao, Xin
Kady, Nermin
Wang, Chenguang
Abdelrahman, Suhaib
Gann, Peter
Sverdlov, Maria
Wolfe, Ashley
Brown, Noah
Reneau, John
Robida, Aaron M.
Murga-Zamalloa, Carlos
Wilcox, Ryan A.
author_sort Gao, Xin
collection PubMed
description The reciprocal relationship between malignant T cells and lymphoma-associated macrophages (LAM) within the tumor microenvironment (TME) is unique, as LAMs are well poised to provide ligands for antigen, costimulatory, and cytokine receptors that promote T-cell lymphoma growth. Conversely, malignant T cells promote the functional polarization and homeostatic survival of LAM. Therefore, we sought to determine the extent to which LAMs are a therapeutic vulnerability in these lymphomas, and to identify effective therapeutic strategies for their depletion. We utilized complementary genetically engineered mouse models and primary peripheral T-cell lymphoma (PTCL) specimens to quantify LAM expansion and proliferation. A high-throughput screen was performed to identify targeted agents that effectively deplete LAM within the context of PTCL. We observed that LAMs are dominant constituents of the TME in PTCL. Furthermore, their dominance was explained, at least in part, by their proliferation and expansion in response to PTCL-derived cytokines. Importantly, LAMs are a true dependency in these lymphomas, as their depletion significantly impaired PTCL progression. These findings were extrapolated to a large cohort of human PTCL specimens where LAM proliferation was observed. A high-throughput screen demonstrated that PTCL-derived cytokines led to relative resistance to CSF1R selective inhibitors, and culminated in the identification of dual CSF1R/JAK inhibition as a novel therapeutic strategy to deplete LAM in these aggressive lymphomas. Malignant T cells promote the expansion and proliferation of LAM, which are a bone fide dependency in these lymphomas, and are effectively depleted with a dual CSF1R/JAK inhibitor. SIGNIFICANCE: LAMs are a therapeutic vulnerability, as their depletion impairs T-cell lymphoma disease progression. Pacritinib, a dual CSF1R/JAK inhibitor, effectively impaired LAM viability and expansion, prolonged survival in preclinical T-cell lymphoma models, and is currently being investigated as a novel therapeutic approach in these lymphomas.
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spelling pubmed-100355202023-03-24 Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas Gao, Xin Kady, Nermin Wang, Chenguang Abdelrahman, Suhaib Gann, Peter Sverdlov, Maria Wolfe, Ashley Brown, Noah Reneau, John Robida, Aaron M. Murga-Zamalloa, Carlos Wilcox, Ryan A. Cancer Res Commun Research Article The reciprocal relationship between malignant T cells and lymphoma-associated macrophages (LAM) within the tumor microenvironment (TME) is unique, as LAMs are well poised to provide ligands for antigen, costimulatory, and cytokine receptors that promote T-cell lymphoma growth. Conversely, malignant T cells promote the functional polarization and homeostatic survival of LAM. Therefore, we sought to determine the extent to which LAMs are a therapeutic vulnerability in these lymphomas, and to identify effective therapeutic strategies for their depletion. We utilized complementary genetically engineered mouse models and primary peripheral T-cell lymphoma (PTCL) specimens to quantify LAM expansion and proliferation. A high-throughput screen was performed to identify targeted agents that effectively deplete LAM within the context of PTCL. We observed that LAMs are dominant constituents of the TME in PTCL. Furthermore, their dominance was explained, at least in part, by their proliferation and expansion in response to PTCL-derived cytokines. Importantly, LAMs are a true dependency in these lymphomas, as their depletion significantly impaired PTCL progression. These findings were extrapolated to a large cohort of human PTCL specimens where LAM proliferation was observed. A high-throughput screen demonstrated that PTCL-derived cytokines led to relative resistance to CSF1R selective inhibitors, and culminated in the identification of dual CSF1R/JAK inhibition as a novel therapeutic strategy to deplete LAM in these aggressive lymphomas. Malignant T cells promote the expansion and proliferation of LAM, which are a bone fide dependency in these lymphomas, and are effectively depleted with a dual CSF1R/JAK inhibitor. SIGNIFICANCE: LAMs are a therapeutic vulnerability, as their depletion impairs T-cell lymphoma disease progression. Pacritinib, a dual CSF1R/JAK inhibitor, effectively impaired LAM viability and expansion, prolonged survival in preclinical T-cell lymphoma models, and is currently being investigated as a novel therapeutic approach in these lymphomas. American Association for Cancer Research 2022-12-30 /pmc/articles/PMC10035520/ /pubmed/36970721 http://dx.doi.org/10.1158/2767-9764.CRC-22-0336 Text en © 2022 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by/4.0/This open access article is distributed under the Creative Commons Attribution 4.0 International (CC BY 4.0) license.
spellingShingle Research Article
Gao, Xin
Kady, Nermin
Wang, Chenguang
Abdelrahman, Suhaib
Gann, Peter
Sverdlov, Maria
Wolfe, Ashley
Brown, Noah
Reneau, John
Robida, Aaron M.
Murga-Zamalloa, Carlos
Wilcox, Ryan A.
Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title_full Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title_fullStr Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title_full_unstemmed Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title_short Targeting Lymphoma-associated Macrophage Expansion via CSF1R/JAK Inhibition is a Therapeutic Vulnerability in Peripheral T-cell Lymphomas
title_sort targeting lymphoma-associated macrophage expansion via csf1r/jak inhibition is a therapeutic vulnerability in peripheral t-cell lymphomas
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10035520/
https://www.ncbi.nlm.nih.gov/pubmed/36970721
http://dx.doi.org/10.1158/2767-9764.CRC-22-0336
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