Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling

While immunotherapies such as immune checkpoint blockade and adoptive T-cell therapy improve survival for a subset of human malignancies, many patients fail to respond. Phagocytes including dendritic cells (DC), monocytes, and macrophages (MF) orchestrate innate and adaptive immune responses against...

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Autores principales: Matos, Israel, Barvalia, Maunish, Chehal, Manreet K., Robertson, A. Gordon, Kulic, Iva, Silva, Jessica A.F.D., Ranganathan, Abhinandan, Short, Amy, Huang, Yu-Hsuan, Long, Erin, Priatel, John J., Dhanji, Salim, Nelson, Brad H., Krebs, Danielle L., Harder, Kenneth W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9997410/
https://www.ncbi.nlm.nih.gov/pubmed/36911097
http://dx.doi.org/10.1158/2767-9764.CRC-22-0278
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author Matos, Israel
Barvalia, Maunish
Chehal, Manreet K.
Robertson, A. Gordon
Kulic, Iva
Silva, Jessica A.F.D.
Ranganathan, Abhinandan
Short, Amy
Huang, Yu-Hsuan
Long, Erin
Priatel, John J.
Dhanji, Salim
Nelson, Brad H.
Krebs, Danielle L.
Harder, Kenneth W.
author_facet Matos, Israel
Barvalia, Maunish
Chehal, Manreet K.
Robertson, A. Gordon
Kulic, Iva
Silva, Jessica A.F.D.
Ranganathan, Abhinandan
Short, Amy
Huang, Yu-Hsuan
Long, Erin
Priatel, John J.
Dhanji, Salim
Nelson, Brad H.
Krebs, Danielle L.
Harder, Kenneth W.
author_sort Matos, Israel
collection PubMed
description While immunotherapies such as immune checkpoint blockade and adoptive T-cell therapy improve survival for a subset of human malignancies, many patients fail to respond. Phagocytes including dendritic cells (DC), monocytes, and macrophages (MF) orchestrate innate and adaptive immune responses against tumors. However, tumor-derived factors may limit immunotherapy effectiveness by altering phagocyte signal transduction, development, and activity. Using Cytometry by Time-of-Flight, we found that tumor-derived GCSF altered myeloid cell distribution both locally and systemically. We distinguished a large number of GCSF-induced immune cell subset and signal transduction pathway perturbations in tumor-bearing mice, including a prominent increase in immature neutrophil/myeloid-derived suppressor cell (Neut/MDSC) subsets and tumor-resident PD-L1(+) Neut/MDSCs. GCSF expression was also linked to distinct tumor-associated MF populations, decreased conventional DCs, and splenomegaly characterized by increased splenic progenitors with diminished DC differentiation potential. GCSF-dependent dysregulation of DC development was recapitulated in bone marrow cultures in vitro, using medium derived from GCSF-expressing tumor cell cultures. Importantly, tumor-derived GCSF impaired T-cell adoptive cell therapy effectiveness and was associated with increased tumor volume and diminished survival of mice with mammary cancer. Treatment with neutralizing anti-GCSF antibodies reduced colonic and circulatory Neut/MDSCs, normalized colonic immune cell composition and diminished tumor burden in a spontaneous model of mouse colon cancer. Analysis of human colorectal cancer patient gene expression data revealed a significant correlation between survival and low GCSF and Neut/MDSC gene expression. Our data suggest that normalizing GCSF bioactivity may improve immunotherapy in cancers associated with GCSF overexpression. SIGNIFICANCE: Tumor-derived GCSF leads to systemic immune population changes. GCSF blockade restores immune populations, improves immunotherapy, and reduces tumor size, paralleling human colorectal cancer data. GCSF inhibition may synergize with current immunotherapies to treat GCSF-secreting tumors.
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spelling pubmed-99974102023-03-10 Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling Matos, Israel Barvalia, Maunish Chehal, Manreet K. Robertson, A. Gordon Kulic, Iva Silva, Jessica A.F.D. Ranganathan, Abhinandan Short, Amy Huang, Yu-Hsuan Long, Erin Priatel, John J. Dhanji, Salim Nelson, Brad H. Krebs, Danielle L. Harder, Kenneth W. Cancer Res Commun Research Article While immunotherapies such as immune checkpoint blockade and adoptive T-cell therapy improve survival for a subset of human malignancies, many patients fail to respond. Phagocytes including dendritic cells (DC), monocytes, and macrophages (MF) orchestrate innate and adaptive immune responses against tumors. However, tumor-derived factors may limit immunotherapy effectiveness by altering phagocyte signal transduction, development, and activity. Using Cytometry by Time-of-Flight, we found that tumor-derived GCSF altered myeloid cell distribution both locally and systemically. We distinguished a large number of GCSF-induced immune cell subset and signal transduction pathway perturbations in tumor-bearing mice, including a prominent increase in immature neutrophil/myeloid-derived suppressor cell (Neut/MDSC) subsets and tumor-resident PD-L1(+) Neut/MDSCs. GCSF expression was also linked to distinct tumor-associated MF populations, decreased conventional DCs, and splenomegaly characterized by increased splenic progenitors with diminished DC differentiation potential. GCSF-dependent dysregulation of DC development was recapitulated in bone marrow cultures in vitro, using medium derived from GCSF-expressing tumor cell cultures. Importantly, tumor-derived GCSF impaired T-cell adoptive cell therapy effectiveness and was associated with increased tumor volume and diminished survival of mice with mammary cancer. Treatment with neutralizing anti-GCSF antibodies reduced colonic and circulatory Neut/MDSCs, normalized colonic immune cell composition and diminished tumor burden in a spontaneous model of mouse colon cancer. Analysis of human colorectal cancer patient gene expression data revealed a significant correlation between survival and low GCSF and Neut/MDSC gene expression. Our data suggest that normalizing GCSF bioactivity may improve immunotherapy in cancers associated with GCSF overexpression. SIGNIFICANCE: Tumor-derived GCSF leads to systemic immune population changes. GCSF blockade restores immune populations, improves immunotherapy, and reduces tumor size, paralleling human colorectal cancer data. GCSF inhibition may synergize with current immunotherapies to treat GCSF-secreting tumors. American Association for Cancer Research 2023-03-09 /pmc/articles/PMC9997410/ /pubmed/36911097 http://dx.doi.org/10.1158/2767-9764.CRC-22-0278 Text en © 2023 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
Matos, Israel
Barvalia, Maunish
Chehal, Manreet K.
Robertson, A. Gordon
Kulic, Iva
Silva, Jessica A.F.D.
Ranganathan, Abhinandan
Short, Amy
Huang, Yu-Hsuan
Long, Erin
Priatel, John J.
Dhanji, Salim
Nelson, Brad H.
Krebs, Danielle L.
Harder, Kenneth W.
Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title_full Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title_fullStr Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title_full_unstemmed Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title_short Tumor-derived GCSF Alters Tumor and Systemic Immune System Cell Subset Composition and Signaling
title_sort tumor-derived gcsf alters tumor and systemic immune system cell subset composition and signaling
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9997410/
https://www.ncbi.nlm.nih.gov/pubmed/36911097
http://dx.doi.org/10.1158/2767-9764.CRC-22-0278
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