Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs

Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs

M2-like tumor-associated macrophages promote tumor progression by establishing an immunosuppressive tumor microenvironment. The phenotype and activity of immunosuppressive macrophages are related to their mitochondrial metabolism. Thus, we studied if drugs targeting mitochondrial metabolic pathways...

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Main Authors: Cesar Oyarce, Ana Vizcaino-Castro, Shipeng Chen, Annemarie Boerma, Toos Daemen
Format: Article
Language:English
Published: Taylor & Francis Group 2021-01-01
Series:OncoImmunology
Subjects:
macrophage polarization
macrophage re-polarization
immunometabolism
mitochondrial respiration
Online Access:http://dx.doi.org/10.1080/2162402X.2021.1898753
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spelling doaj-3ed9264caad847f1bfb6a4280ff40acd2021-03-18T14:42:08ZengTaylor & Francis GroupOncoImmunology2162-402X2021-01-0110110.1080/2162402X.2021.18987531898753Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugsCesar Oyarce0Ana Vizcaino-Castro1Shipeng Chen2Annemarie Boerma3Toos Daemen4University Medical Center Groningen, University of GroningenUniversity Medical Center Groningen, University of GroningenUniversity Medical Center Groningen, University of GroningenUniversity Medical Center Groningen, University of GroningenUniversity Medical Center Groningen, University of GroningenM2-like tumor-associated macrophages promote tumor progression by establishing an immunosuppressive tumor microenvironment. The phenotype and activity of immunosuppressive macrophages are related to their mitochondrial metabolism. Thus, we studied if drugs targeting mitochondrial metabolic pathways can repolarize macrophages from M2 into an M1-like phenotype or can prevent M0-to-M2 polarization. The drugs selected are clinically approved or in clinical trials and target M2-specific metabolic pathways: fatty acid oxidation (Perhexiline and Trimetazidine), glutaminolysis (CB-839), PPAR activation (HX531), and mitochondrial electron transport chain (VLX-600). Murine bone marrow-derived macrophages were either polarized to M2 using IL-4 in the presence of the drugs or polarized first into M2 and then treated with the drugs in presence of IFN-γ for re-polarization. Targeting both fatty acid oxidation with Perhexiline or the electron transport chain with VLX-600 in the presence of IFN-γ, impaired mitochondrial basal, and maximal respiration and resulted in M2 to M1-like re-polarization (increased iNOS expression, NO production, IL-23, IL-27, and TNF-α secretion), similar to LPS+IFN-γ re-polarization. Moreover, drug-induced macrophage re-polarization resulted in a strong tumor-cytotoxic activity. Furthermore, the polarization of M0- to M2-like macrophages was impaired by CB-839, Trimetazidine, HX531, and Perhexiline, while Hx531 and Perhexiline also reduced MCP-1 secretion. Our results show that by targeting cell metabolism, macrophages could be re-polarized from M2- into an anti-tumoral M1-like phenotype and that M0-to-M2 polarization could be prevented. Overall, this study provides rational for the use of clinically applicable drugs to change an immunosuppressive tumor environment into a pro-inflammatory tumor environment that could support cancer immunotherapies.http://dx.doi.org/10.1080/2162402X.2021.1898753macrophage polarizationmacrophage re-polarizationimmunometabolismmitochondrial respiration
collection DOAJ
language English
format Article
sources DOAJ
author Cesar Oyarce
Ana Vizcaino-Castro
Shipeng Chen
Annemarie Boerma
Toos Daemen
spellingShingle Cesar Oyarce
Ana Vizcaino-Castro
Shipeng Chen
Annemarie Boerma
Toos Daemen
Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
OncoImmunology
macrophage polarization
macrophage re-polarization
immunometabolism
mitochondrial respiration
author_facet Cesar Oyarce
Ana Vizcaino-Castro
Shipeng Chen
Annemarie Boerma
Toos Daemen
author_sort Cesar Oyarce
title Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
title_short Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
title_full Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
title_fullStr Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
title_full_unstemmed Re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
title_sort re-polarization of immunosuppressive macrophages to tumor-cytotoxic macrophages by repurposed metabolic drugs
publisher Taylor & Francis Group
series OncoImmunology
issn 2162-402X
publishDate 2021-01-01
description M2-like tumor-associated macrophages promote tumor progression by establishing an immunosuppressive tumor microenvironment. The phenotype and activity of immunosuppressive macrophages are related to their mitochondrial metabolism. Thus, we studied if drugs targeting mitochondrial metabolic pathways can repolarize macrophages from M2 into an M1-like phenotype or can prevent M0-to-M2 polarization. The drugs selected are clinically approved or in clinical trials and target M2-specific metabolic pathways: fatty acid oxidation (Perhexiline and Trimetazidine), glutaminolysis (CB-839), PPAR activation (HX531), and mitochondrial electron transport chain (VLX-600). Murine bone marrow-derived macrophages were either polarized to M2 using IL-4 in the presence of the drugs or polarized first into M2 and then treated with the drugs in presence of IFN-γ for re-polarization. Targeting both fatty acid oxidation with Perhexiline or the electron transport chain with VLX-600 in the presence of IFN-γ, impaired mitochondrial basal, and maximal respiration and resulted in M2 to M1-like re-polarization (increased iNOS expression, NO production, IL-23, IL-27, and TNF-α secretion), similar to LPS+IFN-γ re-polarization. Moreover, drug-induced macrophage re-polarization resulted in a strong tumor-cytotoxic activity. Furthermore, the polarization of M0- to M2-like macrophages was impaired by CB-839, Trimetazidine, HX531, and Perhexiline, while Hx531 and Perhexiline also reduced MCP-1 secretion. Our results show that by targeting cell metabolism, macrophages could be re-polarized from M2- into an anti-tumoral M1-like phenotype and that M0-to-M2 polarization could be prevented. Overall, this study provides rational for the use of clinically applicable drugs to change an immunosuppressive tumor environment into a pro-inflammatory tumor environment that could support cancer immunotherapies.
topic macrophage polarization
macrophage re-polarization
immunometabolism
mitochondrial respiration
url http://dx.doi.org/10.1080/2162402X.2021.1898753
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AT anavizcainocastro repolarizationofimmunosuppressivemacrophagestotumorcytotoxicmacrophagesbyrepurposedmetabolicdrugs
AT shipengchen repolarizationofimmunosuppressivemacrophagestotumorcytotoxicmacrophagesbyrepurposedmetabolicdrugs
AT annemarieboerma repolarizationofimmunosuppressivemacrophagestotumorcytotoxicmacrophagesbyrepurposedmetabolicdrugs
AT toosdaemen repolarizationofimmunosuppressivemacrophagestotumorcytotoxicmacrophagesbyrepurposedmetabolicdrugs
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