Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry

BACKGROUND: Oncolytic viruses are considered part of immunotherapy and have shown promise in preclinical experiments and clinical trials. Results from these studies have suggested that tumor microenvironment remodeling is required to achieve an effective response in solid tumors. Here, we assess the...

Descripción completa

Detalles Bibliográficos
Autores principales: Nguyen, Teresa T, Shin, Dong Ho, Sohoni, Sagar, Singh, Sanjay K, Rivera-Molina, Yisel, Jiang, Hong, Fan, Xuejun, Gumin, Joy, Lang, Frederick F, Alvarez-Breckenridge, Christopher, Godoy-Vitorino, Filipa, Zhu, Lisha, Zheng, W Jim, Zhai, Lijie, Ladomersky, Erik, Lauing, Kristen L, Alonso, Marta M, Wainwright, Derek A, Gomez-Manzano, Candelaria, Fueyo, Juan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2022
Materias:
Oncolytic and Local Immunotherapy
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9341188/
https://www.ncbi.nlm.nih.gov/pubmed/35902132
http://dx.doi.org/10.1136/jitc-2022-004935
_version_ 1784760559713910784
author Nguyen, Teresa T
Shin, Dong Ho
Sohoni, Sagar
Singh, Sanjay K
Rivera-Molina, Yisel
Jiang, Hong
Fan, Xuejun
Gumin, Joy
Lang, Frederick F
Alvarez-Breckenridge, Christopher
Godoy-Vitorino, Filipa
Zhu, Lisha
Zheng, W Jim
Zhai, Lijie
Ladomersky, Erik
Lauing, Kristen L
Alonso, Marta M
Wainwright, Derek A
Gomez-Manzano, Candelaria
Fueyo, Juan
author_facet Nguyen, Teresa T
Shin, Dong Ho
Sohoni, Sagar
Singh, Sanjay K
Rivera-Molina, Yisel
Jiang, Hong
Fan, Xuejun
Gumin, Joy
Lang, Frederick F
Alvarez-Breckenridge, Christopher
Godoy-Vitorino, Filipa
Zhu, Lisha
Zheng, W Jim
Zhai, Lijie
Ladomersky, Erik
Lauing, Kristen L
Alonso, Marta M
Wainwright, Derek A
Gomez-Manzano, Candelaria
Fueyo, Juan
author_sort Nguyen, Teresa T
collection PubMed
description BACKGROUND: Oncolytic viruses are considered part of immunotherapy and have shown promise in preclinical experiments and clinical trials. Results from these studies have suggested that tumor microenvironment remodeling is required to achieve an effective response in solid tumors. Here, we assess the extent to which targeting specific mechanisms underlying the immunosuppressive tumor microenvironment optimizes viroimmunotherapy. METHODS: We used RNA-seq analyses to analyze the transcriptome, and validated the results using Q-PCR, flow cytometry, and immunofluorescence. Viral activity was analyzed by replication assays and viral titration. Kyn and Trp metabolite levels were quantified using liquid chromatography–mass spectrometry. Aryl hydrocarbon receptor (AhR) activation was analyzed by examination of promoter activity. Therapeutic efficacy was assessed by tumor histopathology and survival in syngeneic murine models of gliomas, including Indoleamine 2,3-dioxygenase (IDO)-/- mice. Flow cytometry was used for immunophenotyping and quantification of cell populations. Immune activation was examined in co-cultures of immune and cancer cells. T-cell depletion was used to identify the role played by specific cell populations. Rechallenge experiments were performed to identify the development of anti-tumor memory. RESULTS: Bulk RNA-seq analyses showed the activation of the immunosuppressive IDO-kynurenine-AhR circuitry in response to Delta-24-RGDOX infection of tumors. To overcome the effect of this pivotal pathway, we combined Delta-24-RGDOX with clinically relevant IDO inhibitors. The combination therapy increased the frequency of CD8(+) T cells and decreased the rate of myeloid-derived suppressor cell and immunosupressive Treg tumor populations in animal models of solid tumors. Functional studies demonstrated that IDO-blockade-dependent activation of immune cells against tumor antigens could be reversed by the oncometabolite kynurenine. The concurrent targeting of the effectors and suppressors of the tumor immune landscape significantly prolonged the survival in animal models of orthotopic gliomas. CONCLUSIONS: Our data identified for the first time the in vivo role of IDO-dependent immunosuppressive pathways in the resistance of solid tumors to oncolytic adenoviruses. Specifically, the IDO-Kyn-AhR activity was responsible for the resurface of local immunosuppression and resistance to therapy, which was ablated through IDO inhibition. Our data indicate that combined molecular and immune therapy may improve outcomes in human gliomas and other cancers treated with virotherapy.
format Online
Article
Text
id pubmed-9341188
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher BMJ Publishing Group
record_format MEDLINE/PubMed
spelling pubmed-93411882022-08-17 Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry Nguyen, Teresa T Shin, Dong Ho Sohoni, Sagar Singh, Sanjay K Rivera-Molina, Yisel Jiang, Hong Fan, Xuejun Gumin, Joy Lang, Frederick F Alvarez-Breckenridge, Christopher Godoy-Vitorino, Filipa Zhu, Lisha Zheng, W Jim Zhai, Lijie Ladomersky, Erik Lauing, Kristen L Alonso, Marta M Wainwright, Derek A Gomez-Manzano, Candelaria Fueyo, Juan J Immunother Cancer Oncolytic and Local Immunotherapy BACKGROUND: Oncolytic viruses are considered part of immunotherapy and have shown promise in preclinical experiments and clinical trials. Results from these studies have suggested that tumor microenvironment remodeling is required to achieve an effective response in solid tumors. Here, we assess the extent to which targeting specific mechanisms underlying the immunosuppressive tumor microenvironment optimizes viroimmunotherapy. METHODS: We used RNA-seq analyses to analyze the transcriptome, and validated the results using Q-PCR, flow cytometry, and immunofluorescence. Viral activity was analyzed by replication assays and viral titration. Kyn and Trp metabolite levels were quantified using liquid chromatography–mass spectrometry. Aryl hydrocarbon receptor (AhR) activation was analyzed by examination of promoter activity. Therapeutic efficacy was assessed by tumor histopathology and survival in syngeneic murine models of gliomas, including Indoleamine 2,3-dioxygenase (IDO)-/- mice. Flow cytometry was used for immunophenotyping and quantification of cell populations. Immune activation was examined in co-cultures of immune and cancer cells. T-cell depletion was used to identify the role played by specific cell populations. Rechallenge experiments were performed to identify the development of anti-tumor memory. RESULTS: Bulk RNA-seq analyses showed the activation of the immunosuppressive IDO-kynurenine-AhR circuitry in response to Delta-24-RGDOX infection of tumors. To overcome the effect of this pivotal pathway, we combined Delta-24-RGDOX with clinically relevant IDO inhibitors. The combination therapy increased the frequency of CD8(+) T cells and decreased the rate of myeloid-derived suppressor cell and immunosupressive Treg tumor populations in animal models of solid tumors. Functional studies demonstrated that IDO-blockade-dependent activation of immune cells against tumor antigens could be reversed by the oncometabolite kynurenine. The concurrent targeting of the effectors and suppressors of the tumor immune landscape significantly prolonged the survival in animal models of orthotopic gliomas. CONCLUSIONS: Our data identified for the first time the in vivo role of IDO-dependent immunosuppressive pathways in the resistance of solid tumors to oncolytic adenoviruses. Specifically, the IDO-Kyn-AhR activity was responsible for the resurface of local immunosuppression and resistance to therapy, which was ablated through IDO inhibition. Our data indicate that combined molecular and immune therapy may improve outcomes in human gliomas and other cancers treated with virotherapy. BMJ Publishing Group 2022-07-28 /pmc/articles/PMC9341188/ /pubmed/35902132 http://dx.doi.org/10.1136/jitc-2022-004935 Text en © Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. https://creativecommons.org/licenses/by-nc/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) .
spellingShingle Oncolytic and Local Immunotherapy
Nguyen, Teresa T
Shin, Dong Ho
Sohoni, Sagar
Singh, Sanjay K
Rivera-Molina, Yisel
Jiang, Hong
Fan, Xuejun
Gumin, Joy
Lang, Frederick F
Alvarez-Breckenridge, Christopher
Godoy-Vitorino, Filipa
Zhu, Lisha
Zheng, W Jim
Zhai, Lijie
Ladomersky, Erik
Lauing, Kristen L
Alonso, Marta M
Wainwright, Derek A
Gomez-Manzano, Candelaria
Fueyo, Juan
Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title_full Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title_fullStr Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title_full_unstemmed Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title_short Reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
title_sort reshaping the tumor microenvironment with oncolytic viruses, positive regulation of the immune synapse, and blockade of the immunosuppressive oncometabolic circuitry
topic Oncolytic and Local Immunotherapy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9341188/
https://www.ncbi.nlm.nih.gov/pubmed/35902132
http://dx.doi.org/10.1136/jitc-2022-004935
work_keys_str_mv AT nguyenteresat reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT shindongho reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT sohonisagar reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT singhsanjayk reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT riveramolinayisel reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT jianghong reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT fanxuejun reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT guminjoy reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT langfrederickf reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT alvarezbreckenridgechristopher reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT godoyvitorinofilipa reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT zhulisha reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT zhengwjim reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT zhailijie reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT ladomerskyerik reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT lauingkristenl reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT alonsomartam reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT wainwrightdereka reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT gomezmanzanocandelaria reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry
AT fueyojuan reshapingthetumormicroenvironmentwithoncolyticvirusespositiveregulationoftheimmunesynapseandblockadeoftheimmunosuppressiveoncometaboliccircuitry

Ejemplares similares