Literature DB >> 32350590

Blockade of CD73 delays glioblastoma growth by modulating the immune environment.

J H Azambuja1, R S Schuh2, L R Michels2, I C Iser3, L R Beckenkamp1, G G Roliano3, G S Lenz1, J N Scholl4,5, J Sévigny6,7, M R Wink1,3, M A Stefani8, A M O Battastini5, F Figueiró4,5, H F Teixeira2, E Braganhol9,10.   

Abstract

Immunotherapy as an approach for cancer treatment is clinically promising. CD73, which is the enzyme that produces extracellular adenosine, favors cancer progression and protects the tumor from immune surveillance. While CD73 has recently been demonstrated to be a potential target for glioma treatment, its role in regulating the inflammatory tumor microenvironment has not yet been investigated. Thus, this study explores the immunotherapeutic value of the CD73 blockade in glioblastoma. The immuno-therapeutic value of the CD73 blockade was evaluated in vivo in immunocompetent pre-clinical glioblastoma model. As such, glioblastoma-bearing rats were nasally treated for 15 days with a siRNA CD73-loaded cationic-nanoemulsion (NE-siRNA CD73R). Apoptosis was determined by flow cytometry using Annexin-V staining and cell proliferation was analyzed by Ki67 expression by immunohistochemistry. The frequencies of the CD4+, CD8+, and CD4+CD25highCD39+ (Treg) T lymphocytes; CD11b+CD45high macrophages; CD11b+CD45low-microglia; and CD206+-M2-like phenotypes, along with expression levels of CD39 and CD73 in tumor and tumor-associated immune cells, were determined using flow cytometry, while inflammatory markers associated with tumor progression were evaluated using RT-qPCR. The CD73 blockade by NE-siRNA CD73 was found to induce tumor cell apoptosis. Meanwhile, the population of Tregs, microglia, and macrophages was significantly reduced in the tumor microenvironment, though IL-6, CCL17, and CCL22 increased. The treatment selectively decreased CD73 expression in the GB cells as well as in the tumor-associated-macrophages/microglia. This study indicates that CD73 knockdown using a nanotechnological approach to perform nasal delivery of siRNA-CD73 to CNS can potentially regulate the glioblastoma immune microenvironment and delay tumor growth by inducing apoptosis.

Entities:  

Keywords:  Ecto-5′-nucleotidase/CD73; Glioblastoma; Immunotherapy; Macrophages; Microglia; T regulatory lymphocytes

Mesh:

Substances:

Year:  2020        PMID: 32350590     DOI: 10.1007/s00262-020-02569-w

Source DB:  PubMed          Journal:  Cancer Immunol Immunother        ISSN: 0340-7004            Impact factor:   6.968


  35 in total

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Review 2.  Role of Macrophages in Brain Tumor Growth and Progression.

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Review 3.  Chemoresistance caused by the microenvironment of glioblastoma and the corresponding solutions.

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Journal:  Biomed Pharmacother       Date:  2018-11-02       Impact factor: 6.529

Review 4.  Immunotherapy in Gliomas.

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Journal:  Semin Oncol Nurs       Date:  2018-11-02       Impact factor: 2.315

5.  Glioma sensitive or chemoresistant to temozolomide differentially modulate macrophage protumor activities.

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Review 6.  Tissue is the Issue: Biomarkers of Prognosis and Classification in Adult Gliomas.

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Review 7.  The epidemiology of glioma in adults: a "state of the science" review.

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Review 8.  The possibility of cancer immune editing in gliomas. A critical review.

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Journal:  Oncoimmunology       Date:  2018-04-09       Impact factor: 8.110

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Review 3.  Distinction of Microglia and Macrophages in Glioblastoma: Close Relatives, Different Tasks?

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Journal:  Int J Mol Sci       Date:  2020-12-27       Impact factor: 5.923

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Review 6.  Dendritic Cell Vaccination of Glioblastoma: Road to Success or Dead End.

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7.  CD73-positive extracellular vesicles promote glioblastoma immunosuppression by inhibiting T-cell clonal expansion.

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Journal:  Cell Death Dis       Date:  2021-11-09       Impact factor: 8.469

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9.  Generation of a Retargeted Oncolytic Herpes Virus Encoding Adenosine Deaminase for Tumor Adenosine Clearance.

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Review 10.  Adenosinergic Signaling as a Key Modulator of the Glioma Microenvironment and Reactive Astrocytes.

Authors:  Gabriela N Debom; Dominique S Rubenich; Elizandra Braganhol
Journal:  Front Neurosci       Date:  2022-01-05       Impact factor: 4.677

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