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Glioblastoma hijacks microglial gene expression to support tumor growth
Glioblastoma hijacks microglial gene expression to support tumor growth
by Zhang, Xuan , Morsett, Liza , El Khoury, Joseph , Sen, Pritha , Breakefield, Xandra O. , Maas, Sybren L. N. , Hickman, Suzanne E. , Van De Haar, Lieke L. , Guedes, Joana , Abels, Erik R. , Ting, David T. , Broekman, Marike L. D. , Lai, Charles P. , Sil, Srinjoy , Prabhakar, Shilpa
in Animals / Biomedical and Life Sciences / Biomedicine / Brain cancer / Brain Neoplasms - genetics / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / Brain tumors / Cell Line, Tumor / Development and progression / Exosomes / Extracellular vesicles / Extracellular Vesicles - genetics / Extracellular Vesicles - metabolism / Extracellular Vesicles - pathology / Female / Females / Gene expression / Gene Expression Regulation, Neoplastic / Gene Knock-In Techniques - methods / Genetic aspects / Genetic transformation / Glioblastoma / Glioblastoma - genetics / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / Glioblastomas / Glioma / Health aspects / Immune response / Immune system / Immunoglobulins / Immunology / Male / Mice / Mice, Inbred C57BL / Mice, Transgenic / Microglia / Microglia - metabolism / Microglia - pathology / Microvesicles / Neurobiology / Neurology / Neurosciences / Organelles / Penicillin / Phenotypes / Physiological aspects / Proteins / Transcription / Transcriptomics / Tumor Burden - physiology / Tumor cells / Tumors
2020
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Glioblastoma hijacks microglial gene expression to support tumor growth
by Zhang, Xuan , Morsett, Liza , El Khoury, Joseph , Sen, Pritha , Breakefield, Xandra O. , Maas, Sybren L. N. , Hickman, Suzanne E. , Van De Haar, Lieke L. , Guedes, Joana , Abels, Erik R. , Ting, David T. , Broekman, Marike L. D. , Lai, Charles P. , Sil, Srinjoy , Prabhakar, Shilpa
in Animals / Biomedical and Life Sciences / Biomedicine / Brain cancer / Brain Neoplasms - genetics / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / Brain tumors / Cell Line, Tumor / Development and progression / Exosomes / Extracellular vesicles / Extracellular Vesicles - genetics / Extracellular Vesicles - metabolism / Extracellular Vesicles - pathology / Female / Females / Gene expression / Gene Expression Regulation, Neoplastic / Gene Knock-In Techniques - methods / Genetic aspects / Genetic transformation / Glioblastoma / Glioblastoma - genetics / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / Glioblastomas / Glioma / Health aspects / Immune response / Immune system / Immunoglobulins / Immunology / Male / Mice / Mice, Inbred C57BL / Mice, Transgenic / Microglia / Microglia - metabolism / Microglia - pathology / Microvesicles / Neurobiology / Neurology / Neurosciences / Organelles / Penicillin / Phenotypes / Physiological aspects / Proteins / Transcription / Transcriptomics / Tumor Burden - physiology / Tumor cells / Tumors
2020
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Glioblastoma hijacks microglial gene expression to support tumor growth
Glioblastoma hijacks microglial gene expression to support tumor growth
by Zhang, Xuan , Morsett, Liza , El Khoury, Joseph , Sen, Pritha , Breakefield, Xandra O. , Maas, Sybren L. N. , Hickman, Suzanne E. , Van De Haar, Lieke L. , Guedes, Joana , Abels, Erik R. , Ting, David T. , Broekman, Marike L. D. , Lai, Charles P. , Sil, Srinjoy , Prabhakar, Shilpa
in Animals / Biomedical and Life Sciences / Biomedicine / Brain cancer / Brain Neoplasms - genetics / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / Brain tumors / Cell Line, Tumor / Development and progression / Exosomes / Extracellular vesicles / Extracellular Vesicles - genetics / Extracellular Vesicles - metabolism / Extracellular Vesicles - pathology / Female / Females / Gene expression / Gene Expression Regulation, Neoplastic / Gene Knock-In Techniques - methods / Genetic aspects / Genetic transformation / Glioblastoma / Glioblastoma - genetics / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / Glioblastomas / Glioma / Health aspects / Immune response / Immune system / Immunoglobulins / Immunology / Male / Mice / Mice, Inbred C57BL / Mice, Transgenic / Microglia / Microglia - metabolism / Microglia - pathology / Microvesicles / Neurobiology / Neurology / Neurosciences / Organelles / Penicillin / Phenotypes / Physiological aspects / Proteins / Transcription / Transcriptomics / Tumor Burden - physiology / Tumor cells / Tumors
2020

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Glioblastoma hijacks microglial gene expression to support tumor growth
Glioblastoma hijacks microglial gene expression to support tumor growth
Journal Article

Glioblastoma hijacks microglial gene expression to support tumor growth

Zhang, Xuan,
Morsett, Liza,
El Khoury, Joseph,
Sen, Pritha,
Breakefield, Xandra O.,
Maas, Sybren L. N.,
Hickman, Suzanne E.,
Van De Haar, Lieke L.,
Guedes, Joana,
Abels, Erik R.,
Ting, David T.,
Broekman, Marike L. D.,
Lai, Charles P.,
Sil, Srinjoy,
Prabhakar, Shilpa
2020
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Overview
Background Glioblastomas are the most common and lethal primary brain tumors. Microglia, the resident immune cells of the brain, survey their environment and respond to pathogens, toxins, and tumors. Glioblastoma cells communicate with microglia, in part by releasing extracellular vesicles (EVs). Despite the presence of large numbers of microglia in glioblastoma, the tumors continue to grow, and these neuroimmune cells appear incapable of keeping the tumor in check. To understand this process, we analyzed gene expression in microglia interacting with glioblastoma cells . Methods We used RNASeq of isolated microglia to analyze the expression patterns of genes involved in key microglial functions in mice with glioblastoma. We focused on microglia that had taken up tumor-derived EVs and therefore were within and immediately adjacent to the tumor. Results We show that these microglia have downregulated expression of genes involved in sensing tumor cells and tumor-derived danger signals, as well as genes used for tumor killing. In contrast, expression of genes involved in facilitating tumor spread was upregulated. These changes appear to be in part EV-mediated, since intracranial injection of EVs in normal mice led to similar transcriptional changes in microglia. We observed a similar microglial transcriptomic signature when we analyzed datasets from human patients with glioblastoma. Conclusion Our data define a microglia Glioblastoma specific phenotype, whereby glioblastomas have hijacked gene expression in the neuroimmune system to favor avoiding tumor sensing, suppressing the immune response, clearing a path for invasion, and enhancing tumor propagation. For further exploration, we developed an interactive online tool at http://www.glioma-microglia.com with all expression data and additional functional and pathway information for each gene.
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Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject

Animals

/ Biomedical and Life Sciences

/ Biomedicine

/ Brain cancer

/ Brain Neoplasms - genetics

/ Brain Neoplasms - metabolism

/ Brain Neoplasms - pathology

/ Brain tumors

/ Cell Line, Tumor

/ Development and progression

/ Exosomes

/ Extracellular vesicles

/ Extracellular Vesicles - genetics

/ Extracellular Vesicles - metabolism

/ Extracellular Vesicles - pathology

/ Female

/ Females

/ Gene expression

/ Gene Expression Regulation, Neoplastic

/ Gene Knock-In Techniques - methods

/ Genetic aspects

/ Genetic transformation

/ Glioblastoma

/ Glioblastoma - genetics

/ Glioblastoma - metabolism

/ Glioblastoma - pathology

/ Glioblastoma cells

/ Glioblastomas

/ Glioma

/ Health aspects

/ Immune response

/ Immune system

/ Immunoglobulins

/ Immunology

/ Male

/ Mice

/ Mice, Inbred C57BL

/ Mice, Transgenic

/ Microglia

/ Microglia - metabolism

/ Microglia - pathology

/ Microvesicles

/ Neurobiology

/ Neurology

/ Neurosciences

/ Organelles

/ Penicillin

/ Phenotypes

/ Physiological aspects

/ Proteins

/ Transcription

/ Transcriptomics

/ Tumor Burden - physiology

/ Tumor cells

/ Tumors

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