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Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
by Meng, Chen , Pfaffl, Michael W. , Proescholdt, Martin , Riemenschneider, Markus J. , Reithmair, Marlene , Steinlein, Ortrud K. , Ludwig, Christina , Kirchner, Benedikt , Grätz, Christian , Braun, Frank K. , Schuster, Martina , Chiang, Dapi Meng-Lin , Hau, Peter
in 3D organoid model / Antibodies / Biomarkers / Brain cancer / Brain Neoplasms - immunology / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / CD63 antigen / CD81 antigen / CD9 antigen / Cell culture / Cell Culture Techniques, Three Dimensional - methods / Cell interactions / Cell Line, Tumor / Cells / Communications systems / Data analysis / Extracellular matrix / extracellular vesicle / Extracellular vesicles / Extracellular Vesicles - immunology / Extracellular Vesicles - metabolism / Females / Flow cytometry / Gene expression / Gene Expression Regulation, Neoplastic / Glioblastoma - immunology / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / glioblastoma multiforme / Glioma / Growth factors / Humans / Immune response / Immunology / Malignancy / Mass spectroscopy / microRNA / MicroRNAs / MicroRNAs - genetics / miRNA / Organoids / Organoids - immunology / Preadipocyte factor 1 / Proteomes / Signal Transduction / Tumor Cells, Cultured / Tumor microenvironment / Tumor Microenvironment - immunology / Tumors
2024
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Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
by Meng, Chen , Pfaffl, Michael W. , Proescholdt, Martin , Riemenschneider, Markus J. , Reithmair, Marlene , Steinlein, Ortrud K. , Ludwig, Christina , Kirchner, Benedikt , Grätz, Christian , Braun, Frank K. , Schuster, Martina , Chiang, Dapi Meng-Lin , Hau, Peter
in 3D organoid model / Antibodies / Biomarkers / Brain cancer / Brain Neoplasms - immunology / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / CD63 antigen / CD81 antigen / CD9 antigen / Cell culture / Cell Culture Techniques, Three Dimensional - methods / Cell interactions / Cell Line, Tumor / Cells / Communications systems / Data analysis / Extracellular matrix / extracellular vesicle / Extracellular vesicles / Extracellular Vesicles - immunology / Extracellular Vesicles - metabolism / Females / Flow cytometry / Gene expression / Gene Expression Regulation, Neoplastic / Glioblastoma - immunology / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / glioblastoma multiforme / Glioma / Growth factors / Humans / Immune response / Immunology / Malignancy / Mass spectroscopy / microRNA / MicroRNAs / MicroRNAs - genetics / miRNA / Organoids / Organoids - immunology / Preadipocyte factor 1 / Proteomes / Signal Transduction / Tumor Cells, Cultured / Tumor microenvironment / Tumor Microenvironment - immunology / Tumors
2024
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Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
by Meng, Chen , Pfaffl, Michael W. , Proescholdt, Martin , Riemenschneider, Markus J. , Reithmair, Marlene , Steinlein, Ortrud K. , Ludwig, Christina , Kirchner, Benedikt , Grätz, Christian , Braun, Frank K. , Schuster, Martina , Chiang, Dapi Meng-Lin , Hau, Peter
in 3D organoid model / Antibodies / Biomarkers / Brain cancer / Brain Neoplasms - immunology / Brain Neoplasms - metabolism / Brain Neoplasms - pathology / CD63 antigen / CD81 antigen / CD9 antigen / Cell culture / Cell Culture Techniques, Three Dimensional - methods / Cell interactions / Cell Line, Tumor / Cells / Communications systems / Data analysis / Extracellular matrix / extracellular vesicle / Extracellular vesicles / Extracellular Vesicles - immunology / Extracellular Vesicles - metabolism / Females / Flow cytometry / Gene expression / Gene Expression Regulation, Neoplastic / Glioblastoma - immunology / Glioblastoma - metabolism / Glioblastoma - pathology / Glioblastoma cells / glioblastoma multiforme / Glioma / Growth factors / Humans / Immune response / Immunology / Malignancy / Mass spectroscopy / microRNA / MicroRNAs / MicroRNAs - genetics / miRNA / Organoids / Organoids - immunology / Preadipocyte factor 1 / Proteomes / Signal Transduction / Tumor Cells, Cultured / Tumor microenvironment / Tumor Microenvironment - immunology / Tumors
2024

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Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems
Journal Article

Extracellular vesicles secreted by 3D tumor organoids are enriched for immune regulatory signaling biomolecules compared to conventional 2D glioblastoma cell systems

Meng, Chen,
Pfaffl, Michael W.,
Proescholdt, Martin,
Riemenschneider, Markus J.,
Reithmair, Marlene,
Steinlein, Ortrud K.,
Ludwig, Christina,
Kirchner, Benedikt,
Grätz, Christian,
Braun, Frank K.,
Schuster, Martina,
Chiang, Dapi Meng-Lin,
Hau, Peter
2024
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Overview
Newer 3D culturing approaches are a promising way to better mimic the tumor microenvironment and to study the interactions between the heterogeneous cell populations of glioblastoma multiforme. Like many other tumors, glioblastoma uses extracellular vesicles as an intercellular communication system to prepare surrounding tissue for invasive tumor growth. However, little is known about the effects of 3D culture on extracellular vesicles. The aim of this study was to comprehensively characterize extracellular vesicles in 3D organoid models and compare them to conventional 2D cell culture systems. Primary glioblastoma cells were cultured as 2D and 3D organoid models. Extracellular vesicles were obtained by precipitation and immunoaffinity, with the latter allowing targeted isolation of the CD9/CD63/CD81 vesicle subpopulation. Comprehensive vesicle characterization was performed and miRNA expression profiles were generated by smallRNA-sequencing. analysis of differentially regulated miRNAs was performed to identify mRNA targets and corresponding signaling pathways. The tumor cell media and extracellular vesicle proteome were analyzed by high-resolution mass spectrometry. We observed an increased concentration of extracellular vesicles in 3D organoid cultures. Differential gene expression analysis further revealed the regulation of twelve miRNAs in 3D tumor organoid cultures (with nine miRNAs down and three miRNAs upregulated). MiR-23a-3p, known to be involved in glioblastoma invasion, was significantly increased in 3D. MiR-7-5p, which counteracts glioblastoma malignancy, was significantly decreased. Moreover, we identified four miRNAs (miR-323a-3p, miR-382-5p, miR-370-3p, miR-134-5p) located within the DLK1-DIO3 domain, a cancer-associated genomic region, suggesting a possible importance of this region in glioblastoma progression. Overrepresentation analysis identified alterations of extracellular vesicle cargo in 3D organoids, including representation of several miRNA targets and proteins primarily implicated in the immune response. Our results show that 3D glioblastoma organoid models secrete extracellular vesicles with an altered cargo compared to corresponding conventional 2D cultures. Extracellular vesicles from 3D cultures were found to contain signaling molecules associated with the immune regulatory signaling pathways and as such could potentially change the surrounding microenvironment towards tumor progression and immunosuppressive conditions. These findings suggest the use of 3D glioblastoma models for further clinical biomarker studies as well as investigation of new therapeutic options.
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Publisher
Frontiers Media SA,Frontiers Media S.A
Subject

3D organoid model

/ Antibodies

/ Biomarkers

/ Brain cancer

/ Brain Neoplasms - immunology

/ Brain Neoplasms - metabolism

/ Brain Neoplasms - pathology

/ CD63 antigen

/ CD81 antigen

/ CD9 antigen

/ Cell culture

/ Cell Culture Techniques, Three Dimensional - methods

/ Cell interactions

/ Cell Line, Tumor

/ Cells

/ Communications systems

/ Data analysis

/ Extracellular matrix

/ extracellular vesicle

/ Extracellular vesicles

/ Extracellular Vesicles - immunology

/ Extracellular Vesicles - metabolism

/ Females

/ Flow cytometry

/ Gene expression

/ Gene Expression Regulation, Neoplastic

/ Glioblastoma - immunology

/ Glioblastoma - metabolism

/ Glioblastoma - pathology

/ Glioblastoma cells

/ glioblastoma multiforme

/ Glioma

/ Growth factors

/ Humans

/ Immune response

/ Immunology

/ Malignancy

/ Mass spectroscopy

/ microRNA

/ MicroRNAs

/ MicroRNAs - genetics

/ miRNA

/ Organoids

/ Organoids - immunology

/ Preadipocyte factor 1

/ Proteomes

/ Signal Transduction

/ Tumor Cells, Cultured

/ Tumor microenvironment

/ Tumor Microenvironment - immunology

/ Tumors

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