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Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment
by
Nejo, Takahide
, Levine, Lauren S.
, Hatae, Ryusuke
, Chen, Tiffany
, Okada, Hideho
, Kyewalabye, Keith
, Yamamichi, Akane
, Phyu, Su
, Chuntova, Pavlina
, Spitzer, Matthew H.
in
AMP-Activated Protein Kinases - metabolism
/ Animals
/ Antigens
/ Brain - metabolism
/ Brain cancer
/ Brain tumors
/ CD11b antigen
/ Cell Line, Tumor
/ Chimeric antigen receptors
/ Clinical trials
/ Cytotoxicity
/ Drug screening
/ Glioma
/ Glioma cells
/ Humans
/ Hypotheses
/ Hypoxia
/ Immunology
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Metabolism
/ Metformin
/ Mice
/ Mitochondria
/ Monocytes
/ Oncology
/ Phosphorylation
/ Rapamycin
/ Spleen
/ Suppressor cells
/ T-Lymphocytes
/ TOR protein
/ TOR Serine-Threonine Kinases - metabolism
/ Tumor Microenvironment
/ Tumors
/ Xenograft Model Antitumor Assays
2024
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Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment
by
Nejo, Takahide
, Levine, Lauren S.
, Hatae, Ryusuke
, Chen, Tiffany
, Okada, Hideho
, Kyewalabye, Keith
, Yamamichi, Akane
, Phyu, Su
, Chuntova, Pavlina
, Spitzer, Matthew H.
in
AMP-Activated Protein Kinases - metabolism
/ Animals
/ Antigens
/ Brain - metabolism
/ Brain cancer
/ Brain tumors
/ CD11b antigen
/ Cell Line, Tumor
/ Chimeric antigen receptors
/ Clinical trials
/ Cytotoxicity
/ Drug screening
/ Glioma
/ Glioma cells
/ Humans
/ Hypotheses
/ Hypoxia
/ Immunology
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Metabolism
/ Metformin
/ Mice
/ Mitochondria
/ Monocytes
/ Oncology
/ Phosphorylation
/ Rapamycin
/ Spleen
/ Suppressor cells
/ T-Lymphocytes
/ TOR protein
/ TOR Serine-Threonine Kinases - metabolism
/ Tumor Microenvironment
/ Tumors
/ Xenograft Model Antitumor Assays
2024
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Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment
by
Nejo, Takahide
, Levine, Lauren S.
, Hatae, Ryusuke
, Chen, Tiffany
, Okada, Hideho
, Kyewalabye, Keith
, Yamamichi, Akane
, Phyu, Su
, Chuntova, Pavlina
, Spitzer, Matthew H.
in
AMP-Activated Protein Kinases - metabolism
/ Animals
/ Antigens
/ Brain - metabolism
/ Brain cancer
/ Brain tumors
/ CD11b antigen
/ Cell Line, Tumor
/ Chimeric antigen receptors
/ Clinical trials
/ Cytotoxicity
/ Drug screening
/ Glioma
/ Glioma cells
/ Humans
/ Hypotheses
/ Hypoxia
/ Immunology
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Metabolism
/ Metformin
/ Mice
/ Mitochondria
/ Monocytes
/ Oncology
/ Phosphorylation
/ Rapamycin
/ Spleen
/ Suppressor cells
/ T-Lymphocytes
/ TOR protein
/ TOR Serine-Threonine Kinases - metabolism
/ Tumor Microenvironment
/ Tumors
/ Xenograft Model Antitumor Assays
2024
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Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment
Journal Article
Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment
2024
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Overview
The efficacy of chimeric antigen receptor T cell (CAR-T) therapy has been limited against brain tumors to date. CAR-T cells infiltrating syngeneic intracerebral SB28 EGFRvIII gliomas revealed impaired mitochondrial ATP production and a markedly hypoxic status compared with ones migrating to subcutaneous tumors. Drug screenings to improve metabolic states of T cells under hypoxic conditions led us to evaluate the combination of the AMPK activator metformin and the mTOR inhibitor rapamycin (Met+Rap). Met+Rap-pretreated mouse CAR-T cells showed activated PPAR-γ coactivator 1α (PGC-1α) through mTOR inhibition and AMPK activation, and a higher level of mitochondrial spare respiratory capacity than those pretreated with individual drugs or without pretreatment. Moreover, Met+Rap-pretreated CAR-T cells demonstrated persistent and effective antiglioma cytotoxic activities in the hypoxic condition. Furthermore, a single intravenous infusion of Met+Rap-pretreated CAR-T cells significantly extended the survival of mice bearing intracerebral SB28 EGFRvIII gliomas. Mass cytometric analyses highlighted increased glioma-infiltrating CAR-T cells in the Met+Rap group, with fewer Ly6c+CD11b+ monocytic myeloid-derived suppressor cells in the tumors. Finally, human CAR-T cells pretreated with Met+Rap recapitulated the observations with murine CAR-T cells, demonstrating improved functions under in vitro hypoxic conditions. These findings advocate for translational and clinical exploration of Met+Rap-pretreated CAR-T cells in human trials.
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