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Enhancement of PSMA-Directed CAR Adoptive Immunotherapy by PD-1/PD-L1 Blockade
by
Blasberg, Ronald
, Moroz, Ekaterina
, Mane, Mayuresh
, Serganova, Inna
, Moroz, Maxim
, Zurita, Juan
, Cohen, Ivan
, Shenker, Larissa
, Ponomarev, Vladimir
in
Adoptive immunotherapy
/ anti-PD1
/ Antigens
/ Antitumor activity
/ Apoptosis
/ Bioluminescence
/ bioluminescence imaging
/ BLI
/ Blood cancer
/ Cancer therapies
/ CAR T cells
/ CD3 antigen
/ Cell activation
/ Cell adhesion & migration
/ Cell death
/ Cellular biology
/ Chimeric antigen receptors
/ Clinical trials
/ human PSMA
/ Immunomodulation
/ Immunotherapy
/ luciferase reporters
/ Lymphocytes
/ Lymphocytes T
/ Mitochondria
/ Monoclonal antibodies
/ Morphology
/ Myc protein
/ Nodules
/ Original
/ PD-1 protein
/ PD-L1 protein
/ Prostate cancer
/ Software
/ Solid tumors
/ Studies
/ T cell receptors
/ Tumors
2017
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Enhancement of PSMA-Directed CAR Adoptive Immunotherapy by PD-1/PD-L1 Blockade
by
Blasberg, Ronald
, Moroz, Ekaterina
, Mane, Mayuresh
, Serganova, Inna
, Moroz, Maxim
, Zurita, Juan
, Cohen, Ivan
, Shenker, Larissa
, Ponomarev, Vladimir
in
Adoptive immunotherapy
/ anti-PD1
/ Antigens
/ Antitumor activity
/ Apoptosis
/ Bioluminescence
/ bioluminescence imaging
/ BLI
/ Blood cancer
/ Cancer therapies
/ CAR T cells
/ CD3 antigen
/ Cell activation
/ Cell adhesion & migration
/ Cell death
/ Cellular biology
/ Chimeric antigen receptors
/ Clinical trials
/ human PSMA
/ Immunomodulation
/ Immunotherapy
/ luciferase reporters
/ Lymphocytes
/ Lymphocytes T
/ Mitochondria
/ Monoclonal antibodies
/ Morphology
/ Myc protein
/ Nodules
/ Original
/ PD-1 protein
/ PD-L1 protein
/ Prostate cancer
/ Software
/ Solid tumors
/ Studies
/ T cell receptors
/ Tumors
2017
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Enhancement of PSMA-Directed CAR Adoptive Immunotherapy by PD-1/PD-L1 Blockade
by
Blasberg, Ronald
, Moroz, Ekaterina
, Mane, Mayuresh
, Serganova, Inna
, Moroz, Maxim
, Zurita, Juan
, Cohen, Ivan
, Shenker, Larissa
, Ponomarev, Vladimir
in
Adoptive immunotherapy
/ anti-PD1
/ Antigens
/ Antitumor activity
/ Apoptosis
/ Bioluminescence
/ bioluminescence imaging
/ BLI
/ Blood cancer
/ Cancer therapies
/ CAR T cells
/ CD3 antigen
/ Cell activation
/ Cell adhesion & migration
/ Cell death
/ Cellular biology
/ Chimeric antigen receptors
/ Clinical trials
/ human PSMA
/ Immunomodulation
/ Immunotherapy
/ luciferase reporters
/ Lymphocytes
/ Lymphocytes T
/ Mitochondria
/ Monoclonal antibodies
/ Morphology
/ Myc protein
/ Nodules
/ Original
/ PD-1 protein
/ PD-L1 protein
/ Prostate cancer
/ Software
/ Solid tumors
/ Studies
/ T cell receptors
/ Tumors
2017
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Enhancement of PSMA-Directed CAR Adoptive Immunotherapy by PD-1/PD-L1 Blockade
Journal Article
Enhancement of PSMA-Directed CAR Adoptive Immunotherapy by PD-1/PD-L1 Blockade
2017
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Overview
Chimeric antigen receptor (CAR) T cell therapy in hematologic malignancies has shown remarkable responses, but the same level of success has not been observed in solid tumors. A new prostate cancer model (Myc-CaP:PSMA(+)) and a second-generation anti-hPSMA human CAR T cells expressing a Click Beetle Red luciferase reporter) were used to study hPSMA targeting and assess CAR T cell trafficking and persistence by bioluminescence imaging (BLI). We investigated the antitumor efficacy of human CAR T cells targeting human prostate-specific membrane antigen (hPSMA), in the presence and absence of the target antigen; first alone and then combined with a monoclonal antibody targeting the human programmed death receptor 1 (anti-hPD1 mAb). PDL-1 expression was detected in Myc-CaP murine prostate tumors growing in immune competent FVB/N and immune-deficient SCID mice. Endogenous CD3+ T cells were restricted from the centers of Myc-CaP tumor nodules growing in FVB/N mice. Following anti-programmed cell death protein 1 (PD-1) treatment, the restriction of CD3+ T cells was reversed, and a tumor-treatment response was observed. Adoptive hPSMA-CAR T cell immunotherapy was enhanced when combined with PD-1 blockade, but the treatment response was of comparatively short duration, suggesting other immune modulation mechanisms exist and restrict CAR T cell targeting, function, and persistence in hPSMA expressing Myc-CaP tumors. Interestingly, an “inverse pattern” of CAR T cell BLI intensity was observed in control and test tumors, which suggests CAR T cells undergo changes leading to a loss of signal and/or number following hPSMA-specific activation. The lower BLI signal intensity in the hPSMA test tumors (compared with controls) is due in part to a decrease in T cell mitochondrial function following T cell activation, which may limit the intensity of the ATP-dependent Luciferin-luciferase bioluminescence signal.
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