Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy

Adoptive T cell therapy has shown clinical potential for patients with cancer, though effective treatment is dependent on longevity and potency of the exploited tumor-reactive T cells. Previously, we showed that ex vivo inhibition of AKT using the research compound Akt-inhibitor VIII retained differ...

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Autores principales: Mousset, Charlotte M., Hobo, Willemijn, Ji, Yun, Fredrix, Hanny, De Giorgi, Valeria, Allison, Robert D., Kester, Michel G. D., Falkenburg, J. H. Frederik, Schaap, Nicolaas P. M., Jansen, Joop H., Gattinoni, Luca, Dolstra, Harry, van der Waart, Anniek B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2018
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6169586/
https://www.ncbi.nlm.nih.gov/pubmed/30288356
http://dx.doi.org/10.1080/2162402X.2018.1488565
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author Mousset, Charlotte M.
Hobo, Willemijn
Ji, Yun
Fredrix, Hanny
De Giorgi, Valeria
Allison, Robert D.
Kester, Michel G. D.
Falkenburg, J. H. Frederik
Schaap, Nicolaas P. M.
Jansen, Joop H.
Gattinoni, Luca
Dolstra, Harry
van der Waart, Anniek B.
author_facet Mousset, Charlotte M.
Hobo, Willemijn
Ji, Yun
Fredrix, Hanny
De Giorgi, Valeria
Allison, Robert D.
Kester, Michel G. D.
Falkenburg, J. H. Frederik
Schaap, Nicolaas P. M.
Jansen, Joop H.
Gattinoni, Luca
Dolstra, Harry
van der Waart, Anniek B.
author_sort Mousset, Charlotte M.
collection PubMed
description Adoptive T cell therapy has shown clinical potential for patients with cancer, though effective treatment is dependent on longevity and potency of the exploited tumor-reactive T cells. Previously, we showed that ex vivo inhibition of AKT using the research compound Akt-inhibitor VIII retained differentiation and improved functionality of minor histocompatibility antigen (MiHA)-specific CD8(+) T cells. Here, we compared a panel of clinically applicable AKT-inhibitors with an allosteric or adenosine triphosphate-competitive mode of action. We analyzed phenotype, functionality, metabolism and transcriptome of AKT-inhibited CD8(+) T cells using different T cell activation models. Most inhibitors facilitated T cell expansion while preserving an early memory phenotype, reflected by maintenance of CD62L, CCR7 and CXCR4 expression. Moreover, transcriptome profiling revealed that AKT-inhibited CD8(+) T cells clustered closely to naturally occurring stem cell-memory CD8(+) T cells, while control T cells resembled effector-memory T cells. Interestingly, AKT-inhibited CD8(+) T cells showed enrichment of hypoxia-associated genes, which was consistent with enhanced glycolytic function. Notably, AKT-inhibition during MiHA-specific CD8(+) T cell priming uncoupled preservation of early memory differentiation from ex vivo expansion. Furthermore, AKT-inhibited MiHA-specific CD8(+) T cells showed increased polyfunctionality with co-secretion of IFN-γ and IL-2 upon antigen recall. Together, these data demonstrate that AKT-inhibitors with different modality of action promote the ex vivo generation of stem cell memory-like CD8(+) T cells with a unique metabolic profile and retained polyfunctionality. Akt-inhibitor VIII and GDC-0068 outperformed other inhibitors, and are therefore promising candidates for ex vivo generation of superior tumor-reactive T cells for adoptive immunotherapy in cancer patients.
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spelling pubmed-61695862018-10-04 Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy Mousset, Charlotte M. Hobo, Willemijn Ji, Yun Fredrix, Hanny De Giorgi, Valeria Allison, Robert D. Kester, Michel G. D. Falkenburg, J. H. Frederik Schaap, Nicolaas P. M. Jansen, Joop H. Gattinoni, Luca Dolstra, Harry van der Waart, Anniek B. Oncoimmunology Original Research Adoptive T cell therapy has shown clinical potential for patients with cancer, though effective treatment is dependent on longevity and potency of the exploited tumor-reactive T cells. Previously, we showed that ex vivo inhibition of AKT using the research compound Akt-inhibitor VIII retained differentiation and improved functionality of minor histocompatibility antigen (MiHA)-specific CD8(+) T cells. Here, we compared a panel of clinically applicable AKT-inhibitors with an allosteric or adenosine triphosphate-competitive mode of action. We analyzed phenotype, functionality, metabolism and transcriptome of AKT-inhibited CD8(+) T cells using different T cell activation models. Most inhibitors facilitated T cell expansion while preserving an early memory phenotype, reflected by maintenance of CD62L, CCR7 and CXCR4 expression. Moreover, transcriptome profiling revealed that AKT-inhibited CD8(+) T cells clustered closely to naturally occurring stem cell-memory CD8(+) T cells, while control T cells resembled effector-memory T cells. Interestingly, AKT-inhibited CD8(+) T cells showed enrichment of hypoxia-associated genes, which was consistent with enhanced glycolytic function. Notably, AKT-inhibition during MiHA-specific CD8(+) T cell priming uncoupled preservation of early memory differentiation from ex vivo expansion. Furthermore, AKT-inhibited MiHA-specific CD8(+) T cells showed increased polyfunctionality with co-secretion of IFN-γ and IL-2 upon antigen recall. Together, these data demonstrate that AKT-inhibitors with different modality of action promote the ex vivo generation of stem cell memory-like CD8(+) T cells with a unique metabolic profile and retained polyfunctionality. Akt-inhibitor VIII and GDC-0068 outperformed other inhibitors, and are therefore promising candidates for ex vivo generation of superior tumor-reactive T cells for adoptive immunotherapy in cancer patients. Taylor & Francis 2018-08-06 /pmc/articles/PMC6169586/ /pubmed/30288356 http://dx.doi.org/10.1080/2162402X.2018.1488565 Text en © 2018 The Author(s). Published by Taylor & Francis. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
spellingShingle Original Research
Mousset, Charlotte M.
Hobo, Willemijn
Ji, Yun
Fredrix, Hanny
De Giorgi, Valeria
Allison, Robert D.
Kester, Michel G. D.
Falkenburg, J. H. Frederik
Schaap, Nicolaas P. M.
Jansen, Joop H.
Gattinoni, Luca
Dolstra, Harry
van der Waart, Anniek B.
Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title_full Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title_fullStr Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title_full_unstemmed Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title_short Ex vivo AKT-inhibition facilitates generation of polyfunctional stem cell memory-like CD8(+) T cells for adoptive immunotherapy
title_sort ex vivo akt-inhibition facilitates generation of polyfunctional stem cell memory-like cd8(+) t cells for adoptive immunotherapy
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6169586/
https://www.ncbi.nlm.nih.gov/pubmed/30288356
http://dx.doi.org/10.1080/2162402X.2018.1488565
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