EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma

Glioblastoma (GBM) is the most common primary malignant brain tumor in adults and is uniformly lethal. T-cell-based immunotherapy offers a promising platform for treatment given its potential to specifically target tumor tissue while sparing the normal brain. However, the diffuse and infiltrative na...

Descripción completa

Detalles Bibliográficos
Autores principales: Miao, Hongsheng, Choi, Bryan D., Suryadevara, Carter M., Sanchez-Perez, Luis, Yang, Shicheng, De Leon, Gabriel, Sayour, Elias J., McLendon, Roger, Herndon, James E., Healy, Patrick, Archer, Gary E., Bigner, Darell D., Johnson, Laura A., Sampson, John H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3983153/
https://www.ncbi.nlm.nih.gov/pubmed/24722266
http://dx.doi.org/10.1371/journal.pone.0094281
_version_ 1782311272945025024
author Miao, Hongsheng
Choi, Bryan D.
Suryadevara, Carter M.
Sanchez-Perez, Luis
Yang, Shicheng
De Leon, Gabriel
Sayour, Elias J.
McLendon, Roger
Herndon, James E.
Healy, Patrick
Archer, Gary E.
Bigner, Darell D.
Johnson, Laura A.
Sampson, John H.
author_facet Miao, Hongsheng
Choi, Bryan D.
Suryadevara, Carter M.
Sanchez-Perez, Luis
Yang, Shicheng
De Leon, Gabriel
Sayour, Elias J.
McLendon, Roger
Herndon, James E.
Healy, Patrick
Archer, Gary E.
Bigner, Darell D.
Johnson, Laura A.
Sampson, John H.
author_sort Miao, Hongsheng
collection PubMed
description Glioblastoma (GBM) is the most common primary malignant brain tumor in adults and is uniformly lethal. T-cell-based immunotherapy offers a promising platform for treatment given its potential to specifically target tumor tissue while sparing the normal brain. However, the diffuse and infiltrative nature of these tumors in the brain parenchyma may pose an exceptional hurdle to successful immunotherapy in patients. Areas of invasive tumor are thought to reside behind an intact blood brain barrier, isolating them from effective immunosurveillance and thereby predisposing the development of "immunologically silent" tumor peninsulas. Therefore, it remains unclear if adoptively transferred T cells can migrate to and mediate regression in areas of invasive GBM. One barrier has been the lack of a preclinical mouse model that accurately recapitulates the growth patterns of human GBM in vivo. Here, we demonstrate that D-270 MG xenografts exhibit the classical features of GBM and produce the diffuse and invasive tumors seen in patients. Using this model, we designed experiments to assess whether T cells expressing third-generation chimeric antigen receptors (CARs) targeting the tumor-specific mutation of the epidermal growth factor receptor, EGFRvIII, would localize to and treat invasive intracerebral GBM. EGFRvIII-targeted CAR (EGFRvIII(+) CAR) T cells demonstrated in vitro EGFRvIII antigen-specific recognition and reactivity to the D-270 MG cell line, which naturally expresses EGFRvIII. Moreover, when administered systemically, EGFRvIII(+) CAR T cells localized to areas of invasive tumor, suppressed tumor growth, and enhanced survival of mice with established intracranial D-270 MG tumors. Together, these data demonstrate that systemically administered T cells are capable of migrating to the invasive edges of GBM to mediate antitumor efficacy and tumor regression.
format Online
Article
Text
id pubmed-3983153
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-39831532014-04-15 EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma Miao, Hongsheng Choi, Bryan D. Suryadevara, Carter M. Sanchez-Perez, Luis Yang, Shicheng De Leon, Gabriel Sayour, Elias J. McLendon, Roger Herndon, James E. Healy, Patrick Archer, Gary E. Bigner, Darell D. Johnson, Laura A. Sampson, John H. PLoS One Research Article Glioblastoma (GBM) is the most common primary malignant brain tumor in adults and is uniformly lethal. T-cell-based immunotherapy offers a promising platform for treatment given its potential to specifically target tumor tissue while sparing the normal brain. However, the diffuse and infiltrative nature of these tumors in the brain parenchyma may pose an exceptional hurdle to successful immunotherapy in patients. Areas of invasive tumor are thought to reside behind an intact blood brain barrier, isolating them from effective immunosurveillance and thereby predisposing the development of "immunologically silent" tumor peninsulas. Therefore, it remains unclear if adoptively transferred T cells can migrate to and mediate regression in areas of invasive GBM. One barrier has been the lack of a preclinical mouse model that accurately recapitulates the growth patterns of human GBM in vivo. Here, we demonstrate that D-270 MG xenografts exhibit the classical features of GBM and produce the diffuse and invasive tumors seen in patients. Using this model, we designed experiments to assess whether T cells expressing third-generation chimeric antigen receptors (CARs) targeting the tumor-specific mutation of the epidermal growth factor receptor, EGFRvIII, would localize to and treat invasive intracerebral GBM. EGFRvIII-targeted CAR (EGFRvIII(+) CAR) T cells demonstrated in vitro EGFRvIII antigen-specific recognition and reactivity to the D-270 MG cell line, which naturally expresses EGFRvIII. Moreover, when administered systemically, EGFRvIII(+) CAR T cells localized to areas of invasive tumor, suppressed tumor growth, and enhanced survival of mice with established intracranial D-270 MG tumors. Together, these data demonstrate that systemically administered T cells are capable of migrating to the invasive edges of GBM to mediate antitumor efficacy and tumor regression. Public Library of Science 2014-04-10 /pmc/articles/PMC3983153/ /pubmed/24722266 http://dx.doi.org/10.1371/journal.pone.0094281 Text en © 2014 Miao et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Miao, Hongsheng
Choi, Bryan D.
Suryadevara, Carter M.
Sanchez-Perez, Luis
Yang, Shicheng
De Leon, Gabriel
Sayour, Elias J.
McLendon, Roger
Herndon, James E.
Healy, Patrick
Archer, Gary E.
Bigner, Darell D.
Johnson, Laura A.
Sampson, John H.
EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title_full EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title_fullStr EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title_full_unstemmed EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title_short EGFRvIII-Specific Chimeric Antigen Receptor T Cells Migrate to and Kill Tumor Deposits Infiltrating the Brain Parenchyma in an Invasive Xenograft Model of Glioblastoma
title_sort egfrviii-specific chimeric antigen receptor t cells migrate to and kill tumor deposits infiltrating the brain parenchyma in an invasive xenograft model of glioblastoma
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3983153/
https://www.ncbi.nlm.nih.gov/pubmed/24722266
http://dx.doi.org/10.1371/journal.pone.0094281
work_keys_str_mv AT miaohongsheng egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT choibryand egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT suryadevaracarterm egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT sanchezperezluis egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT yangshicheng egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT deleongabriel egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT sayoureliasj egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT mclendonroger egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT herndonjamese egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT healypatrick egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT archergarye egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT bignerdarelld egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT johnsonlauraa egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma
AT sampsonjohnh egfrviiispecificchimericantigenreceptortcellsmigratetoandkilltumordepositsinfiltratingthebrainparenchymainaninvasivexenograftmodelofglioblastoma

Ejemplares similares