Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy
Abstract Expression of PDL1 on the surface of tumor cells can blunt the efficacy of many cancer immunotherapies. For example, our lab has previously shown that tumors derived from malignant cells incapable of expressing PDL1 are highly susceptible to immunotherapy induced by oncolytic virus treatmen...
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doaj-0cda94d2b59b42d1ade2c0d8bb034b592020-11-25T00:41:49ZengBMJ Publishing GroupJournal for ImmunoTherapy of Cancer2051-14262019-01-01711810.1186/s40425-018-0496-6Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapyMee Y. Bartee0Parker C. Dryja1Eric Bartee2Department of Microbiology and Immunology, Medical University of South CarolinaDepartment of Microbiology and Immunology, Medical University of South CarolinaDepartment of Microbiology and Immunology, Medical University of South CarolinaAbstract Expression of PDL1 on the surface of tumor cells can blunt the efficacy of many cancer immunotherapies. For example, our lab has previously shown that tumors derived from malignant cells incapable of expressing PDL1 are highly susceptible to immunotherapy induced by oncolytic virus treatment while tumors derived from PDL1 capable cells are highly resistant. In patient biopsies, however, expression of PDL1 on malignant cells is often not uniform with some cells expressing PDL1 while others do not. Importantly, how this partial PDL1 positivity influences the outcomes of immunotherapy remains largely unknown. In the current work, we expand on our previous findings by generating partially PDL1 positive tumors in immune competent animals and asking what percentage of tumor cells must express PDL1 for a tumor to become functionally resistant to oncolytic treatment. Our results indicate that the responsiveness of partially PDL1+ tumors correlates linearly with the percentage of PDL1 capable cells present at the initiation of treatment. Additionally, we observe that tumors which relapse after treatment display a significant increase in the numbers of PDL1 capable cells present suggesting that specific editing of mixed tumors might play a role in disease relapse. These data indicate that varying levels of PDL1 expression can play a significant role in the outcomes of oncolytic immunotherapy and challenges the concept that tumors should be viewed as simply PDL1+ or PDL1−.http://link.springer.com/article/10.1186/s40425-018-0496-6ImmunotherapyOncolytic virotherapyMyxoma virusTumor heterogeneityPDL1 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Mee Y. Bartee Parker C. Dryja Eric Bartee |
spellingShingle |
Mee Y. Bartee Parker C. Dryja Eric Bartee Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy Journal for ImmunoTherapy of Cancer Immunotherapy Oncolytic virotherapy Myxoma virus Tumor heterogeneity PDL1 |
author_facet |
Mee Y. Bartee Parker C. Dryja Eric Bartee |
author_sort |
Mee Y. Bartee |
title |
Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy |
title_short |
Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy |
title_full |
Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy |
title_fullStr |
Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy |
title_full_unstemmed |
Chimeric tumor modeling reveals role of partial PDL1 expression in resistance to virally induced immunotherapy |
title_sort |
chimeric tumor modeling reveals role of partial pdl1 expression in resistance to virally induced immunotherapy |
publisher |
BMJ Publishing Group |
series |
Journal for ImmunoTherapy of Cancer |
issn |
2051-1426 |
publishDate |
2019-01-01 |
description |
Abstract Expression of PDL1 on the surface of tumor cells can blunt the efficacy of many cancer immunotherapies. For example, our lab has previously shown that tumors derived from malignant cells incapable of expressing PDL1 are highly susceptible to immunotherapy induced by oncolytic virus treatment while tumors derived from PDL1 capable cells are highly resistant. In patient biopsies, however, expression of PDL1 on malignant cells is often not uniform with some cells expressing PDL1 while others do not. Importantly, how this partial PDL1 positivity influences the outcomes of immunotherapy remains largely unknown. In the current work, we expand on our previous findings by generating partially PDL1 positive tumors in immune competent animals and asking what percentage of tumor cells must express PDL1 for a tumor to become functionally resistant to oncolytic treatment. Our results indicate that the responsiveness of partially PDL1+ tumors correlates linearly with the percentage of PDL1 capable cells present at the initiation of treatment. Additionally, we observe that tumors which relapse after treatment display a significant increase in the numbers of PDL1 capable cells present suggesting that specific editing of mixed tumors might play a role in disease relapse. These data indicate that varying levels of PDL1 expression can play a significant role in the outcomes of oncolytic immunotherapy and challenges the concept that tumors should be viewed as simply PDL1+ or PDL1−. |
topic |
Immunotherapy Oncolytic virotherapy Myxoma virus Tumor heterogeneity PDL1 |
url |
http://link.springer.com/article/10.1186/s40425-018-0496-6 |
work_keys_str_mv |
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