PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer

Myeloid-derived suppressor cells (MDSCs) are an immature innate cell population that expands in pathological conditions such as cancer and suppresses T cells via production of immunosuppressive factors. Conversely, efficient cytotoxic T cell priming is dependent on the ability of antigen-presenting...

Descripción completa

Detalles Bibliográficos
Autores principales: Chaib, Mehdi, Sipe, Laura M., Yarbro, Johnathan R., Bohm, Margaret S., Counts, Brittany R., Tanveer, Ubaid, Pingili, Ajeeth K., Daria, Deidre, Marion, Tony N., Carson, James A., Thomas, Paul G., Makowski, Liza
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9867936/
https://www.ncbi.nlm.nih.gov/pubmed/35074498
http://dx.doi.org/10.1016/j.canlet.2022.01.017
_version_ 1784876442432045056
author Chaib, Mehdi
Sipe, Laura M.
Yarbro, Johnathan R.
Bohm, Margaret S.
Counts, Brittany R.
Tanveer, Ubaid
Pingili, Ajeeth K.
Daria, Deidre
Marion, Tony N.
Carson, James A.
Thomas, Paul G.
Makowski, Liza
author_facet Chaib, Mehdi
Sipe, Laura M.
Yarbro, Johnathan R.
Bohm, Margaret S.
Counts, Brittany R.
Tanveer, Ubaid
Pingili, Ajeeth K.
Daria, Deidre
Marion, Tony N.
Carson, James A.
Thomas, Paul G.
Makowski, Liza
author_sort Chaib, Mehdi
collection PubMed
description Myeloid-derived suppressor cells (MDSCs) are an immature innate cell population that expands in pathological conditions such as cancer and suppresses T cells via production of immunosuppressive factors. Conversely, efficient cytotoxic T cell priming is dependent on the ability of antigen-presenting cells (APCs) to cross-present tumor antigens to CD8(+) T cells, a process that requires a specific subtype of dendritic cells (DCs) called conventional DC1 (cDC1) which are often dysfunctional in cancer. One way to activate cDC1 is ligation of CD40 which is abundantly expressed by myeloid cells and its agonism leads to myeloid cell activation. Thus, targeting MDSCs while simultaneously expanding cross-presenting DCs represents a promising strategy that, when combined with agonistic CD40, may result in long-lasting protective immunity. In this study, we investigated the effect of PKC agonists PEP005 and prostratin on MDSC expansion, differentiation, and recruitment to the tumor microenvironment. Our findings demonstrate that PKC agonists decreased MDSC expansion from hematopoietic progenitors and induced M-MDSC differentiation to an APC-like phenotype that expresses cDC1-related markers via activation of the p38 mitogen-activated protein kinase (MAPK) pathway. Simultaneously, PKC agonists favored cDC1 expansion at the expense of cDC2 and plasmacytoid DCs (pDC). Functionally, PKC agonists blunted MDSC suppressive activity and enhanced MDSC cross-priming capacity both in vitro and in vivo. Finally, combination of PKC agonism with agonistic CD40 mAb resulted in a marked reduction in tumor growth with a significant increase in intratumoral activated CD8(+) T cells and tissue-resident memory CD8(+) T cells in a syngeneic breast cancer mouse model. In sum, this work proposes a novel promising strategy to simultaneously target MDSCs and promote APC function that may have highly impactful clinical relevance in cancer patients.
format Online
Article
Text
id pubmed-9867936
institution National Center for Biotechnology Information
language English
publishDate 2022
record_format MEDLINE/PubMed
spelling pubmed-98679362023-01-22 PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer Chaib, Mehdi Sipe, Laura M. Yarbro, Johnathan R. Bohm, Margaret S. Counts, Brittany R. Tanveer, Ubaid Pingili, Ajeeth K. Daria, Deidre Marion, Tony N. Carson, James A. Thomas, Paul G. Makowski, Liza Cancer Lett Article Myeloid-derived suppressor cells (MDSCs) are an immature innate cell population that expands in pathological conditions such as cancer and suppresses T cells via production of immunosuppressive factors. Conversely, efficient cytotoxic T cell priming is dependent on the ability of antigen-presenting cells (APCs) to cross-present tumor antigens to CD8(+) T cells, a process that requires a specific subtype of dendritic cells (DCs) called conventional DC1 (cDC1) which are often dysfunctional in cancer. One way to activate cDC1 is ligation of CD40 which is abundantly expressed by myeloid cells and its agonism leads to myeloid cell activation. Thus, targeting MDSCs while simultaneously expanding cross-presenting DCs represents a promising strategy that, when combined with agonistic CD40, may result in long-lasting protective immunity. In this study, we investigated the effect of PKC agonists PEP005 and prostratin on MDSC expansion, differentiation, and recruitment to the tumor microenvironment. Our findings demonstrate that PKC agonists decreased MDSC expansion from hematopoietic progenitors and induced M-MDSC differentiation to an APC-like phenotype that expresses cDC1-related markers via activation of the p38 mitogen-activated protein kinase (MAPK) pathway. Simultaneously, PKC agonists favored cDC1 expansion at the expense of cDC2 and plasmacytoid DCs (pDC). Functionally, PKC agonists blunted MDSC suppressive activity and enhanced MDSC cross-priming capacity both in vitro and in vivo. Finally, combination of PKC agonism with agonistic CD40 mAb resulted in a marked reduction in tumor growth with a significant increase in intratumoral activated CD8(+) T cells and tissue-resident memory CD8(+) T cells in a syngeneic breast cancer mouse model. In sum, this work proposes a novel promising strategy to simultaneously target MDSCs and promote APC function that may have highly impactful clinical relevance in cancer patients. 2022-04-10 2022-01-21 /pmc/articles/PMC9867936/ /pubmed/35074498 http://dx.doi.org/10.1016/j.canlet.2022.01.017 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) ).
spellingShingle Article
Chaib, Mehdi
Sipe, Laura M.
Yarbro, Johnathan R.
Bohm, Margaret S.
Counts, Brittany R.
Tanveer, Ubaid
Pingili, Ajeeth K.
Daria, Deidre
Marion, Tony N.
Carson, James A.
Thomas, Paul G.
Makowski, Liza
PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title_full PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title_fullStr PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title_full_unstemmed PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title_short PKC agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic CD40 antibody therapy to activate CD8(+) T cells in breast cancer
title_sort pkc agonism restricts innate immune suppression, promotes antigen cross-presentation and synergizes with agonistic cd40 antibody therapy to activate cd8(+) t cells in breast cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9867936/
https://www.ncbi.nlm.nih.gov/pubmed/35074498
http://dx.doi.org/10.1016/j.canlet.2022.01.017
work_keys_str_mv AT chaibmehdi pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT sipelauram pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT yarbrojohnathanr pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT bohmmargarets pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT countsbrittanyr pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT tanveerubaid pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT pingiliajeethk pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT dariadeidre pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT mariontonyn pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT carsonjamesa pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT thomaspaulg pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer
AT makowskiliza pkcagonismrestrictsinnateimmunesuppressionpromotesantigencrosspresentationandsynergizeswithagonisticcd40antibodytherapytoactivatecd8tcellsinbreastcancer

Ejemplares similares