Leveraging the Treg-intrinsic CTLA4-PKCeta signaling pathway for cancer immunotherapy
| dc.contributor.author | Liu, Hsin-Yu | |
| dc.contributor.author | Pedros, Christophe | |
| dc.contributor.author | Kong, Kok-Fai | |
| dc.contributor.author | Canonigo-Balancio, Ann J. | |
| dc.contributor.author | Xue, Wen | |
| dc.contributor.author | Altman, Amnon | |
| dc.date | 2022-08-11T08:10:06.000 | |
| dc.date.accessioned | 2022-08-23T16:55:27Z | |
| dc.date.available | 2022-08-23T16:55:27Z | |
| dc.date.issued | 2021-09-01 | |
| dc.date.submitted | 2022-06-02 | |
| dc.identifier.citation | <p>Liu HY, Pedros C, Kong KF, Canonigo-Balancio AJ, Xue W, Altman A. Leveraging the Treg-intrinsic CTLA4-PKCη signaling pathway for cancer immunotherapy. J Immunother Cancer. 2021 Sep;9(9):e002792. doi: 10.1136/jitc-2021-002792. PMID: 34588224; PMCID: PMC8483050. <a href="https://doi.org/10.1136/jitc-2021-002792">Link to article on publisher's site</a></p> | |
| dc.identifier.issn | 2051-1426 (Linking) | |
| dc.identifier.doi | 10.1136/jitc-2021-002792 | |
| dc.identifier.pmid | 34588224 | |
| dc.identifier.uri | http://hdl.handle.net/20.500.14038/42717 | |
| dc.description.abstract | BACKGROUND: Our previous studies revealed a critical role of a novel CTLA4-protein kinase C-eta (PKCeta) signaling axis in mediating the suppressive activity of regulatory T cells (Tregs) in antitumor immunity. These studies have employed adoptive transfer of germline PKCeta-deficient (Prkch (-/-)) Tregs into Prkch (+/+) mice prior to tumor implantation. Here, we extended these findings into a biologically and clinically more relevant context. METHODS: We have analyzed the role of PKCeta in antitumor immunity and the tumor microenvironment (TME) in intact tumor-bearing mice with Treg-specific or CD8(+) T cell-specific Prkch deletion, including in a therapeutic model of combinatorial treatment. In addition to measuring tumor growth, we analyzed the phenotype and functional attributes of tumor-infiltrating immune cells, particularly Tregs and dendritic cells (DCs). RESULTS: Using two models of mouse transplantable cancer and a genetically engineered autochthonous hepatocellular carcinoma (HCC) model, we found, first, that mice with Treg-specific Prkch deletion displayed a significantly reduced growth of B16-F10 melanoma and TRAMP-C1 adenocarcinoma tumors. Tumor growth reduction was associated with a less immunosuppressive TME, indicated by increased numbers and function of tumor-infiltrating CD8(+) effector T cells and elevated expression of the costimulatory ligand CD86 on intratumoral DCs. In contrast, CD8(+) T cell-specific Prkch deletion had no effect on tumor growth or the abundance and functionality of CD8(+) effector T cells, consistent with findings that Prkch (-/-) CD8(+) T cells proliferated normally in response to in vitro polyclonal or specific antigen stimulation. Similar beneficial antitumor effects were found in mice with germline or Treg-specific Prkch deletion that were induced to develop an autochthonous HCC. Lastly, using a therapeutic model, we found that monotherapies consisting of Treg-specific Prkch deletion or vaccination with irradiated Fms-like tyrosine kinase 3 ligand (Flt3L)-expressing B16-F10 tumor cells post-tumor implantation significantly delayed tumor growth. This effect was more pronounced in mice receiving a combination of the two immunotherapies. CONCLUSION: These findings demonstrate the potential utility of PKCeta inhibition as a viable clinical approach to treat patients with cancer, especially when combined with adjuvant therapies. | |
| dc.language.iso | en_US | |
| dc.relation | <p><a href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=pubmed&cmd=Retrieve&list_uids=34588224&dopt=Abstract">Link to Article in PubMed</a></p> | |
| dc.rights | Copyright © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/. | |
| dc.rights.uri | http://creativecommons.org/licenses/by-nc/4.0/ | |
| dc.subject | CD8-positive T lymphocytes | |
| dc.subject | CTLA4 antigen | |
| dc.subject | combined modality therapy | |
| dc.subject | melanoma | |
| dc.subject | tumor microenvironment | |
| dc.subject | Cancer Biology | |
| dc.subject | Immunotherapy | |
| dc.subject | Neoplasms | |
| dc.title | Leveraging the Treg-intrinsic CTLA4-PKCeta signaling pathway for cancer immunotherapy | |
| dc.type | Journal Article | |
| dc.source.journaltitle | Journal for immunotherapy of cancer | |
| dc.source.volume | 9 | |
| dc.source.issue | 9 | |
| dc.identifier.legacyfulltext | https://escholarship.umassmed.edu/cgi/viewcontent.cgi?article=5996&context=oapubs&unstamped=1 | |
| dc.identifier.legacycoverpage | https://escholarship.umassmed.edu/oapubs/4961 | |
| dc.identifier.contextkey | 29511297 | |
| refterms.dateFOA | 2022-08-23T16:55:27Z | |
| html.description.abstract | <p>BACKGROUND: Our previous studies revealed a critical role of a novel CTLA4-protein kinase C-eta (PKCeta) signaling axis in mediating the suppressive activity of regulatory T cells (Tregs) in antitumor immunity. These studies have employed adoptive transfer of germline PKCeta-deficient (Prkch (-/-)) Tregs into Prkch (+/+) mice prior to tumor implantation. Here, we extended these findings into a biologically and clinically more relevant context.</p> <p>METHODS: We have analyzed the role of PKCeta in antitumor immunity and the tumor microenvironment (TME) in intact tumor-bearing mice with Treg-specific or CD8(+) T cell-specific Prkch deletion, including in a therapeutic model of combinatorial treatment. In addition to measuring tumor growth, we analyzed the phenotype and functional attributes of tumor-infiltrating immune cells, particularly Tregs and dendritic cells (DCs).</p> <p>RESULTS: Using two models of mouse transplantable cancer and a genetically engineered autochthonous hepatocellular carcinoma (HCC) model, we found, first, that mice with Treg-specific Prkch deletion displayed a significantly reduced growth of B16-F10 melanoma and TRAMP-C1 adenocarcinoma tumors. Tumor growth reduction was associated with a less immunosuppressive TME, indicated by increased numbers and function of tumor-infiltrating CD8(+) effector T cells and elevated expression of the costimulatory ligand CD86 on intratumoral DCs. In contrast, CD8(+) T cell-specific Prkch deletion had no effect on tumor growth or the abundance and functionality of CD8(+) effector T cells, consistent with findings that Prkch (-/-) CD8(+) T cells proliferated normally in response to in vitro polyclonal or specific antigen stimulation. Similar beneficial antitumor effects were found in mice with germline or Treg-specific Prkch deletion that were induced to develop an autochthonous HCC. Lastly, using a therapeutic model, we found that monotherapies consisting of Treg-specific Prkch deletion or vaccination with irradiated Fms-like tyrosine kinase 3 ligand (Flt3L)-expressing B16-F10 tumor cells post-tumor implantation significantly delayed tumor growth. This effect was more pronounced in mice receiving a combination of the two immunotherapies.</p> <p>CONCLUSION: These findings demonstrate the potential utility of PKCeta inhibition as a viable clinical approach to treat patients with cancer, especially when combined with adjuvant therapies.</p> | |
| dc.identifier.submissionpath | oapubs/4961 | |
| dc.contributor.department | RNA Therapeutics Institute | |
| dc.source.pages | e002792 |
Files in this item
This item appears in the following Collection(s)
Except where otherwise noted, this item's license is described as Copyright © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ. This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See http://creativecommons.org/licenses/by-nc/4.0/.