Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy

Strategies to augment anti-cancer immune responses have recently demonstrated therapeutic utility. To date clinical success has been achieved through targeting co-inhibitory checkpoints such as CTLA-4, PD-1, and PD-L1. However, approaches that target co-activatory pathways are also being actively be...

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Autores principales: Dovedi, Simon J., Adlard, Amy L., Ota, Yosuke, Murata, Masashi, Sugaru, Eiji, Koga-Yamakawa, Erina, Eguchi, Ken, Hirose, Yuko, Yamamoto, Setsuko, Umehara, Hiroki, Honeychurch, Jamie, Cheadle, Eleanor J., Hughes, Gareth, Jewsbury, Philip J., Wilkinson, Robert W., Stratford, Ian J., Illidge, Timothy M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4941369/
https://www.ncbi.nlm.nih.gov/pubmed/26959743
http://dx.doi.org/10.18632/oncotarget.7928
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author Dovedi, Simon J.
Adlard, Amy L.
Ota, Yosuke
Murata, Masashi
Sugaru, Eiji
Koga-Yamakawa, Erina
Eguchi, Ken
Hirose, Yuko
Yamamoto, Setsuko
Umehara, Hiroki
Honeychurch, Jamie
Cheadle, Eleanor J.
Hughes, Gareth
Jewsbury, Philip J.
Wilkinson, Robert W.
Stratford, Ian J.
Illidge, Timothy M.
author_facet Dovedi, Simon J.
Adlard, Amy L.
Ota, Yosuke
Murata, Masashi
Sugaru, Eiji
Koga-Yamakawa, Erina
Eguchi, Ken
Hirose, Yuko
Yamamoto, Setsuko
Umehara, Hiroki
Honeychurch, Jamie
Cheadle, Eleanor J.
Hughes, Gareth
Jewsbury, Philip J.
Wilkinson, Robert W.
Stratford, Ian J.
Illidge, Timothy M.
author_sort Dovedi, Simon J.
collection PubMed
description Strategies to augment anti-cancer immune responses have recently demonstrated therapeutic utility. To date clinical success has been achieved through targeting co-inhibitory checkpoints such as CTLA-4, PD-1, and PD-L1. However, approaches that target co-activatory pathways are also being actively being developed. Here we report that the novel TLR7-selective agonist DSR-29133 is well tolerated in mice and leads to acute immune activation. Administration of DSR-29133 leads to the induction of IFNα/γ, IP-10, TNFα, IL-1Ra and IL-12p70, and to a reduction in tumor burden in syngeneic models of renal cancer (Renca), metastatic osteosarcoma (LM8) and colorectal cancer (CT26). Moreover, we show that the efficacy of DSR-29133 was significantly improved when administered in combination with low-dose fractionated radiotherapy (RT). Effective combination therapy required weekly administration of DSR-29133 commencing on day 1 of a fractionated RT treatment cycle, whereas no enhancement of radiation response was observed when DSR-29133 was administered at the end of the fractionated RT cycle. Combined therapy resulted in curative responses in a high proportion of mice bearing established CT26 tumors which was dependent on the activity of CD8(+) T-cells but independent of CD4(+) T-cells and NK/NKT cells. Moreover, long-term surviving mice originally treated with DSR-29133 and RT were protected by a tumor-specific memory immune response which could prevent tumor growth upon rechallenge. These results demonstrate that DSR-29133 is a potent selective TLR7 agonist that when administered intravenously can induce anti-tumor immune responses that can be further enhanced through combination with low-dose fractionated RT.
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spelling pubmed-49413692016-07-19 Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy Dovedi, Simon J. Adlard, Amy L. Ota, Yosuke Murata, Masashi Sugaru, Eiji Koga-Yamakawa, Erina Eguchi, Ken Hirose, Yuko Yamamoto, Setsuko Umehara, Hiroki Honeychurch, Jamie Cheadle, Eleanor J. Hughes, Gareth Jewsbury, Philip J. Wilkinson, Robert W. Stratford, Ian J. Illidge, Timothy M. Oncotarget Research Paper Strategies to augment anti-cancer immune responses have recently demonstrated therapeutic utility. To date clinical success has been achieved through targeting co-inhibitory checkpoints such as CTLA-4, PD-1, and PD-L1. However, approaches that target co-activatory pathways are also being actively being developed. Here we report that the novel TLR7-selective agonist DSR-29133 is well tolerated in mice and leads to acute immune activation. Administration of DSR-29133 leads to the induction of IFNα/γ, IP-10, TNFα, IL-1Ra and IL-12p70, and to a reduction in tumor burden in syngeneic models of renal cancer (Renca), metastatic osteosarcoma (LM8) and colorectal cancer (CT26). Moreover, we show that the efficacy of DSR-29133 was significantly improved when administered in combination with low-dose fractionated radiotherapy (RT). Effective combination therapy required weekly administration of DSR-29133 commencing on day 1 of a fractionated RT treatment cycle, whereas no enhancement of radiation response was observed when DSR-29133 was administered at the end of the fractionated RT cycle. Combined therapy resulted in curative responses in a high proportion of mice bearing established CT26 tumors which was dependent on the activity of CD8(+) T-cells but independent of CD4(+) T-cells and NK/NKT cells. Moreover, long-term surviving mice originally treated with DSR-29133 and RT were protected by a tumor-specific memory immune response which could prevent tumor growth upon rechallenge. These results demonstrate that DSR-29133 is a potent selective TLR7 agonist that when administered intravenously can induce anti-tumor immune responses that can be further enhanced through combination with low-dose fractionated RT. Impact Journals LLC 2016-03-05 /pmc/articles/PMC4941369/ /pubmed/26959743 http://dx.doi.org/10.18632/oncotarget.7928 Text en Copyright: © 2016 Dovedi et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Dovedi, Simon J.
Adlard, Amy L.
Ota, Yosuke
Murata, Masashi
Sugaru, Eiji
Koga-Yamakawa, Erina
Eguchi, Ken
Hirose, Yuko
Yamamoto, Setsuko
Umehara, Hiroki
Honeychurch, Jamie
Cheadle, Eleanor J.
Hughes, Gareth
Jewsbury, Philip J.
Wilkinson, Robert W.
Stratford, Ian J.
Illidge, Timothy M.
Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title_full Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title_fullStr Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title_full_unstemmed Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title_short Intravenous administration of the selective toll-like receptor 7 agonist DSR-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
title_sort intravenous administration of the selective toll-like receptor 7 agonist dsr-29133 leads to anti-tumor efficacy in murine solid tumor models which can be potentiated by combination with fractionated radiotherapy
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4941369/
https://www.ncbi.nlm.nih.gov/pubmed/26959743
http://dx.doi.org/10.18632/oncotarget.7928
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