Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy

Strategies boosting both innate and adaptive immunity have great application prospects in cancer immunotherapy. Antibodies dual blocking the innate checkpoint CD47 and adaptive checkpoint PD-L1 or TIGIT could achieve durable anti-tumor effects. However, a small molecule dual blockade of CD47/SIRPα a...

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Autores principales: Zhou, Xiuman, Jiao, Ling, Qian, Yuzhen, Dong, Qingyu, Sun, Yixuan, Zheng, Wei V., Zhao, Wenshan, Zhai, Wenjie, Qiu, Lu, Wu, Yahong, Wang, Hongfei, Gao, Yanfeng, Chen, Junhui
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8150775/
https://www.ncbi.nlm.nih.gov/pubmed/34068552
http://dx.doi.org/10.3390/biom11050706
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author Zhou, Xiuman
Jiao, Ling
Qian, Yuzhen
Dong, Qingyu
Sun, Yixuan
Zheng, Wei V.
Zhao, Wenshan
Zhai, Wenjie
Qiu, Lu
Wu, Yahong
Wang, Hongfei
Gao, Yanfeng
Chen, Junhui
author_facet Zhou, Xiuman
Jiao, Ling
Qian, Yuzhen
Dong, Qingyu
Sun, Yixuan
Zheng, Wei V.
Zhao, Wenshan
Zhai, Wenjie
Qiu, Lu
Wu, Yahong
Wang, Hongfei
Gao, Yanfeng
Chen, Junhui
author_sort Zhou, Xiuman
collection PubMed
description Strategies boosting both innate and adaptive immunity have great application prospects in cancer immunotherapy. Antibodies dual blocking the innate checkpoint CD47 and adaptive checkpoint PD-L1 or TIGIT could achieve durable anti-tumor effects. However, a small molecule dual blockade of CD47/SIRPα and TIGIT/PVR pathways has not been investigated. Here, an elevated expression of CD47 and PVR was observed in tumor tissues and cell lines analyzed with the GEO datasets and by flow cytometry, respectively. Compounds approved by the FDA were screened with the software MOE by docking to the potential binding pockets of SIRPα and PVR identified with the corresponding structural analysis. The candidate compounds were screened by blocking and MST binding assays. Azelnidipine was found to dual block CD47/SIRPα and TIGIT/PVR pathways by co-targeting SIRPα and PVR. In vitro, azelnidipine could enhance the macrophage phagocytosis when co-cultured with tumor cells. In vivo, azelnidipine alone or combined with irradiation could significantly inhibit the growth of MC38 tumors. Azelnidipine also significantly inhibits the growth of CT26 tumors, by enhancing the infiltration and function of CD8(+) T cell in tumor and systematic immune response in the tumor-draining lymph node and spleen in a CD8(+) T cell dependent manner. Our research suggests that the anti-hypertensive drug azelnidipine could be repositioned for cancer immunotherapy.
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spelling pubmed-81507752021-05-27 Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy Zhou, Xiuman Jiao, Ling Qian, Yuzhen Dong, Qingyu Sun, Yixuan Zheng, Wei V. Zhao, Wenshan Zhai, Wenjie Qiu, Lu Wu, Yahong Wang, Hongfei Gao, Yanfeng Chen, Junhui Biomolecules Article Strategies boosting both innate and adaptive immunity have great application prospects in cancer immunotherapy. Antibodies dual blocking the innate checkpoint CD47 and adaptive checkpoint PD-L1 or TIGIT could achieve durable anti-tumor effects. However, a small molecule dual blockade of CD47/SIRPα and TIGIT/PVR pathways has not been investigated. Here, an elevated expression of CD47 and PVR was observed in tumor tissues and cell lines analyzed with the GEO datasets and by flow cytometry, respectively. Compounds approved by the FDA were screened with the software MOE by docking to the potential binding pockets of SIRPα and PVR identified with the corresponding structural analysis. The candidate compounds were screened by blocking and MST binding assays. Azelnidipine was found to dual block CD47/SIRPα and TIGIT/PVR pathways by co-targeting SIRPα and PVR. In vitro, azelnidipine could enhance the macrophage phagocytosis when co-cultured with tumor cells. In vivo, azelnidipine alone or combined with irradiation could significantly inhibit the growth of MC38 tumors. Azelnidipine also significantly inhibits the growth of CT26 tumors, by enhancing the infiltration and function of CD8(+) T cell in tumor and systematic immune response in the tumor-draining lymph node and spleen in a CD8(+) T cell dependent manner. Our research suggests that the anti-hypertensive drug azelnidipine could be repositioned for cancer immunotherapy. MDPI 2021-05-10 /pmc/articles/PMC8150775/ /pubmed/34068552 http://dx.doi.org/10.3390/biom11050706 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Zhou, Xiuman
Jiao, Ling
Qian, Yuzhen
Dong, Qingyu
Sun, Yixuan
Zheng, Wei V.
Zhao, Wenshan
Zhai, Wenjie
Qiu, Lu
Wu, Yahong
Wang, Hongfei
Gao, Yanfeng
Chen, Junhui
Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title_full Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title_fullStr Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title_full_unstemmed Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title_short Repositioning Azelnidipine as a Dual Inhibitor Targeting CD47/SIRPα and TIGIT/PVR Pathways for Cancer Immuno-Therapy
title_sort repositioning azelnidipine as a dual inhibitor targeting cd47/sirpα and tigit/pvr pathways for cancer immuno-therapy
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8150775/
https://www.ncbi.nlm.nih.gov/pubmed/34068552
http://dx.doi.org/10.3390/biom11050706
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