Affiliation:
1. Laboratory of DDS Design and Drug Disposition Graduate School of Pharmaceutical Sciences Chiba University 1‐8‐1 Inohana, Chuo‐ku Chiba City Chiba 260‐0856 Japan
2. Laboratory of Drug Design and Drug Disposition Graduate School of Pharmaceutical Sciences Tohoku University 6‐3 Aoba, Aramaki, Aoba‐ku Sendai 980‐8578 Japan
Abstract
AbstractThe reactivation of anticancer immunity is a fundamental principle in cancer immunotherapy as evidenced by the use of immune checkpoint inhibitors (ICIs). While treatment with the ICIs is shown to have remarkable and durable therapeutic effects in the responders, the low objective response rate (<40%) continues to be a major problem. Since myeloid‐derived suppressor cells (MDSCs), heterogenous cells with strong immunosuppressive activity that originate in the hematopoietic system, suppress the anticancer immunity via parallel immune checkpoint‐dependent and independent pathways, these cells are potential targets for improving the efficacy of cancer immunotherapy. In this study, it is demonstrated that MDSCs can be depleted by delivering synthetic glucocorticoid dexamethasone to phagocytic cells in the spleen using a lipid nanoparticle. Since the interaction of nanoparticles with T cells is intrinsically poor, this strategy also enables the “detargeting” from T cells, thus avoiding the nonspecific suppression of cytotoxic immune responses against cancer cells. In addition to the direct anticancer effect of the nanoparticulated dexamethasone, their synergistic anticancer effect with ICIs is also reported.
Funder
Kato Memorial Bioscience Foundation
Japan Science and Technology Corporation
Core Research for Evolutional Science and Technology
Takeda Science Foundation
Japan Society for the Promotion of Science
Subject
Biomaterials,Biotechnology,General Materials Science,General Chemistry
Cited by
1 articles.
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