| Literature DB >> 28680743 |
Yanling Sun1, Zu'an Zheng2, Huafeng Zhang1, Yuandong Yu1, Jingwei Ma1,3, Ke Tang1, Pingwei Xu1, Tiantian Ji1, Xiaoyu Liang4, Degao Chen4, Xun Jin4, Tianzhen Zhang4, Zhixiong Long5, Yuying Liu4,6, Bo Huang1,4,6.
Abstract
Stem cell-like tumor-repopulating cells (TRCs) have a critical role in establishing a tumor immunosuppressive microenvironment. However, means to enhance antitumor immunity by disrupting TRCs are absent. Our previous studies have shown that tumor cell-derived microparticles (T-MPs) preferentially abrogate TRCs by delivering antitumor drugs into nuclei of TRCs. Here, we show that low dose irradiation (LDI) enhances the effect of cisplatin-packaging T-MPs (Cis-MPs) on TRCs, leading to inhibiting tumor growth in different tumor models. This antitumor effect is not due to the direct killing of tumor cells but is T cell-dependent and relies on macrophages for their efficacy. The underlying mechanism is involved in therapeutic reprograming macrophages from tumor-promotion to tumor-inhibition by disrupting TRCs and curtailing their vicious education on macrophages. These findings provide a novel strategy to reset macrophage polarization and confer their function more like M1 than M2 types with highly promising potential clinical applications.Entities:
Keywords: Drug-packaging microparticles; antitumor immunity; low-dose irradiation; macrophage remodeling; tumor-repopulating cells
Year: 2017 PMID: 28680743 PMCID: PMC5486181 DOI: 10.1080/2162402X.2017.1309487
Source DB: PubMed Journal: Oncoimmunology ISSN: 2162-4011 Impact factor: 8.110