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Amplified Cancer Immunotherapy of a Surface-Engineered Antigenic Microparticle Vaccine by Synergistically Modulating Tumor Microenvironment

ACS Nano.. 2019; 
Zhao H1,2, Zhao B1, Wu L1, Xiao H1, Ding K1, Zheng C1, Song Q1, Sun L1, Wang L1,2,3, Zhang Z1,2,3.
Products/Services Used Details Operation
Peptide Synthesis Red blood cells were removed using lysis buffer per the manufacturer’s instructions. 2×105 splenocytes were then plated into a mouse IFN-γ ELISPOT Kit plates (DAKEWE, China) in RPMI 1640 growth media with either 2 μg/ml of gp100 peptide (EGSRNQDWL, Genscript) or 2 μg/ml of TRP2 peptide (SVYDFFVWL, Genscript) for 24 h. Get A Quote

摘要

Efficient cancer vaccines not only require the co-delivery of potent antigens and highly immunostimulatory adjuvants to initiate robust tumor-specific host immune response but also solve the spatiotemporal consistency of host immunity and tumor microenvironment (TME) immunomodulation. Here, we designed a biomaterials-based strategy for converting tumor-derived antigenic microparticles (T-MPs) into a cancer vaccine to meet this conundrum and demonstrated its therapeutic potential in multiple murine tumor models. The internal cavity of T-MPs was employed to store nano-Fe3O4 (Fe3O4/T-MPs), and then dense adjuvant CpG-loaded liposome arrays (CpG/Lipo) were tethered on the surface of Fe3O4/T-MP through mild surface ... More

关键词

anticancer vaccine; cell-engineering; immunomodulation; spatiotemporal; tumor microenvironment