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Cancer immunity is subjected to spatiotemporal regulation by leukocyte interaction with neoplastic and stromal cells, contributing to immune evasion and immunotherapy resistance. Here, we identify a distinct mesenchymal-like population of endothelial cells (ECs) that form an immunosuppressive vascular niche in glioblastoma (GBM). We reveal a spatially restricted, Twist1/SATB1-mediated sequential transcriptional activation mechanism, through which tumor ECs produce osteopontin to promote immunosuppressive macrophage (Mφ) phenotypes. Genetic or pharmacological ablation of Twist1 reverses Mφ-mediated immunosuppression and enhances T cell infiltration and activation, leading to reduced GBM growth and extended mouse survival, and sensitizing tumor to chimeric antigen receptor T immunotherapy. Thus, these findings uncover a spatially restricted mechanism controlling tumor immunity and suggest that targeting endothelial Twist1 may offer attractive opportunities for optimizing cancer immunotherapy.more » « less
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Redox-switchable polymerization has drawn increasing attention, in particular for the ring-opening polymerization (ROP) of biomass-derived monomers. However, an understanding of how the switch determines the observed changes is still limited. In this study, DFT calculations were employed to understand the redox-switchable ROP mechanism of ε-caprolactone catalyzed by group 4 metal complexes bearing [OSSO]-type ferrocene ligands. Our results suggest that two oxidized forms show higher reactivity because of the higher Lewis acidity of their catalytic metal centers in comparison with that of the corresponding reduced states. In one case, however, a lower activity of the oxidized species was observed that is likely due to the increased stability of the substrate-catalyst intermediate leading to a high activation barrier. In addition, other analogous metal complexes were computationally modelled by changing the metal center or modifying the ancillary ligand with different bridging-heteroatoms, and the results provide useful information on the development of new redox-switchable polymerization catalysts.more » « less
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