Litcius/Paper detail

A Fc-VEGF chimeric fusion enhances PD-L1 immunotherapy via inducing immune reprogramming and infiltration in the immunosuppressive tumor microenvironment

Cheng‐Liang Kuo, Han-Yu Chou, Hui‐Wen Lien, Chia-An Yeh, Jingrong Wang, Chung–Hsing Chen, Chi‐Chen Fan, Chih‐Ping Hsu, Ting‐Yu Kao, Tai-Ming Ko, Alan Yueh‐Luen Lee

2022Cancer Immunology Immunotherapy18 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Immunotherapy is an emerging cancer therapy with potential great success; however, immune checkpoint inhibitor (e.g., anti-PD-1) has response rates of only 10-30% in solid tumor because of the immunosuppressive tumor microenvironment (TME). This affliction can be solved by vascular normalization and TME reprogramming. METHODS: By using the single-cell RNA sequencing (scRNAseq) approach, we tried to find out the reprogramming mechanism that the Fc-VEGF chimeric antibody drug (Fc-VFD) enhances immune cell infiltration in the TME. RESULTS: (Fc-VEGF chimeric antibody drug, Fc-VFD) arrests excess angiogenesis and tumor growth through vascular normalization using in vitro and in vivo studies. The results confirmed that the treatment of Fc-VFD increases immune cell infiltration including cytotoxic T, NK, and M1-macrophages cells. Indeed, Fc-VFD inhibits Lon-induced M2 macrophages polarization that induces angiogenesis. Furthermore, Fc-VFD inhibits the secretion of VEGF-A, IL-6, TGF-β, or IL-10 from endothelial, cancer cells, and M2 macrophage, which reprograms immunosuppressive TME. Importantly, Fc-VFD enhances the synergistic effect on the combination immunotherapy with anti-PD-L1 in vivo. CONCLUSIONS: In short, Fc-VFD fusion normalizes intratumor vasculature to reprogram the immunosuppressive TME and enhance cancer immunotherapy.

Topics & Concepts

ReprogrammingImmunotherapyImmune systemInfiltration (HVAC)Tumor microenvironmentVEGF receptorsCancer researchImmunologyMedicineChemistryCellMaterials scienceComposite materialBiochemistryCAR-T cell therapy researchSingle-cell and spatial transcriptomicsMonoclonal and Polyclonal Antibodies Research