| Literature DB >> 31343989 |
Hannah Yang1,2, Won Suk Lee1,2, So Jung Kong1,2, Chang Gon Kim3, Joo Hoon Kim1,2, Sei Kyung Chang4, Sewha Kim5, Gwangil Kim5, Hong Jae Chon1,2, Chan Kim1,2.
Abstract
The stimulator of interferon genes (STING) signaling pathway is a critical link between innate and adaptive immunity, and induces anti-tumor immune responses. STING is expressed in vasculatures, but its role in tumor angiogenesis has not been elucidated. Here we investigated STING-induced tumor vascular remodeling and the potential of STING-based combination immunotherapy. Endothelial STING expression was correlated with enhanced T-cell infiltration and prolonged survival in human colon and breast cancer. Intratumoral STING activation with STING agonists (cGAMP or RR-CDA) normalized tumor vasculatures in implanted and spontaneous cancers, but not in STING-deficient mice. These were mediated by upregulation of type I/II interferon genes and vascular stabilizing genes (e.g., Angpt1, Pdgfrb, and Col4a). STING in non-hematopoietic cells is as important as STING in hematopoietic cells to induce a maximal therapeutic efficacy of exogenous STING agonist. Vascular normalizing effects of STING agonists were dependent on type I interferon signaling and CD8+ T cells. Notably, STING-based immunotherapy was maximally effective when combined with VEGFR2 blockade and/or immune checkpoint blockade (αPD-1 or αCTLA-4), leading to complete regression of immunotherapy-resistant tumors. Our data show that intratumoral STING activation can normalize tumor vasculature and the tumor microenvironment, providing a rationale for combining STING-based immunotherapy and anti-angiogenic therapy.Entities:
Keywords: Angiogenesis; Cancer; Cancer immunotherapy; Immunology; endothelial cells
Year: 2019 PMID: 31343989 PMCID: PMC6763266 DOI: 10.1172/JCI125413
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808