Direct Activation of STING in the Tumor Microenvironment Leads to Potent and Systemic Tumor Regression and Immunity

Corrales, Leticia; Glickman, Laura Hix; McWhirter, Sarah M.; Kanne, David B.; Sivick, Kelsey E.; Katibah, George E.; Woo, Seng‐Ryong; Lemmens, Edward E.; Banda, Tamara; Leong, Justin J.; Metchette, Ken; Dubensky, Thomas W.; Gajewski, Thomas F.

doi:10.1016/j.celrep.2015.04.031

articleCell ReportsMay 1, 2015GOLD OA

Direct Activation of STING in the Tumor Microenvironment Leads to Potent and Systemic Tumor Regression and Immunity

LCLeticia Corrales LHLaura Hix Glickman SMSarah M. McWhirter DBDavid B. Kanne KEKelsey E. Sivick

University of Chicago · Aduro BioTech (United States)

PubMed

Indexed incrossrefdoajpubmed

Abstract

Spontaneous tumor-initiated T cell priming is dependent on IFN-β production by tumor-resident dendritic cells. On the basis of recent observations indicating that IFN-β expression was dependent upon activation of the host STING pathway, we hypothesized that direct engagement of STING through intratumoral (IT) administration of specific agonists would result in effective anti-tumor therapy. After proof-of-principle studies using the mouse STING agonist DMXAA showed a potent therapeutic effect, we generated synthetic cyclic dinucleotide (CDN) derivatives that activated all human STING alleles as well as murine STING. IT injection of STING agonists induced profound regression of established tumors in mice and…

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Topics & keywords

Topics

Keywords

Sting
Tumor microenvironment
Immunity
Immunology
Cancer research
Innate immune system
Biology
Medicine

UN Sustainable Development Goals

Good health and well-being

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Funding

UO
University of California Berkeley