2020
DOI: 10.1371/journal.pone.0237743
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G10 is a direct activator of human STING

Abstract: The cGAS/STING pathway initiates an innate immune response when DNA is detected in the cytosol. DNA bound cGAS synthesizes cyclic dinucleotides which bind and activate the adaptor STING, leading to downstream secretion of Type I interferons and other pro-inflammatory NFκB pathway cytokines. In the mouse, the STING driven innate immune response is central to immune based clearance of various tumors and this has triggered a significant effort focused on the discovery of human STING agonists for the treatment of … Show more

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Cited by 21 publications
(16 citation statements)
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“…G10 was shown to selectively activate INF/IRF3 signaling. While it was postulated that the agonistic effects may not be due to the direct activation of STING by G10, in vitro experiments utilizing the stimulation of HEK293T harboring a luciferase reporter expressed with an ISRE/ISG promoter using G10 confirmed G10 to be a weak direct binder of STING, with differing potencies to the STING variant expressed [79].…”
Section: Discussionmentioning
confidence: 99%
“…G10 was shown to selectively activate INF/IRF3 signaling. While it was postulated that the agonistic effects may not be due to the direct activation of STING by G10, in vitro experiments utilizing the stimulation of HEK293T harboring a luciferase reporter expressed with an ISRE/ISG promoter using G10 confirmed G10 to be a weak direct binder of STING, with differing potencies to the STING variant expressed [79].…”
Section: Discussionmentioning
confidence: 99%
“…Scientists at Curadev Pharma discovered that certain bicyclic benzamides could target the STING pathway as the compounds demonstrated the ability to induce the production of STING-associated cytokines ( e.g. , type I IFNs, CXCL10, and TNF-α). Notably, a set of three intratumoral injections of their lead compounds administered every other day led to significant suppression of tumor growth in BALB/c mice with hSTING-expressing CT26 tumors. Investigators at Merck explored benzothiophene derivatives in the context of STING activation and identified compounds with micromolar potency in both direct STING binding and a cellular reporter assay for type I IFN production .…”
Section: Sting Pathway Agonistsmentioning
confidence: 99%
“…[31] Unlike CDN-mimetic STING agonists, G10, a human STING agonist, agonized STING-IRF3 cascade by directly interacting with human STING protein. [32] Although this report did not include STING-mediated cancer immunotherapy, G10 might be utilized for cancer immunotherapy in clinical models as G10 has strong affinity with human STING protein and can initiate STING activation. [32] Up to this point, all the STING agonists discussed have been administered intratumorally, to improve in their clinical translation, recent studies have aimed at systemically administrable STING agonists.…”
Section: Sting-binding Moleculesmentioning
confidence: 99%