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Development of Potent Immune Modulators Targeting Stimulator of Interferon Genes Receptor.

Min Jae JeonHyelim LeeJeehee LeeSoo Yeon BaekDonghee LeeSeongman JoJoo-Youn LeeMiso KangHee Ra JungSoo Bong HanNam-Jung KimSanghee LeeHyejin Kim
Published in: Journal of medicinal chemistry (2022)
Stimulator of interferon genes (STING) is an endoplasmic reticulum-membrane protein that plays important roles in cancer immunotherapy by activating innate immune responses. We designed and synthesized STING modulators and characterized compounds 4a and 4c that share a crucial amidobenzimidazole moiety. In vitro STING binding and cell-based activity assays demonstrated the potency and efficacy of the compounds that function as direct STING agonists by stimulating STING downstream signaling and promoting type I interferon immune responses. In vitro metabolic studies and the pharmacokinetic properties of the compounds led us to investigate their anticancer activity in an in vivo syngeneic model . Intravenous injection of compounds 4a and 4c significantly decreased tumor volume in a CT26 murine colorectal carcinoma model, and the immunological memory-derived cancer inhibition was observed in 4c -treated mouse models. The present results suggest the therapeutic potential of the compounds for cancer immunotherapy via STING-mediated immune activation .
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