Corrales Leticia, Glickman Laura Hix, McWhirter Sarah M, Kanne David B, Sivick Kelsey E, Katibah George E, Woo Seng-Ryong, Lemmens Edward, Banda Tamara, Leong Justin J, Metchette Ken, Dubensky Thomas W, Gajewski Thomas F
Department of Pathology, The University of Chicago, 929 E57th Street GCIS 3H, Chicago, IL 60637, USA.
Aduro BioTech, Inc., 626 Bancroft Way, 3C, Berkeley, CA 94710, USA.
Cell Rep. 2015 May 19;11(7):1018-30. doi: 10.1016/j.celrep.2015.04.031. Epub 2015 May 7.
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 generated substantial systemic immune responses capable of rejecting distant metastases and providing long-lived immunologic memory. Synthetic CDNs have high translational potential as a cancer therapeutic.
自发性肿瘤引发的T细胞启动依赖于肿瘤驻留树突状细胞产生的IFN-β。基于基于最近的观察结果表明IFN-β的表达依赖于宿主STING通路的激活,基于此,我们推测通过瘤内(IT)给予特异性激动剂直接激活STING将产生有效的抗肿瘤治疗效果。在使用小鼠STING激动剂DMXAA进行的原理验证研究显示出强大的治疗效果后,我们合成了能够激活所有人类STING等位基因以及小鼠STING的环状二核苷酸(CDN)衍生物。瘤内注射STING激动剂可使小鼠体内已建立的肿瘤显著消退,并产生强大的全身免疫反应,能够排斥远处转移灶并提供长期免疫记忆。合成CDN作为一种癌症治疗药物具有很高的转化潜力。
