STING suppresses bone cancer pain via immune and neuronal modulation.
Kaiyuan WangChristopher R DonnellyChangyu JiangYihan LiaoXin LuoXueshu TaoSangsu BangAidan McGinnisMichael LeeMatthew J HiltonRu-Rong JiPublished in: Nature communications (2021)
Patients with advanced stage cancers frequently suffer from severe pain as a result of bone metastasis and bone destruction, for which there is no efficacious treatment. Here, using multiple mouse models of bone cancer, we report that agonists of the immune regulator STING (stimulator of interferon genes) confer remarkable protection against cancer pain, bone destruction, and local tumor burden. Repeated systemic administration of STING agonists robustly attenuates bone cancer-induced pain and improves locomotor function. Interestingly, STING agonists produce acute pain relief through direct neuronal modulation. Additionally, STING agonists protect against local bone destruction and reduce local tumor burden through modulation of osteoclast and immune cell function in the tumor microenvironment, providing long-term cancer pain relief. Finally, these in vivo effects are dependent on host-intrinsic STING and IFN-I signaling. Overall, STING activation provides unique advantages in controlling bone cancer pain through distinct and synergistic actions on nociceptors, immune cells, and osteoclasts.
Keyphrases
- chronic pain
- papillary thyroid
- bone mineral density
- pain management
- bone loss
- squamous cell
- soft tissue
- lymph node metastasis
- risk factors
- gene expression
- squamous cell carcinoma
- childhood cancer
- signaling pathway
- postmenopausal women
- early onset
- liver failure
- genome wide
- endothelial cells
- mouse model
- drug delivery
- transcription factor
- extracorporeal membrane oxygenation
- innate immune