A gp130-Src-YAP module links inflammation to epithelial regeneration

摘要

除了激发先天和后天免疫外，炎症还能通过我们基本上还不知道的机制触发组织修复和再生。这项研究在一个小鼠实验性结肠炎模型中显示了一个独立于STAT3的治愈通道通过涉及gp130(白介素-6家族细胞因子的一个共受体)和下游效应子Src、Yes、YAP及Notch的一个过程是如何被激发的。%Inflammation promotes regeneration of injured tissues through poorly understood mechanisms, some of which involve interleukin (IL)-6 family members, the expression of which is elevated in many diseases including inflammatory bowel diseases and colorectal cancer. Here we show in mice and human cells that gp130, a co-receptor for IL- 6 cytokines, triggers activation of YAP and Notch, transcriptional regulators that control tissue growth and regeneration, independently of the gp130 effector STAT3. Through YAP and Notch, intestinal gp130 signalling stimulates epithelial cell proliferation, causes aberrant differentiation and confers resistance to mucosal erosion. gp130 associates with the related tyrosine kinases Src and Yes, which are activated on receptor engagement to phosphorylate YAP and induce its stabilization and nuclear translocation. This signalling module is strongly activated upon mucosal injury to promote healing and maintain barrier function.