Infectious and Inflammatory Disease Center, Sanford-Burnham Medical Research Institute, La Jolla, CA 92037, USA.
Cell Host Microbe. 2012 Mar 15;11(3):306-18. doi: 10.1016/j.chom.2012.02.002.
Pathogens commonly utilize endocytic pathways to gain cellular access. The endosomal pattern recognition receptors TLR7 and TLR9 detect pathogen-encoded nucleic acids to initiate MyD88-dependent proinflammatory responses to microbial infection. Using genome-wide RNAi screening and integrative systems-based analysis, we identify 190 cofactors required for TLR7- and TLR9-directed signaling responses. A set of cofactors were crossprofiled for their activities downstream of several immunoreceptors and then functionally mapped based on the known architecture of NF-κB signaling pathways. Protein complexes and pathways involved in ubiquitin-protein ligase activities, sphingolipid metabolism, chromatin modifications, and ancient stress responses were found to modulate innate recognition of endosomal nucleic acids. Additionally, hepatocyte growth factor-regulated tyrosine kinase substrate (HRS) was characterized as necessary for ubiquitin-dependent TLR9 targeting to the endolysosome. Proteins and pathways identified here should prove useful in delineating strategies to manipulate innate responses for treatment of autoimmune disorders and microbial infection.
病原体通常利用内吞途径进入细胞。内体模式识别受体 TLR7 和 TLR9 检测病原体编码的核酸,以启动 MyD88 依赖性促炎反应,从而对微生物感染做出反应。我们使用全基因组 RNAi 筛选和基于整合系统的分析,鉴定了 190 种 TLR7 和 TLR9 信号转导所需的共因子。一组共因子根据几种免疫受体下游的活性进行交叉分析,然后根据 NF-κB 信号通路的已知结构进行功能映射。涉及泛素-蛋白连接酶活性、鞘脂代谢、染色质修饰和古老应激反应的蛋白质复合物和途径被发现可调节内体核酸的先天识别。此外,还发现肝细胞生长因子调节的酪氨酸激酶底物 (HRS) 是 TLR9 靶向内溶酶体所必需的。这里鉴定的蛋白质和途径对于制定策略来操纵先天反应以治疗自身免疫性疾病和微生物感染应该是有用的。
