Yan Nan
Department of Immunology, Department of Microbiology, University of Texas Southwestern Medical Center , Dallas, Texas.
J Interferon Cytokine Res. 2017 May;37(5):198-206. doi: 10.1089/jir.2016.0086.
The innate immune system is the first line of defense against invading pathogens. One important feature of innate immune recognition is self versus nonself discrimination. The selectivity for microbial ligands is achieved through substrate motif specificity, spatial compartmentalization, and functions of negative regulators. Loss-of-function mutations in negative regulators or gain-of-function mutations in drivers of innate immune signaling have been associated with autoimmune diseases such as lupus, rheumatoid arthritis, inflammatory vasculopathy, and a variety of interferonopathies. This review will focus on TREX1 and STING, which are opposing regulators of the cytosolic DNA-sensing pathway. Tremendous effort over the past decade among academic and clinical research groups has elucidated molecular mechanisms underlying immune diseases associated with TREX1 and STING dysfunction. We have also witnessed rapid therapeutic translation of the molecular findings. Several targeted treatment options or druggable candidates are now available for these once incurable diseases. With great enthusiasm from both academia and industry partners, we look forward to seeing the remaining scientific questions answered and, more importantly, the affected patients benefited from these discoveries.
先天免疫系统是抵御入侵病原体的第一道防线。先天免疫识别的一个重要特征是自我与非自我的区分。对微生物配体的选择性是通过底物基序特异性、空间分隔和负调节因子的功能来实现的。负调节因子的功能丧失突变或先天免疫信号传导驱动因子的功能获得突变与自身免疫性疾病有关,如狼疮、类风湿性关节炎、炎症性血管病和多种干扰素病。本综述将聚焦于TREX1和STING,它们是胞质DNA传感途径的相反调节因子。在过去十年中,学术和临床研究团队付出了巨大努力,阐明了与TREX1和STING功能障碍相关的免疫疾病的分子机制。我们也见证了分子研究成果在治疗上的迅速转化。对于这些曾经无法治愈的疾病,现在有几种靶向治疗方案或可成药的候选药物。在学术界和行业合作伙伴的极大热情推动下,我们期待看到剩下的科学问题得到解答,更重要的是,让受影响的患者从这些发现中受益。
