Structural Biology Program, Memorial Sloan-Kettering Cancer Center, New York, New York, USA.
Nat Struct Mol Biol. 2010 Jul;17(7):781-7. doi: 10.1038/nsmb.1863. Epub 2010 Jun 27.
RIG-I is a cytosolic helicase that senses 5'-ppp RNA contained in negative-strand RNA viruses and triggers innate antiviral immune responses. Calorimetric binding studies established that the RIG-I C-terminal regulatory domain (CTD) binds to blunt-end double-stranded 5'-ppp RNA a factor of 17 more tightly than to its single-stranded counterpart. Here we report on the crystal structure of RIG-I CTD bound to both blunt ends of a self-complementary 5'-ppp dsRNA 12-mer, with interactions involving 5'-pp clearly visible in the complex. The structure, supported by mutation studies, defines how a lysine-rich basic cleft within the RIG-I CTD sequesters the observable 5'-pp of the bound RNA, with a stacked phenylalanine capping the terminal base pair. Key intermolecular interactions observed in the crystalline state are retained in the complex of 5'-ppp dsRNA 24-mer and full-length RIG-I under in vivo conditions, as evaluated from the impact of binding pocket RIG-I mutations and 2'-OCH(3) RNA modifications on the interferon response.
RIG-I 是一种胞质解旋酶,可识别负链 RNA 病毒中的 5'-ppp RNA,并触发先天抗病毒免疫反应。量热结合研究表明,RIG-I C 端调节结构域(CTD)与平端双链 5'-ppp RNA 的结合亲和力比其单链对应物高 17 倍。在此,我们报告了 RIG-I CTD 与自我互补的 5'-ppp dsRNA 12 聚体的两个平端结合的晶体结构,复合物中清楚地显示了 5'-pp 的相互作用。该结构得到突变研究的支持,定义了 RIG-I CTD 内富含赖氨酸的碱性裂隙如何隔离结合 RNA 的可观察到的 5'-pp,一个堆叠的苯丙氨酸覆盖末端碱基对。从结合口袋 RIG-I 突变和 2'-OCH(3) RNA 修饰对干扰素反应的影响评估,在体内条件下,在 5'-ppp dsRNA 24 聚体和全长 RIG-I 的复合物中保留了观察到的关键分子间相互作用。
Zotero 插件
