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The mechanism of RNA duplex recognition and unwinding by DEAD-box helicase DDX3X

机译:死箱螺旋酶DDX3x RNA双工识别和展开的机制

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摘要

DEAD-box helicases (DDXs) regulate RNA processing and metabolism by unwinding short double-stranded (ds) RNAs. Sharing a helicase core composed of two RecA-like domains (D1D2), DDXs function in an ATP-dependent, non-processive manner. As an attractive target for cancer and AIDS treatment, DDX3X and its orthologs are extensively studied, yielding a wealth of biochemical and biophysical data, including structures of apo-D1D2 and post-unwound D1D2:single-stranded RNA complex, and the structure of a D2:dsRNA complex that is thought to represent a pre-unwound state. However, the structure of a pre-unwound D1D2:dsRNA complex remains elusive, and thus, the mechanism of DDX action is not fully understood. Here, we describe the structure of a D1D2 core in complex with a 23-base pair dsRNA at pre-unwound state, revealing that two DDXs recognize a 2-turn dsRNA, each DDX mainly recognizes a single RNA strand, and conformational changes induced by ATP binding unwinds the RNA duplex in a cooperative manner.
机译:死箱螺旋酶(DDXS)通过释放短的双链(DS)RNA来调节RNA处理和代谢。共享由两个RECA样域(D1D2),DDXS函数以ATP相关的,非加工方式共享螺旋酶核心。作为癌症和艾滋病治疗的有吸引力的靶标,DDX3X及其矫正物被广泛研究,产生了丰富的生化和生物物理数据,包括APO-D1D2和后退D1D2的结构:单链RNA复合物,以及A的结构D2:被认为代表预展示状态的DSRNA复合物。然而,预先解序D1D2的结构:DSRNA复合物仍然难以捉摸,因此,DDX动作的机制尚不完全理解。在这里,我们描述了在预展示状态下与23碱基对DsRNA复合物的D1D2核的结构,揭示了两个DDXS识别2转序列,每个DDX主要识别单个RNA链,并诱导构象变化ATP绑定以合作方式向RNA双工展开。

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