Gherghe Costin M, Mortimer Stefanie A, Krahn Joseph M, Thompson Nancy L, Weeks Kevin M
Department of Chemistry, University of North Carolina, Chapel Hill, North Carolina 27599-3290, USA.
J Am Chem Soc. 2008 Jul 16;130(28):8884-5. doi: 10.1021/ja802691e. Epub 2008 Jun 18.
RNA molecules undergo local conformational dynamics on timescales spanning picoseconds to minutes. Slower local motions have the greater potential to govern RNA folding, ligand recognition, and ribonucleoprotein assembly reactions but are difficult to detect in large RNAs with complex structures. RNA SHAPE chemistry employs acylation of the ribose 2'-hydroxyl position to measure local nucleotide flexibility in RNA and is well-characterized by a mechanism in which each nucleotide samples unreactive (closed) and reactive (open) states. We monitor RNA conformational dynamics over distinct time domains by varying the electrophilicity of the acylating reagent. Select C2'-endo nucleotides are nonreactive toward fast reagents but reactive toward slower SHAPE reagents in both model RNAs and in a large RNA with a tertiary fold. We conclude, first, that the C2'-endo conformation by itself does not govern SHAPE reactivity. However, some C2'-endo nucleotides undergo extraordinarily slow conformational changes, on the order of 10(-4) s(-1). Due to their distinctive local dynamics, C2'-endo nucleotides have the potential to function as rate-determining molecular switches and are likely to play central, currently unexplored, roles in RNA folding and function.
RNA分子在从皮秒到分钟的时间尺度上经历局部构象动力学变化。较慢的局部运动在控制RNA折叠、配体识别和核糖核蛋白组装反应方面具有更大的潜力,但在具有复杂结构的大型RNA中却难以检测到。RNA SHAPE化学方法利用核糖2'-羟基位置的酰化作用来测量RNA中局部核苷酸的灵活性,其机制已得到充分表征,即每个核苷酸会经历非反应性(闭合)和反应性(开放)状态。我们通过改变酰化试剂的亲电性来监测RNA在不同时间域内的构象动力学。在模型RNA和具有三级折叠的大型RNA中,特定的C2'-内型核苷酸对快速试剂无反应,但对较慢的SHAPE试剂有反应。我们首先得出结论,C2'-内型构象本身并不决定SHAPE反应性。然而,一些C2'-内型核苷酸会经历极其缓慢的构象变化,速率约为10^(-4) s^(-1)。由于其独特的局部动力学,C2'-内型核苷酸有可能作为速率决定性分子开关发挥作用,并且很可能在RNA折叠和功能中发挥目前尚未被探索的核心作用。
