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通过核苷酸类似物干扰图谱研究发夹状核酶中腺苷碱基的电离作用。

Investigation of adenosine base ionization in the hairpin ribozyme by nucleotide analog interference mapping.

作者信息

Ryder S P, Oyelere A K, Padilla J L, Klostermeier D, Millar D P, Strobel S A

机构信息

Yale University, Department of Molecular Biophysics and Biochemistry, New Haven, Connecticut 06520-8114, USA.

出版信息

RNA. 2001 Oct;7(10):1454-63.

Abstract

Tertiary structure in globular RNA folds can create local environments that lead to pKa perturbation of specific nucleotide functional groups. To assess the prevalence of functionally relevant adenosine-specific pKa perturbation in RNA structure, we have altered the nucleotide analog interference mapping (NAIM) approach to include a series of a phosphorothioate-tagged adenosine analogs with shifted N1 pKa values. We have used these analogs to analyze the hairpin ribozyme, a small self-cleaving/ligating RNA catalyst that is proposed to employ a general acid-base reaction mechanism. A single adenosine (A10) within the ribozyme active site displayed an interference pattern consistent with a functionally significant base ionization. The exocyclic amino group of a second adenosine (A38) contributes substantially to hairpin catalysis, but ionization of the nucleotide does not appear to be important for activity. Within the hairpin ribozyme crystal structure, A10 and A38 line opposite edges of a solvent-excluded cavity adjacent to the 5'-OH nucleophile. The results are inconsistent with the model of ribozyme chemistry in which A38 acts as a general acid-base catalyst, and suggest that the hairpin ribozyme uses an alternative mechanism to achieve catalytic rate enhancement that utilizes functional groups within a solvent-excluded cleft in the ribozyme active site.

摘要

球状RNA折叠中的三级结构可形成局部环境,导致特定核苷酸官能团的pKa发生扰动。为了评估RNA结构中功能相关的腺苷特异性pKa扰动的普遍性,我们改进了核苷酸类似物干扰图谱(NAIM)方法,纳入了一系列N1 pKa值发生偏移的硫代磷酸酯标记的腺苷类似物。我们使用这些类似物分析了发夹状核酶,这是一种小型的自我切割/连接RNA催化剂,有人提出它采用一般酸碱反应机制。核酶活性位点内的单个腺苷(A10)显示出与功能上重要的碱基电离一致的干扰模式。第二个腺苷(A38)的环外氨基对发夹催化有很大贡献,但该核苷酸的电离似乎对活性并不重要。在发夹状核酶晶体结构中,A10和A38位于与5'-OH亲核试剂相邻的溶剂排除腔的相对边缘。这些结果与A38作为一般酸碱催化剂的核酶化学模型不一致,并表明发夹状核酶使用一种替代机制来提高催化速率,该机制利用核酶活性位点中溶剂排除裂缝内的官能团。

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