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Evolutionary optimization of a modular ligase ribozyme: a small catalytic unit and a hairpin motif masking an element that could form an inactive structure

机译:模块化连接酶核酶的进化优化:一个小的催化单元和一个发夹基序掩盖了可能形成无活性结构的元素

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摘要

The YFL ribozyme is an artificial ligase ribozyme isolated by a 'design and selection' strategy, in which a modular catalytic unit was generated on a rationally designed modular scaffold RNA. This ligase ribozyme has a versatile catalytic unit that accepts not only beta-nicotinamide mononucleotide (beta-NMN) but also inorganic pyrophosphate as leaving groups for template-dependent RNA ligation. Although this property is interesting from an evolutionary viewpoint regarding primitive RNA ligation/polymerization systems in the RNA world, structural analysis of the YFL ribozyme has not been continued due to apparent structural nonuniformity of its folded state. To elucidate the active structure of the YFL ribozyme, we performed in vitro evolution experiments to improve its folding ability. Biochemical and phylogenetic analyses of evolved variants indicated that the catalytic unit of the YFL ribozyme is compact and the 3' single-stranded region of the parent YFL-1 ribozyme contributes to mask an element that could form an inactive structure.
机译:YFL核酶是通过“设计和选择”策略分离的人工连接酶核酶,其中在合理设计的模块化支架RNA上生成了模块化催化单元。该连接酶核酶具有通用的催化单元,该单元不仅接受β-烟酰胺单核苷酸(β-NMN),而且还接受无机焦磷酸盐作为模板依赖性RNA连接的离去基团。尽管从关于RNA世界中原始RNA连接/聚合系统的进化观点来看,该性质是令人感兴趣的,但是由于其折叠状态的明显结构不均匀性,YFL核酶的结构分析尚未继续进行。为了阐明YFL核酶的活性结构,我们进行了体外进化实验以提高其折叠能力。进化变异的生化和系统发育分析表明,YFL核酶的催化单元很紧凑,亲本YFL-1核酶的3'单链区域有助于掩盖可能形成无活性结构的元素。

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