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Ribosome Subunit Stapling for Orthogonal Translation in E. coli

机译:核糖体亚基吻合在大肠杆菌中的正交翻译

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摘要

The creation of orthogonal large and small ribosomal subunits, which interact with each other but not with endogenous ribosomal subunits, would extend our capacity to create new functions in the ribosome by making the large subunit evolvable. To this end, we rationally designed a ribosomal RNA that covalently links the ribosome subunits via an RNA staple. The stapled ribosome is directed to an orthogonal mRNA, allowing the introduction of mutations into the large subunit that reduce orthogonal translation, but have minimal effects on cell growth. Our approach provides a promising route towards orthogonal subunit association, which may enable the evolution of key functional centers in the large subunit, including the peptidyl-transferase center, for unnatural polymer synthesis in cells.
机译:相互正交但不与内源性核糖体亚基相互作用的正交大和小的核糖体亚基,将扩大我们通过使大亚基可进化而在核糖体中产生新功能的能力。为此,我们合理地设计了一个核糖体RNA,该RNA通过RNA钉共价连接核糖体亚基。装订的核糖体直接针对正交的mRNA,可将突变引入大亚基中,从而减少正交翻译,但对细胞生长的影响却很小。我们的方法为正交亚基缔合提供了一条有希望的途径,它可能使大亚基中关键功能中心(包括肽基转移酶中心)的进化成为细胞中非天然聚合物的合成。

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