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An extended structural signature for the tRNA anticodon loop.

机译:tRNA反密码子环的扩展结构特征。

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摘要

Anticodon hairpins are structural motifs with contradictory functions. The recognition by aminoacyl synthetases implies extended interactions with the anticodon base triplet and thus, usually, an unfolding of the anticodon loop. The recognition by the ribosome and cognate interaction with a mRNA codon implies, on the other hand, the formation of a mini-helix with a canonical anticodon hairpin structure as observed by crystallography and NMR. To be able to understand the various properties of this motif, a precise description of its structural conservation is required. Here, on the basis of phylogenetic, structural, and molecular dynamics data, we discuss a conserved interaction established between the ribose of the U33 and the base at position 35, either a purine or a pyrimidine. This interaction involves the hydrogen bonding donor or acceptor potential of the hydroxyl group of U33 and has to be integrated in an extended definition of the anticodon hairpin. The extended structural signature provides also an explanation for the role played by pseudouridines at position 35.
机译:反密码子发夹是具有相反功能的结构图案。氨酰基合成酶的识别意味着与反密码子碱基三重态的相互作用延长,因此通常反密码子环的展开。另一方面,通过核糖体和同源相互作用与mRNA密码子的识别意味着通过晶体学和NMR观察到具有标准反密码子发夹结构的小螺旋的形成。为了能够理解该图案的各种特性,需要对其结构保守性进行精确描述。在这里,根据系统发育,结构和分子动力学数据,我们讨论U33核糖与35位碱基(嘌呤或嘧啶)之间建立的保守相互作用。此相互作用涉及U33羟基的氢键供体或受体电势,必须整合到反密码子发夹的扩展定义中。扩展的结构特征也为假尿苷在位置35上的作用提供了解释。

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