A Common Structural Motif in Elongation Factor Ts and Ribosomal Protein L7/12 May Be Involved in the Interaction with Elongation Factor Tu

被引:0
|
作者
Hans-Joachim Wieden
Wolfgang Wintermeyer
Marina V. Rodnina
机构
[1] Institute of Physical Biochemistry,
[2] University of Witten/Herdecke,undefined
[3] 58448 Witten,undefined
[4] Germany,undefined
[5] Institute of Molecular Biology,undefined
[6] University of Witten/Herdecke,undefined
[7] 58448 Witten,undefined
[8] Germany,undefined
来源
Journal of Molecular Evolution | 2001年 / 52卷
关键词
Key words: Protein synthesis — Nucleotide exchange — Translation — Ribosomal proteins;
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摘要
Elongation factor (EF) Tu alternates between two interaction partners, EF-Ts and the ribosome, during its functional cycle. On the ribosome, the interaction involves, among others, ribosomal protein L7/12. Here we compare EF-Ts and L7/12 with respect to the conservation of sequence and structure. There is significant conservation of functionally important residues in the N-terminal domain of EF-Ts and in the C-terminal domain of L7/12. The structure alignment based on the crystal structures of the two domains suggests a high degree of similarity between the αA–βD–αB motif in L7/12 and the h1–turn–h2 motif in EF-Ts which defines a common structural motif. The motif is remarkably similar with respect to fold, bulkiness, and charge distribution of the solution surface, suggesting that it has a common function in binding EF-Tu.
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页码:129 / 136
页数:7
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