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Signature amino acids enable the archaeal L7Ae box C/D RNP core protein to recognize and bind the K-loop RNA motif

机译:签名氨基酸使古细菌L7Ae盒C / D RNP核心蛋白能够识别并结合K环RNA基序

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摘要

The archaeal L7Ae and eukaryotic 15.5kD protein homologs are members of the L7Ae/15.5kD protein family that characteristically recognize K-turn motifs found in both archaeal and eukaryotic RNAs. In Archaea, the L7Ae protein uniquely binds the K-loop motif found in box C/D and H/ACA sRNAs, whereas the eukaryotic 15.5kD homolog is unable to recognize this variant K-turn RNA. Comparative sequence and structural analyses, coupled with amino acid replacement experiments, have demonstrated that five amino acids enable the archaeal L7Ae core protein to recognize and bind the K-loop motif. These signature residues are highly conserved in the archaeal L7Ae and eukaryotic 15.5kD homologs, but differ between the two domains of life. Interestingly, loss of K-loop binding by archaeal L7Ae does not disrupt C′/D′ RNP formation or RNA-guided nucleotide modification. L7Ae is still incorporated into the C′/D′ RNP despite its inability to bind the K-loop, thus indicating the importance of protein–protein interactions for RNP assembly and function. Finally, these five signature amino acids are distinct for each of the L7Ae/L30 family members, suggesting an evolutionary continuum of these RNA-binding proteins for recognition of the various K-turn motifs contained in their cognate RNAs.
机译:古细菌L7Ae和真核15.5kD蛋白同源物是L7Ae / 15.5kD蛋白家族的成员,其特征在于识别古细菌和真核RNA中都存在的K-turn模体。在古细菌中,L7Ae蛋白独特地结合在框C / D和H / ACA sRNA中发现的K环基序,而真核15.5kD同源物则无法识别这种变异的K-turn RNA。比较的序列和结构分析,再加上氨基酸替代实验,已证明五个氨基酸使古细菌L7Ae核心蛋白能够识别并结合K环基序。这些特征残基在古细菌L7Ae和真核15.5kD同源物中高度保守,但在生活的两个结构域之间有所不同。有趣的是,古细菌L7Ae失去K环结合不会破坏C'/ D'RNP的形成或RNA引导的核苷酸修饰。尽管L7Ae无法结合K环,但L7Ae仍被并入C'/ D'RNP中,因此表明蛋白质间相互作用对RNP组装和功能的重要性。最后,对于L7Ae / L30家族成员中的每一个,这五个签名氨基酸是不同的,这表明这些RNA结合蛋白的进化连续体可以识别其同源RNA中包含的各种K-turn基序。

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  • 来源
    《RNA》 |2010年第1期|79-90|共12页
  • 作者单位

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

    Department of Chemistry, Wake Forest University, Winston-Salem, North Carolina 27109, USA;

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

    Department of Molecular and Structural Biochemistry, North Carolina State University, Raleigh, North Carolina 27695, USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    box C/D snoRNA; snoRNP; kink-turn; L7Ae/L30 proteins; RNA–protein interaction;

    机译:盒C / D snoRNA;snoRNP;扭折;L7Ae / L30蛋白质;RNA-蛋白质相互作用;

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