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首页> 外文期刊>Nucleic Acids Research >A critical switch in the enzymatic properties of the Cid1 protein deciphered from its product-bound crystal structure
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A critical switch in the enzymatic properties of the Cid1 protein deciphered from its product-bound crystal structure

机译:从其产品结晶结构中破译CID1蛋白的酶促性能的临界开关

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摘要

The addition of uridine nucleotide by the poly(U) polymerase (PUP) enzymes has a demonstrated impact on various classes of RNAs such as microRNAs (miRNAs), histone-encoding RNAs and messenger RNAs. Cid1 protein is a member of the PUP family. We solved the crystal structure of Cid1 in complex with non-hydrolyzable UMPNPP and a short dinucleotide compound ApU. These structures revealed new residues involved in substrate/product stabilization. In particular, one of the three catalytic aspartate residues explains the RNA dependence of its PUP activity. Moreover, other residues such as residue N165 or the beta-trapdoor are shown to be critical for Cid1 activity. We finally suggest that the length and sequence of Cid1 substrate RNA influence the balance between Cid1's processive and distributive activities. We propose that particular processes regulated by PUPs require the enzymes to switch between the two types of activity as shown for the miRNA biogenesis where PUPs can either promote DICER cleavage via short U-tail or trigger miRNA degradation by adding longer poly(U) tail. The enzymatic properties of these enzymes may be critical for determining their particular function in vivo.
机译:由聚(U)聚合酶(PUP)酶添加尿苷核苷酸对各种RNA的影响,例如MicroRNA(miRNA),组蛋白编码的RNA和信使RNA。 Cid1蛋白是幼崽家族的成员。我们解决了CID1的晶体结构与非水解uMPNPP和短二核苷酸化合物APU的复合物。这些结构揭示了底物/产物稳定的新残留物。特别地,三种催化天冬氨酸残基中的一种解释了其幼崽活性的RNA依赖性。此外,其他残留物如残留物N165或β-捕集器被证明对CID1活性至关重要。我们终于表明CID1衬底RNA的长度和序列影响了CID1的加工和分配活动之间的平衡。我们提出了幼崽调节的特定方法需要酶在两种类型的活性之间切换,如MiRNA生物发生,其中幼崽通过短U形尾或触发miRNA劣化通过添加更长的聚(U)尾部来促进Dicer切割。这些酶的酶促性质对于确定其体内的特定功能至关重要。

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  • 来源
    《Nucleic Acids Research》 |2014年第5期|共9页
  • 作者单位

    Department of Molecular Biology University of Geneva Geneva 1211 Switzerland;

    Department of Molecular Biology University of Geneva Geneva 1211 Switzerland;

    Department of Molecular Biology University of Geneva Geneva 1211 Switzerland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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