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人核苷二磷酸激酶B与GDP复合物在2埃分辨率下的X射线结构。

X-ray structure of human nucleoside diphosphate kinase B complexed with GDP at 2 A resolution.

作者信息

Moréra S, Lacombe M L, Xu Y, LeBras G, Janin J

机构信息

Laboratoire de Biologie Structurale, UMR 9920 CNRS-Université Paris-Sud, Gif-sur-Yvette, France.

出版信息

Structure. 1995 Dec 15;3(12):1307-14. doi: 10.1016/s0969-2126(01)00268-4.

Abstract

BACKGROUND

Nucleoside diphosphate (NDP) kinases provide precursors for DNA and RNA synthesis. In mammals, these enzymes are also involved in cell regulations. Human NDP kinase B, product of the human nm23-H2 gene, is both an enzyme and a transcription factor. It activates transcription of the c-myc oncogene independently of its catalytic function, by binding to its promoter DNA. How do the two functions coexist?

RESULTS

Recombinant human NDP kinase B was co-crystallized with GDP. The X-ray structure was solved at 2.0 A resolution by molecular replacement from the homologous Drosophila Awd protein. Both enzymes are homo-hexamers with a characteristic beta alpha beta beta alpha beta fold. GDP binds near the active site His118. The guanine base is in a surface cleft and interacts with the C terminus of another subunit.

CONCLUSIONS

The beta alpha beta beta alpha beta fold, also present in the 'palm' domain of Escherichia coli DNA polymerase I and HIV reverse transcriptase, is both a mononucleotide- and a polynucleotide-binding fold. If NDP kinase B binds DNA in the same way as the polymerases, the enzyme must undergo a conformation change in order to carry out gene activation.

摘要

背景

核苷二磷酸(NDP)激酶为DNA和RNA合成提供前体。在哺乳动物中,这些酶也参与细胞调节。人类NDP激酶B是人类nm23 - H2基因的产物,既是一种酶又是一种转录因子。它通过与c - myc癌基因的启动子DNA结合,独立于其催化功能激活该基因的转录。这两种功能是如何共存的呢?

结果

重组人NDP激酶B与GDP共结晶。通过同源果蝇Awd蛋白的分子置换,以2.0埃的分辨率解析了X射线结构。两种酶均为具有特征性β-α-β-β-α-β折叠的同型六聚体。GDP结合在活性位点His118附近。鸟嘌呤碱基位于表面裂隙中,并与另一个亚基的C末端相互作用。

结论

β-α-β-β-α-β折叠也存在于大肠杆菌DNA聚合酶I和HIV逆转录酶的“手掌”结构域中,是一种单核苷酸和多核苷酸结合折叠。如果NDP激酶B以与聚合酶相同的方式结合DNA,那么该酶必须经历构象变化才能进行基因激活。

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