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表面活性素合成酶激活酶sfp的晶体结构:4'-磷酸泛酰巯基乙胺基转移酶超家族的一个原型

Crystal structure of the surfactin synthetase-activating enzyme sfp: a prototype of the 4'-phosphopantetheinyl transferase superfamily.

作者信息

Reuter K, Mofid M R, Marahiel M A, Ficner R

机构信息

Institut für Molekularbiologie und Tumorforschung, Philipps-Universität Marburg, Emil-Mannkopff-Strasse 2, D-35037 Marburg.

出版信息

EMBO J. 1999 Dec 1;18(23):6823-31. doi: 10.1093/emboj/18.23.6823.

Abstract

The Bacillus subtilis Sfp protein activates the peptidyl carrier protein (PCP) domains of surfactin synthetase by transferring the 4'-phosphopantetheinyl moiety of coenzyme A (CoA) to a serine residue conserved in all PCPs. Its wide PCP substrate spectrum renders Sfp a biotechnologically valuable enzyme for use in combinatorial non-ribosomal peptide synthesis. The structure of the Sfp-CoA complex determined at 1.8 A resolution reveals a novel alpha/beta-fold exhibiting an unexpected intramolecular 2-fold pseudosymmetry. This suggests a similar fold and dimerization mode for the homodimeric phosphopantetheinyl transferases such as acyl carrier protein synthase. The active site of Sfp accommodates a magnesium ion, which is complexed by the CoA pyrophosphate, the side chains of three acidic amino acids and one water molecule. CoA is bound in a fashion that differs in many aspects from all known CoA-protein complex structures. The structure reveals regions likely to be involved in the interaction with the PCP substrate.

摘要

枯草芽孢杆菌Sfp蛋白通过将辅酶A(CoA)的4'-磷酸泛酰巯基乙胺部分转移至所有肽基载体蛋白(PCP)中保守的丝氨酸残基上,从而激活表面活性素合成酶的PCP结构域。其广泛的PCP底物谱使Sfp成为组合非核糖体肽合成中具有生物技术价值的一种酶。以1.8 Å分辨率测定的Sfp-CoA复合物结构揭示了一种新型的α/β折叠,呈现出意想不到的分子内2倍假对称性。这表明同源二聚体磷酸泛酰巯基乙胺转移酶(如酰基载体蛋白合成酶)具有相似的折叠和二聚化模式。Sfp的活性位点容纳一个镁离子,该镁离子与CoA焦磷酸、三个酸性氨基酸的侧链和一个水分子络合。CoA的结合方式在许多方面与所有已知的CoA-蛋白质复合物结构不同。该结构揭示了可能参与与PCP底物相互作用的区域。

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