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活性丝氨酸参与短杆菌肽S合成酶每个反应中心的共价底物氨基酸结合。

An active serine is involved in covalent substrate amino acid binding at each reaction center of gramicidin S synthetase.

作者信息

Schlumbohm W, Stein T, Ullrich C, Vater J, Krause M, Marahiel M A, Kruft V, Wittmann-Liebold B

机构信息

Institute of Biochemistry and Molecular Biology, Technical University of Berlin, Federal Republic of Germany.

出版信息

J Biol Chem. 1991 Dec 5;266(34):23135-41.

PMID:1744112
Abstract

The condensing peptide forming multienzyme of gramicidin S synthetase (gramicidin S synthetase 2) was specifically labeled at its putative thiotemplate sites for L-valine and L-leucine by covalent incorporation of the 14C-labeled substrate amino acids. The thioester complexes of the multienzyme were digested with CNBr, Staphylococcus aureus V8 protease, and pepsin. Reaction center peptides containing the [14C]valine and [14C]leucine labels were isolated in pure form. They show a high degree of sequence similarity and contain the same consensus sequence LGGH/DXL. The labels were eliminated in the first Edman degradation step. A dehydroalanine was identified which can originate from either a cysteine or a serine. The comparison of the chemical results with the deduced amino acid sequence of the grsB gene encoding the gramicidin S synthetase 2 revealed that 4 such motifs are located within the gene structure, each of them being localized in the 3'-terminal region of one of 4 gene segments grsB1-B4. They have a size of approximately 2 kilobases and presumably code for the 4 amino acid activating domains of the synthetase. Surprisingly a serine was found at each putative substrate amino acid-binding position instead of a cysteine as postulated by the thiotemplate mechanism. Therefore the data suggest that active serine residues are involved in nonribosomal peptide syntheses of microbial peptides.

摘要

短杆菌肽S合成酶(短杆菌肽S合成酶2)的缩合肽形成多酶在其假定的L-缬氨酸和L-亮氨酸硫酯模板位点通过共价掺入14C标记的底物氨基酸进行特异性标记。用溴化氰、金黄色葡萄球菌V8蛋白酶和胃蛋白酶消化该多酶的硫酯复合物。以纯形式分离出含有[14C]缬氨酸和[14C]亮氨酸标记的反应中心肽。它们显示出高度的序列相似性,并包含相同的共有序列LGGH/DXL。这些标记在第一个埃德曼降解步骤中被去除。鉴定出一种脱氢丙氨酸,其可能源自半胱氨酸或丝氨酸。将化学结果与编码短杆菌肽S合成酶2的grsB基因推导的氨基酸序列进行比较,结果表明在基因结构中有4个这样的基序,每个基序位于4个基因片段grsB1-B4之一的3'末端区域。它们的大小约为2千碱基,可能编码合成酶的4个氨基酸活化结构域。令人惊讶的是,在每个假定的底物氨基酸结合位置发现的是丝氨酸而不是硫酯模板机制所假定的半胱氨酸。因此,数据表明活性丝氨酸残基参与微生物肽的非核糖体肽合成。

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1
An active serine is involved in covalent substrate amino acid binding at each reaction center of gramicidin S synthetase.活性丝氨酸参与短杆菌肽S合成酶每个反应中心的共价底物氨基酸结合。
J Biol Chem. 1991 Dec 5;266(34):23135-41.
2
Detection of 4'-phosphopantetheine at the thioester binding site for L-valine of gramicidinS synthetase 2.在短杆菌肽S合成酶2的L-缬氨酸硫酯结合位点检测4'-磷酸泛酰巯基乙胺。
FEBS Lett. 1994 Feb 28;340(1-2):39-44. doi: 10.1016/0014-5793(94)80169-x.
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Characterization of the binding site of the tripeptide intermediate D-Phenylalanyl L-prolyl-L-valine in gramicidin S biosynthesis.短杆菌肽S生物合成中三肽中间体D-苯丙氨酰-L-脯氨酰-L-缬氨酸结合位点的表征
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The multiple carrier model of nonribosomal peptide biosynthesis at modular multienzymatic templates.模块化多酶模板上非核糖体肽生物合成的多载体模型。
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The fidelity of gramicidin S synthetase.短杆菌肽S合成酶的保真度。
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(3,3'-Leu)-gramicidin S formation by gramicidin S synthetase.短杆菌肽S合成酶催化形成(3,3'-亮氨酸)-短杆菌肽S
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Three conserved glycine residues in valine activation of gramicidin S synthetase 2 from Bacillus brevis.来自短短芽孢杆菌的短杆菌肽S合成酶2缬氨酸激活中的三个保守甘氨酸残基。
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Acta Microbiol Acad Sci Hung. 1975;22(4):419-25.
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Gramicidin S synthetase. Stability of reactive thioester intermediates and formation of 3-amino-2-piperidone.短杆菌肽S合成酶。活性硫酯中间体的稳定性及3-氨基-2-哌啶酮的形成。
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Proteinchemical and kinetic features of gramicidin S synthetase.
Biol Chem Hoppe Seyler. 1989 Sep;370(9):1013-8. doi: 10.1515/bchm3.1989.370.2.1013.

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