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链霉菌K15青霉素结合蛋白/DD-肽酶的氨基酸序列。A类低分子量青霉素结合蛋白的预测二级结构。

Amino acid sequence of the penicillin-binding protein/DD-peptidase of Streptomyces K15. Predicted secondary structures of the low Mr penicillin-binding proteins of class A.

作者信息

Palomeque-Messia P, Englebert S, Leyh-Bouille M, Nguyen-Distèche M, Duez C, Houba S, Dideberg O, Van Beeumen J, Ghuysen J M

机构信息

Centre d'Ingénierie des Protéines, Université de Liège, Belgium.

出版信息

Biochem J. 1991 Oct 1;279 ( Pt 1)(Pt 1):223-30. doi: 10.1042/bj2790223.

Abstract

The low-Mr penicillin-binding protein (PBP)/DD-transpeptidase of Streptomyces K15 is synthesized in the form of a 291-amino acid-residue precursor possessing a cleavable 29-amino acid-residue signal peptide. Sequence-similarity searches and hydrophobic-cluster analysis show that the Streptomyces K15 enzyme, the Escherichia coli PBPs/DD-carboxy-peptidases 5 and 6, the Bacillus subtilis PBP/DD-carboxypeptidase 5 and the spoIIA product (a putative PBP involved in the sporulation of B. subtilis) are structurally related and form a distinct class A of low-Mr PBPs/DD-peptidases. The distribution of the hydrophobic clusters along the amino acid sequences also shows that the Streptomyces K15 PBP, and by extension the other PBPs of class A, have similarity in the polypeptide folding, with the beta-lactamases of class A, with as reference the Streptomyces albus G and Staphylococcus aureus beta-lactamases of known three-dimensional structure. This comparison allows one to predict most of the secondary structures in the PBPs and the amino acid motifs that define the enzyme active sites.

摘要

链霉菌K15的低分子量青霉素结合蛋白(PBP)/DD-转肽酶以291个氨基酸残基前体的形式合成,该前体具有一个可裂解的29个氨基酸残基的信号肽。序列相似性搜索和疏水簇分析表明,链霉菌K15酶、大肠杆菌PBPs/DD-羧肽酶5和6、枯草芽孢杆菌PBP/DD-羧肽酶5以及spoIIA产物(一种参与枯草芽孢杆菌芽孢形成的推定PBP)在结构上相关,形成了一个独特的低分子量PBPs/DD-肽酶A类。疏水簇沿氨基酸序列的分布还表明,链霉菌K15 PBP,进而A类的其他PBPs,在多肽折叠方面与A类β-内酰胺酶相似,以已知三维结构的白色链霉菌G和金黄色葡萄球菌β-内酰胺酶作为参考。这种比较使人们能够预测PBPs中的大多数二级结构以及定义酶活性位点的氨基酸基序。

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