Carboxyl proteinase from Pseudomonas defines a novel family of subtilisin-like enzymes

被引:0
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作者
Alexander Wlodawer
Mi Li
Zbigniew Dauter
Alla Gustchina
Kenichi Uchida
Hiroshi Oyama
Ben M. Dunn
Kohei Oda
机构
[1] Protein Structure Section,Department of Biosciences
[2] Macromolecular Crystallography Laboratory,Department of Applied Biology
[3] National Cancer Institute at Frederick,Department of Biochemistry and Molecular Biology
[4] Intramural Research Support Program,undefined
[5] SAIC Frederick,undefined
[6] National Cancer Institute at Frederick,undefined
[7] Synchrotron Radiation Research Section,undefined
[8] Macromolecular Crystallography Laboratory,undefined
[9] National Cancer Institute and NSLS,undefined
[10] Brookhaven National Laboratory,undefined
[11] School of Science and Engineering,undefined
[12] Teikyo University,undefined
[13] Faculty of Textile Science,undefined
[14] Kyoto Institute of Technology,undefined
[15] University of Florida,undefined
来源
Nature Structural Biology | 2001年 / 8卷
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摘要
The crystal structure of a pepstatin-insensitive carboxyl proteinase from Pseudomonas sp. 101 (PSCP) has been solved by single-wavelength anomalous diffraction using the absorption peak of bromide anions. Structures of the uninhibited enzyme and of complexes with an inhibitor that was either covalently or noncovalently bound were refined at 1.0–1.4 Å resolution. The structure of PSCP comprises a single compact domain with a diameter of ∼55 Å, consisting of a seven-stranded parallel β-sheet flanked on both sides by a number of helices. The fold of PSCP is a superset of the subtilisin fold, and the covalently bound inhibitor is linked to the enzyme through a serine residue. Thus, the structure of PSCP defines a novel family of serine-carboxyl proteinases (defined as MEROPS S53) with a unique catalytic triad consisting of Glu 80, Asp 84 and Ser 287.
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页码:442 / 446
页数:4
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