STRUCTURE DETERMINATION AND ANALYSIS OF HUMAN NEUTROPHIL COLLAGENASE COMPLEXED WITH A HYDROXAMATE INHIBITOR

被引:159
作者
GRAMS, F
CRIMMIN, M
HINNES, L
HUXLEY, P
PIEPER, M
TSCHESCHE, H
BODE, W
机构
[1] BRITISH BIOTECHNOL LTD,OXFORD OX4 5LY,ENGLAND
[2] MAX PLANCK INST BIOCHEM,STRUKT FORSCH ABT,D-82152 MARTINSRIED,GERMANY
[3] UNIV BIELEFELD,FAK CHEM & BIOCHEM,D-33501 BIELEFELD,GERMANY
关键词
D O I
10.1021/bi00043a007
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Matrix metalloproteinases are a family of zinc endopeptidases involved in tissue remodeling. They have been implicated in various disease processes including metastasis, joint destruction, and neurodegeneration, Human neutrophil collagenase (HNC, MMP-8) represents one of the three ''interstitial'' collagenases that cleave triple-helical collagens types I, II, and III. Its 163-residue catalytic domain (Met80 to Gly242) has been expressed in Escherichia coli and crystallized as a noncovalent complex with the hydroxamate inhibitor batimastat. The crystal structure, refined to 2.1 Angstrom, demonstrates that batimastat binds to the S1-S2' sites and coordinates to the catalytic zinc in a bidentate manner via the hydroxyl and carbonyl oxygens of the hydroxamate group. The batimastat-collagenase complex is described in detail, and the activities of batimastat analogues are discussed in the light of the protein-inhibitor interactions revealed by the crystallography studies,
引用
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页码:14012 / 14020
页数:9
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