MATRIX METALLOPROTEINASE-3 (STROMELYSIN-1) - IDENTIFICATION AS THE CARTILAGE ACID METALLOPROTEASE AND EFFECT OF PH ON CATALYTIC PROPERTIES AND CALCIUM AFFINITY

被引:0
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作者
WILHELM, SM [1 ]
SHAO, ZH [1 ]
HOUSLEY, TJ [1 ]
SEPERACK, PK [1 ]
BAUMANN, AP [1 ]
GUNJASMITH, Z [1 ]
WOESSNER, JF [1 ]
机构
[1] UNIV MIAMI,SCH MED,DEPT MED,MIAMI,FL 33101
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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
Human pro-MMP-3 (pro-matrix metalloproteinase-3) was purified from three sources: articular cartilage and conditioned media from synovial fibroblasts and Chinese hamster ovary cells expressing recombinant pro-MMP-3. All three preparations reacted with two monoclonal antibodies specific for human fibroblast pro-MMP-3. Each preparation of active MMP-3 possessed properties identical to those previously reported for the cartilage acid metalloproteinase (MMP-6; Azzo and Woessner, J. F., Jr. (1986) J. Biol. Chem. 261, 5434-5441): an acid pH optimum of 5.3-5.5 for digestion of cartilage aggrecan; digestion of oxidized insulin B-chain at Ala14-Leu15 and Tyr16-Leu17 in a ratio of 3:1; and heat stability at neutral pH. Further characterization of MMP-3 establishes that the acid pH optimum for cartilage aggrecan is not due to substrate denaturation since the same optimum is found by viscosity assay, by SDS-polyacrylamide gel electrophoresis assay of G1 domain, and by digestion of aggrecan in fresh cartilage fragments in vitro. Fibronectin was also digested optimally at pH 5.5 and NH2-terminal sequence analysis revealed no pH change in a major proteolytic site of cleavage at the Pro689-Leu690 bond. The specificity constant k(cat)/K(m) is maximal at pH 5.5 as determined in a quenched fluorescence peptide assay. This is due to an increase in k(cat) at pH 5.5 without any substantial effect on K(m). The affinity of MMP-3 for calcium is decreased about 10-fold at pH 5.3 compared to neutral pH. Finally, the neutral cartilage metalloproteinase is identified as 72-kDa pro-MMP-2 based on M(r), specificity of insulin B-chain cleavage, and reactivity with a specific polyconal antibody to human MMP-2.
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页码:21906 / 21913
页数:8
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