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J. Biol. Chem., Vol. 266, Issue 9, 5625-5628, Mar, 1991
JJ Wu, MW Lark, LE Chun and DR Eyre
Human recombinant stromelysin-1 was shown to cleave four types of collagen
(types II, IX, X, and XI) prepared from bovine and rat cartilages at
specific sites. Stromelysin-1 cleaved salt-soluble native molecules of type
IX collagen into two main triple-helical fragments, COL1 and COL2,3.
Protein microsequencing identified the exact cleavage sites in the NC2
domain of all three chains, alpha 1(IX), alpha 2(IX), and alpha 3(IX).
Stromelysin-1 also acted as a "telopeptidase," in that it efficiently
clipped intact molecules of types II and XI collagens at sites just inside
their terminal cross-linking hydroxylysine residues. Native molecules of
type X collagen were cleaved by stromelysin-1 within their triple helical
domains at a COOH-terminal site that reduced the alpha 1(X) chain size by
10 kDa. These findings suggest an important role for stromelysin in the
turnover and remodeling of the collagenous matrix of cartilage both
normally and in degenerative joint disease.
Sites of stromelysin cleavage in collagen types II, IX, X, and XI of cartilage
Department of Orthopaedics, University of Washington, Seattle 98195.
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