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Collagen fibril architecture, domain organization, and triple-helical conformation govern its proteolysis

Journal Article · · Proc. Natl. Acad. Sci. USA
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We describe the molecular structure of the collagen fibril and how it affects collagen proteolysis or 'collagenolysis.' The fibril-forming collagens are major components of all mammalian connective tissues, providing the structural and organizational framework for skin, blood vessels, bone, tendon, and other tissues. The triple helix of the collagen molecule is resistant to most proteinases, and the matrix metalloproteinases that do proteolyze collagen are affected by the architecture of collagen fibrils, which are notably more resistant to collagenolysis than lone collagen monomers. Until now, there has been no molecular explanation for this. Full or limited proteolysis of the collagen fibril is known to be a key process in normal growth, development, repair, and cell differentiation, and in cancerous tumor progression and heart disease. Peptide fragments generated by collagenolysis, and the conformation of exposed sites on the fibril as a result of limited proteolysis, regulate these processes and that of cellular attachment, but it is not known how or why. Using computational and molecular visualization methods, we found that the arrangement of collagen monomers in the fibril (its architecture) protects areas vulnerable to collagenolysis and strictly governs the process. This in turn affects the accessibility of a cell interaction site located near the cleavage region. Our observations suggest that the C-terminal telopeptide must be proteolyzed before collagenase can gain access to the cleavage site. Collagenase then binds to the substrate's 'interaction domain,' which facilitates the triple-helix unwinding/dissociation function of the enzyme before collagenolysis.

Research Organization:
Advanced Photon Source (APS), Argonne National Laboratory (ANL), Argonne, IL (US)
Sponsoring Organization:
USDOE
OSTI ID:
1006641
Journal Information:
Proc. Natl. Acad. Sci. USA, Journal Name: Proc. Natl. Acad. Sci. USA Journal Issue: (8) ; 02, 2008 Vol. 105; ISSN PNASA6; ISSN 0027-8424
Country of Publication:
United States
Language:
ENGLISH

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Related Subjects

60 APPLIED LIFE SCIENCES
BLOOD VESSELS
CARDIOVASCULAR DISEASES
CELL DIFFERENTIATION
CLEAVAGE
COLLAGEN
CONNECTIVE TISSUE
ENZYMES
FUNCTIONS
GAIN
GROWTH
INTERACTIONS
MOLECULAR STRUCTURE
MOLECULES
MONOMERS
NEOPLASMS
PEPTIDES
PROTEOLYSIS
REPAIR
SKIN