Abstract

Connective tissues comprise a diverse group of tissues, including tendon, cartilage, bone, skin, and vitreous which require specific mechanical and structural properties appropriate to their function. These tissues all have collagen fibrils as a major structure component, and their required tissue specific properties depend on the molecular and supramolecular organization of collagen together with other molecules in the extracellular matrix. Our laboratory has embarked on a program to characterize the structural differences in a range of connective tissues with different genetic types and different non-collagenous components, at the level of molecular and fibril organization. Tissue specific variations in collagen structure will be related to the interactions which stabilize these aggregates. The molecular packing and molecular interactions will be characterized for D-periodic fibrils formed by different genetic types of collagens. Fibrils of types I, II and III collagens differ in molecular density, and the mediation of such density differences by water interactions, sequence differences and carbohydrate content will be examined. The minor collagens type V and 1 alpha, 2 alpha, 3 alpha can form fibrils which appear to be of very uniform small diameter and to have an axial D period. The fibril structures, fibril forming process, and structural effects of terminal peptides found in intact tissue forms will be characterized for these minor collagens. The organization of fibrils in tissues and the effects of proteoglycan on collagen organization will be examined for type II collagen in notochord. The small uniform type II fibrils in lamprey notochord have a large center to center distance, equal to almost twice the fibril diameter. The forces stabilizing this array of fibrils will be investigated, to determine if they involve an equilibrium state, e.g. repulsion of surface charges on fibrils, or more rigid structures, e.g. covalent cross-linking or a coating of the fibril surface. The role of proteoglycan in collagen structure will be examined by determining the effect of proteoglycan removal on collagen molecular packing, fibril diameter, and interfibrillar distance, and on the charge and water interactions between collagen fibrils.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
2R01AR019626-09A1
Application #
3155062
Study Section
Pathobiochemistry Study Section (PBC)
Project Start
1977-03-01
Project End
1990-11-30
Budget Start
1986-12-01
Budget End
1987-11-30
Support Year
9
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Type
Schools of Medicine
DUNS #
622146454
City
Piscataway
State
NJ
Country
United States
Zip Code
08854

  Publications

Kramer, R Z; Bella, J; Brodsky, B et al. (2001) The crystal and molecular structure of a collagen-like peptide with a biologically relevant sequence. J Mol Biol 311:131-47
Kramer, R Z; Venugopal, M G; Bella, J et al. (2000) Staggered molecular packing in crystals of a collagen-like peptide with a single charged pair. J Mol Biol 301:1191-205
Ackerman, M S; Bhate, M; Shenoy, N et al. (1999) Sequence dependence of the folding of collagen-like peptides. Single amino acids affect the rate of triple-helix nucleation. J Biol Chem 274:7668-73
Shah, N K; Brodsky, B; Kirkpatrick, A et al. (1999) Structural consequences of D-amino acids in collagen triple-helical peptides. Biopolymers 49:297-302
Baum, J; Brodsky, B (1999) Folding of peptide models of collagen and misfolding in disease. Curr Opin Struct Biol 9:122-8
Beck, K; Brodsky, B (1998) Supercoiled protein motifs: the collagen triple-helix and the alpha-helical coiled coil. J Struct Biol 122:17-29
Kramer, R Z; Vitagliano, L; Bella, J et al. (1998) X-ray crystallographic determination of a collagen-like peptide with the repeating sequence (Pro-Pro-Gly). J Mol Biol 280:623-38
Liu, X; Kim, S; Dai, Q H et al. (1998) Nuclear magnetic resonance shows asymmetric loss of triple helix in peptides modeling a collagen mutation in brittle bone disease. Biochemistry 37:15528-33
Ramshaw, J A; Shah, N K; Brodsky, B (1998) Gly-X-Y tripeptide frequencies in collagen: a context for host-guest triple-helical peptides. J Struct Biol 122:86-91
Yang, W; Battineni, M L; Brodsky, B (1997) Amino acid sequence environment modulates the disruption by osteogenesis imperfecta glycine substitutions in collagen-like peptides. Biochemistry 36:6930-5

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