Abstract

A proteoglycan consists of a core portein to which one or more glycosaminoglycans are covalently attached. In cartilage, proteoglycans are large, complex components of the extracellular matrix where they are found primarily organized into aggregates. It has been known for some time that proteoglycans isolated form immature and adult cartilages differ with respect to the size and composition of their glycosaminoglycan and protein moieties. More recent studies have brought forth evidence that there are different species of proteoglycans in cartilage. The purpose of this research is to re-evaluate the biochemical basis of the age-related diferences in light of this new evidence. More specifically, we intend to establish whether the age-related differences reflect differences in the composition of one or more of the proteoglycan species or whether they reflect differences in the relative proportions of the different species present at any one age. At first, we will restrict ourselves to the study of aggregating proteoglycans because the great majority (Greater than 80%) of articular cartilage proteoglycans are of the aggregating type and because it is difficult to rule out the possibility that some of the non-aggregating proteoglycans represent degradation products of the aggregates. Aggregating proteoglycans will be purified from the articular cartilage of immature calves (1-2 month old) or older steers (About 18 months old) and they will subjected to a number of prepartive procedures and analytical assays to characterize quantitatively and qualitatively each of the aggregating species at the two ages studied. We have obtained preliminary evidence that suggests that in steer articular cartilage there are two major species of aggregating proteoglycans whereas in the calf only one is apparent. In addition to studying the proteoglycans as they exists in the parent cartilages, we intend to examine the nature of the age-related differences at the level of biosynthesis. For this purpose, we will use a recently developed chondrocyte culture system in which calf and steer chondrocytes grown as monolayers continue to synthesize """"""""calf-like"""""""" and """"""""steer-like"""""""" proteoglycans for as long as three weeks following plating. We will use the system to ascertain that proteoglycan heterogeniety (i.e. more than one species) is not the result of partial degradation of a single proteoglycan species but rather than proteoglycans are synthesized as multiple species. The ability to manufacture typical immature-like or adult-like proteoglycans in vitro will be used to study the age-related differences at the level of biosynthesis and to examine whether heterogeneity can be detected prior to the addition of the glycosaminoglycans to the core protein(s) in the Golgi apparatus.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG004736-03
Application #
3115300
Study Section
Pathobiochemistry Study Section (PBC)
Project Start
1984-04-01
Project End
1987-03-31
Budget Start
1986-04-01
Budget End
1987-03-31
Support Year
3
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Rush University Medical Center
Department
Type
DUNS #
City
Chicago
State
IL
Country
United States
Zip Code
60612

  Publications

Chiba, Kazuhiro; Masuda, Koichi; Andersson, Gunnar B J et al. (2007) Matrix replenishment by intervertebral disc cells after chemonucleolysis in vitro with chondroitinase ABC and chymopapain. Spine J 7:694-700
Masuda, K; Pfister, B E; Sah, R L et al. (2006) Osteogenic protein-1 promotes the formation of tissue-engineered cartilage using the alginate-recovered-chondrocyte method. Osteoarthritis Cartilage 14:384-91
Minihane, Keith P; Turner, Thomas M; Urban, Robert M et al. (2005) Effect of hip hemiarthroplasty on articular cartilage and bone in a canine model. Clin Orthop Relat Res :157-63
An, Howard S; Takegami, Kenji; Kamada, Hiroshi et al. (2005) Intradiscal administration of osteogenic protein-1 increases intervertebral disc height and proteoglycan content in the nucleus pulposus in normal adolescent rabbits. Spine (Phila Pa 1976) 30:25-31; discussion 31-2
Chia, Stanley H; Homicz, Mark R; Schumacher, Barbara L et al. (2005) Characterization of human nasal septal chondrocytes cultured in alginate. J Am Coll Surg 200:691-704
Masuda, Koichi; Aota, Yoichi; Muehleman, Carol et al. (2005) A novel rabbit model of mild, reproducible disc degeneration by an anulus needle puncture: correlation between the degree of disc injury and radiological and histological appearances of disc degeneration. Spine (Phila Pa 1976) 30:5-14
Takegami, Kenji; An, Howard S; Kumano, Fumio et al. (2005) Osteogenic protein-1 is most effective in stimulating nucleus pulposus and annulus fibrosus cells to repair their matrix after chondroitinase ABC-induced in vitro chemonucleolysis. Spine J 5:231-8
Chia, Stanley H; Schumacher, Barbara L; Klein, Travis J et al. (2004) Tissue-engineered human nasal septal cartilage using the alginate-recovered-chondrocyte method. Laryngoscope 114:38-45
Masuda, Koichi; Sah, Robert L; Hejna, Michael J et al. (2003) A novel two-step method for the formation of tissue-engineered cartilage by mature bovine chondrocytes: the alginate-recovered-chondrocyte (ARC) method. J Orthop Res 21:139-48
Williams, James M; Rayan, Vineeta; Sumner, D Rick et al. (2003) The use of intra-articular Na-hyaluronate as a potential chondroprotective device in experimentally induced acute articular cartilage injury and repair in rabbits. J Orthop Res 21:305-11

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