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Upper zone of growth plate and cartilage matrix associated protein protects cartilage during inflammatory arthritis
by
Baum, Wolfgang
, Schett, Georg
, Seuffert, Fritz
, Stock, Michael
, Weidner, Daniela
in
ADAMTS
/ ADAMTS5 Protein - genetics
/ ADAMTS5 Protein - metabolism
/ Aggrecanase
/ Aggrecans - metabolism
/ Animals
/ Arthritis
/ Cartilage
/ Cartilage degeneration
/ Cartilage, Articular - metabolism
/ Cell Line
/ Chondrocytes - metabolism
/ Complications and side effects
/ Degeneration (Pathology)
/ Development and progression
/ Health aspects
/ HEK293 Cells
/ Humans
/ Medicine
/ Medicine & Public Health
/ Mice, Inbred C57BL
/ Mice, Knockout
/ Orthopedics
/ Osteoarthritis - genetics
/ Osteoarthritis - metabolism
/ Osteophyte formation
/ Physiological aspects
/ Prevention
/ Protein Binding
/ Protein-protein interactions
/ Proteins - genetics
/ Proteins - metabolism
/ Proteoglycans - metabolism
/ Research Article
/ Rheumatology
/ Risk factors
/ Signaling peptides and proteins
2018
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Upper zone of growth plate and cartilage matrix associated protein protects cartilage during inflammatory arthritis
by
Baum, Wolfgang
, Schett, Georg
, Seuffert, Fritz
, Stock, Michael
, Weidner, Daniela
in
ADAMTS
/ ADAMTS5 Protein - genetics
/ ADAMTS5 Protein - metabolism
/ Aggrecanase
/ Aggrecans - metabolism
/ Animals
/ Arthritis
/ Cartilage
/ Cartilage degeneration
/ Cartilage, Articular - metabolism
/ Cell Line
/ Chondrocytes - metabolism
/ Complications and side effects
/ Degeneration (Pathology)
/ Development and progression
/ Health aspects
/ HEK293 Cells
/ Humans
/ Medicine
/ Medicine & Public Health
/ Mice, Inbred C57BL
/ Mice, Knockout
/ Orthopedics
/ Osteoarthritis - genetics
/ Osteoarthritis - metabolism
/ Osteophyte formation
/ Physiological aspects
/ Prevention
/ Protein Binding
/ Protein-protein interactions
/ Proteins - genetics
/ Proteins - metabolism
/ Proteoglycans - metabolism
/ Research Article
/ Rheumatology
/ Risk factors
/ Signaling peptides and proteins
2018
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Upper zone of growth plate and cartilage matrix associated protein protects cartilage during inflammatory arthritis
by
Baum, Wolfgang
, Schett, Georg
, Seuffert, Fritz
, Stock, Michael
, Weidner, Daniela
in
ADAMTS
/ ADAMTS5 Protein - genetics
/ ADAMTS5 Protein - metabolism
/ Aggrecanase
/ Aggrecans - metabolism
/ Animals
/ Arthritis
/ Cartilage
/ Cartilage degeneration
/ Cartilage, Articular - metabolism
/ Cell Line
/ Chondrocytes - metabolism
/ Complications and side effects
/ Degeneration (Pathology)
/ Development and progression
/ Health aspects
/ HEK293 Cells
/ Humans
/ Medicine
/ Medicine & Public Health
/ Mice, Inbred C57BL
/ Mice, Knockout
/ Orthopedics
/ Osteoarthritis - genetics
/ Osteoarthritis - metabolism
/ Osteophyte formation
/ Physiological aspects
/ Prevention
/ Protein Binding
/ Protein-protein interactions
/ Proteins - genetics
/ Proteins - metabolism
/ Proteoglycans - metabolism
/ Research Article
/ Rheumatology
/ Risk factors
/ Signaling peptides and proteins
2018
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Upper zone of growth plate and cartilage matrix associated protein protects cartilage during inflammatory arthritis
Journal Article
Upper zone of growth plate and cartilage matrix associated protein protects cartilage during inflammatory arthritis
2018
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Overview
Background
ADAMTS aggrecanases play a major role in cartilage degeneration during degenerative and inflammatory arthritis. The cartilage-specific secreted protein Upper zone of growth plate and cartilage matrix associated protein (Ucma) has been shown to block ADAMTS-triggered aggrecanolysis in experimental osteoarthritis. Here we aimed to investigate whether and how Ucma may affect cartilage destruction and osteophyte formation in the context of inflammatory arthritis.
Methods
Ucma–ADAMTS5 protein interactions were studied using slot blot and solid phase binding assays. Chondrocyte cultures were stimulated with ADAMTS5 or IL-1β in the presence or absence of Ucma and aggrecanolysis was assessed by neoepitope formation. Arthritis was induced by transfer of K/BxN serum into wild-type (WT), Ucma-deficient and WT mice treated with recombinant Ucma. Cartilage proteoglycan loss and cartilage damage was assessed by safranin-O stain, aggrecanase-induced neoepitope formation and histomorphometry, respectively. Osteophytes were assessed by histomorphometry, micro-computed tomography, RNA in-situ hybridisation for
collagen10a1
and
osteocalcin
, and staining for TRAP activity. Gene expression analyses were performed using real-time RT-PCR.
Results
Ucma physically interacted with ADAMTS5 and blocked its aggrecanase activity in chondrocyte cultures. Ucma was highly expressed in the articular cartilage and in osteophytes during arthritis. Ucma had no effect on inflammation and bone erosion. In contrast, Ucma-deficient mice developed significantly more severe cartilage proteoglycan loss and cartilage destruction. Conversely, treatment with Ucma inhibited cartilage degeneration in arthritis. Ucma effectively inhibited ADAMTS5-triggered or IL-1β-triggered aggrecanolysis in vitro and in vivo. Furthermore, osteophyte formation was reduced in Ucma-deficient mice.
Conclusions
These results indicate that Ucma inhibits aggrecanolysis by physical interaction with ADAMTS5 and protects from cartilage degeneration in inflammatory arthritis. Ucma therefore represents an interesting novel and specific target for preventing cartilage degradation in the context of inflammatory arthritis.
Publisher
BioMed Central,BioMed Central Ltd,BMC
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