Differential mechanisms of inorganic pyrophosphate production by plasma cell membrane glycoprotein-1 and B10 in chondrocytes

Johnson, Kristen; Vaingankar, Sucheta M.; Chen, Ying; Moffa, Allison; Goldring, Mary B.; Sano, Kimihiko; Piao, Jinhua; Sali, Adnan; Goding, James W.; Terkeltaub, Robert

doi:10.1002/1529-0131(199909)42:9<1986::aid-anr26>3.0.co;2-o

Cited by 123 publications

(192 citation statements)

References 49 publications

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“…To maintain joint health and integrity, cartilage calcification needs to be tightly controlled and restricted to specific regions. Chondrocytes, the resident cell type in cartilage, release ATP constitutively [70], display high levels of NPP1 activity and can produce large amounts of extracellular pyrophosphate [71,72]. In the degenerative joint disease osteoarthritis (OA), aberrant articular cartilage calcification may occur and damage the surrounding tissue [73].…”

Section: Pyrophosphate and Cartilage Mineralisationmentioning

confidence: 99%

Pyrophosphate: a key inhibitor of mineralisation

Orriss

Arnett

Russell

2016

Current Opinion in Pharmacology

130

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Section: Pyrophosphate and Cartilage Mineralisationmentioning

confidence: 99%

Pyrophosphate: a key inhibitor of mineralisation

Orriss

Arnett

Russell

2016

Current Opinion in Pharmacology

130

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“…The enzyme-inactive mutant of TNAP does not upregulate NTPPH, indicating that ePi production is required. Conversely, NPP1 overexpression in articular chondrocytes does not influence TNAP expression (48). These data suggest that TNAP activity may regulate ePPi production, but not vice versa.…”

Section: Dysregulated Eppi/epi Production In Pathologymentioning

confidence: 70%

“…CILP/NTPPH expression is 6-fold and 3-fold higher in OA with and without CPPD crystals, respectively, than it is in normal articular chondrocytes (116). However, mRNA levels for NPP1 and NPP3 are not significantly higher in OA than in normal cartilage (48). In contrast, OA enhances NPP1 and CILP/NTPPH expression in human knee menisci (36).…”

Section: Dysregulated Eppi/epi Production In Pathologymentioning

confidence: 88%

“…Articular chondrocytes constitutively elaborate large amounts of ePPi (48,49) and possess the highest known NTPPH activity (50). Several tissues that synthesize collagenous extracellular matrices express NPP1, NPP2␣, and NPP3 (36,41,48,51).…”

Section: Regulation Of Eppi/epi Balance In Articular Cartilage By Ectmentioning

confidence: 99%

“…Several tissues that synthesize collagenous extracellular matrices express NPP1, NPP2␣, and NPP3 (36,41,48,51). All 3 ectoenzymes have been immunolocalized in human knee menisci (36), whereas human articular chondrocytes transcribe mRNA for NPP1 and NPP3 (48). NPP1 is located in the plasma membrane and MVs, while NPP3 is restricted to the pre-Golgi (48) (Figure 4).…”

Section: Regulation Of Eppi/epi Balance In Articular Cartilage By Ectmentioning

confidence: 99%

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Extracellular nucleotide metabolism and signaling in the pathophysiology of articular cartilage

Picher¹,

Graff²,

Lee³

2003

Arthritis & Rheumatism

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Mitochondrial oxidative phosphorylation is a downstream regulator of nitric oxide effects on chondrocyte matrix synthesis and mineralization

Johnson

Jung

Murphy³

et al. 2000

Arthritis & Rheumatism

Self Cite

177

105

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Objective. Increased chondrocyte nitric oxide (NO) and peroxynitrite production appears to modulate decreased matrix synthesis and increased mineralization in osteoarthritis (OA). Because NO inhibits mitochondrial respiration, this study was undertaken to directly assess the potential role of chondrocyte mitochondrial oxidative phosphorylation (OXPHOS) in matrix synthesis and mineralization.Methods. We studied cultured human articular chondrocytes and immortalized costal chondrocytes (TC28 cells). We also assessed the effects of antimycin A and oligomycin (inhibitors of mitochondrial complexes III and V, respectively) on chondrocyte mitochondrial respiration, ATP synthesis, and inorganic pyrophosphate (PPi) generation, and the mineralizing potential of released matrix vesicles (MV).Results. Articular chondrocytes and TC28 cells respired at comparable rates. Peroxynitrite and NO donors markedly suppressed respiration and ATP generation in chondrocytes. Because NO exerts multiple effects on chondrocytes, we investigated the primary functions of mitochondrial respiration and OXPHOS. To do so, we identified minimally cytotoxic doses of antimycin and oligomycin, which both induced intracellular ATP depletion (by 50-80%), attenuated collagen and proteoglycan synthesis, and blocked transforming growth factor ␤ from increasing intracellular ATP and elaboration of PPi, a critical inhibitor of hydroxyapatite deposition. Antimycin and oligomycin also abrogated the ability of the ATP-hydrolyzing enzyme plasma cell membrane glycoprotein 1 (PC-1) to increase chondrocyte PPi generation. Finally, MV from cells treated with antimycin or oligomycin contained less PPi and precipitated >50% more 45 Ca.Conclusion. Chondrocyte mitochondrial reserve, as NO-sensitive mitochondrial respiration-mediated ATP production, appears to support matrix synthesis and PPi elaboration and to regulate MV composition and mineralizing activity. NO-induced depression of chondrocyte respiration could modulate matrix loss and secondary cartilage mineralization in OA.The pathogenesis of osteoarthritis (OA) includes elaboration of increased amounts of nitric oxide (NO), as a consequence of up-regulation of chondrocyteinducible NO synthase induced by interleukin-1 (IL-1) and other factors (1-3). In chondrocytes, increased NO generation promotes OA (3,4) through effects that include inhibition of chondrocyte cytoskeletal actin polymerization and ␤1 integrin-dependent signaling (5,6), decreased expression of IL-1 receptor antagonist and transforming growth factor ␤ (TGF␤) (7,8), suppression of chondrocyte collagen and proteoglycan synthesis (9,10), activation of metalloproteinases (11), and suppression of proliferation as well as promotion of apoptosis (4,12). Cytokine-induced and NO-induced oxidative stress, the potentiation of injury by other oxidants, the formation of peroxynitrite from NO and O 2 Ϫ , and the nitration of proteins mediate several of the aforementioned effects of NO on chondrocytes (3,4,10,13,14).

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Differential mechanisms of inorganic pyrophosphate production by plasma cell membrane glycoprotein-1 and B10 in chondrocytes

Cited by 123 publications

References 49 publications

Pyrophosphate: a key inhibitor of mineralisation

Pyrophosphate: a key inhibitor of mineralisation

Extracellular nucleotide metabolism and signaling in the pathophysiology of articular cartilage

Mitochondrial oxidative phosphorylation is a downstream regulator of nitric oxide effects on chondrocyte matrix synthesis and mineralization

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