A gene expression study of normal and damaged cartilage in anteromedial gonarthrosis, a phenotype of osteoarthritis

Snelling, Sarah; Rout, R; Davidson, Rose; Clark, Ian M.; Carr, Andrew; Hulley, P A; Price, Andrew

doi:10.1016/j.joca.2013.12.009

Cited by 74 publications

(71 citation statements)

References 45 publications

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“…ADAM12 is the ADAM most consistently reported to display increased expression in human OA cartilage10, 11, 12, 15, 16, 17, 62. Its expression is reported to correlate with Mankin score 62 , and increased expression has also been reported in mice 2 weeks after DMM surgery 7 .…”

Section: Adamtssmentioning

confidence: 99%

ADAMTS and ADAM metalloproteinases in osteoarthritis – looking beyond the ‘usual suspects’

Yang

Chanalaris

Troeberg

2017

Osteoarthritis and Cartilage

216

164

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SummaryIntroductionMatrix metalloproteinases (MMPs) and ‘aggrecanase’ a disintegrin and metalloproteinase with thrombospondin motifs (ADAMTSs) are well established to play key roles in osteoarthritis (OA) through degradation of extracellular matrix (ECM) type II collagen and aggrecan, and are thus potential targets for development of OA therapies.ObjectiveThis paper aims to provide a comprehensive review of the expression and potential roles of other, lesser-known ADAMTSs and related adamalysins (or a disintegrin and metalloproteinases (ADAMs)) in cartilage, with a view to identifying potentially protective or homeostatic metalloproteinases in the joint and informing consequent selective inhibitor design.DesignA comprehensive literature search was performed using PubMed terms ‘osteoarthritis’ and ‘ADAMTS’ or ‘ADAM’.ResultsSeveral ADAMTSs and ADAMs were identified as having reportedly increased expression in OA. These include enzymes likely to play roles in cartilage matrix anabolism (e.g., the procollagen N-proteinases ADAMTS-2, ADAMTS-3 and ADAMTS-14), chondrocyte differentiation and proliferation (e.g., ADAM9, ADAM10, ADAM12), as well as enzymes contributing to cartilage catabolism (e.g., Cartilage oligomeric protein (COMP)-degrading ADAMTS-7 and ADAMTS-12).ConclusionsIn addition to the well-characterised MMPs, ADAMTS-4 and ADAMTS-5, many other ADAMTSs and ADAMs are expressed in cartilage and several show significantly altered expression in OA. Studies aimed at elucidating the pathophysiological roles of these enzymes in cartilage will contribute to our understanding of OA pathogenesis and enable design of targeted inhibitors that effectively target metalloproteinase-mediated cartilage degradation while sparing cartilage repair pathways.

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Section: Adamtssmentioning

confidence: 99%

ADAMTS and ADAM metalloproteinases in osteoarthritis – looking beyond the ‘usual suspects’

Yang

Chanalaris

Troeberg

2017

Osteoarthritis and Cartilage

216

164

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“…In the present study, we demonstrated the negative effect of PNE on IGF1 signaling and matrix genes expression. Due to the critical role of IGF1 signaling in promoting proteoglycan and collagen network formation, and thereby improving mechanical properties, a reduction of IGF1 signaling was associated with OA progression (35, 36). It is possible that reduced IGF1 signaling mediate the toxic effect of PNE on cartilage development.…”

Section: Discussionmentioning

confidence: 99%

Intrauterine low‐functional programming of IGF1 by prenatal nicotine exposure mediates the susceptibility to osteoarthritis in female adult rat offspring

et al. 2015

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This study aimed to evaluate whether female adult offspring born with intrauterine growth retardation induced by prenatal nicotine exposure (PNE) are susceptible to osteoarthritis (OA) and to explore the underlying programming mechanisms. Pregnant rats were treated with nicotine or saline at 2.0 mg/kg/d from gestational d 11 to 20. The female adult offspring with or without PNE were forced with a strenuous treadmill running for 6 wk to induce OA. Nicotine's effects on fetal articular chondrocytes were studied by exposing chondrocytes to nicotine for 10 d, and dihydro-β-erythroidine, a selective α4β2-nicotinic acetylcholine receptor (nAChR) inhibitor, was used to identify the change of nicotine's effect. For adult offspring, increased cartilage destruction and accelerated OA progression were observed in the PNE group with running; the expression of α1 chain of type II collagen (Col2A1), aggrecan, SRY-type high mobility group box 9 (Sox9), and IGF1 signaling molecules in the cartilage of PNE offspring were decreased. For fetuses, elevated serum corticosteroid and nicotine levels and suppressed IGF1 levels were observed; expression of Col2A1, aggrecan, Sox9, and IGF1 were reduced. The result of chondrocytes revealed that nicotine impeded the expression of Col2A1, aggrecan, and IGF1; blocking α4β2-nAChR rescued nicotine's suppression. In conclusion, PNE increases the susceptibility of adult offspring to OA; the potential mechanism involves IGF1 low-functional programming in articular cartilage caused directly by the action of nicotine on α4β2-nAChR.

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“…Indeed, comparison between damaged and undamaged areas of the condyle, as described in (Snelling et al . ), shows expression patterns of genes involved in cell signalling, extracellular matrix remodelling and inflammatory responses; these include matrix metalloproteinases (MMPs), growth factor signalling proteins, collagens and SOX 9, amongst other common OA genes (Sato et al . ; Geyer et al .…”

Section: Separating Initiation and Progression Phases Using Human Tismentioning

confidence: 99%

“…The use of such protocols has identified various pathways and molecular markers for early and late OA. Indeed, comparison between damaged and undamaged areas of the condyle, as described in (Snelling et al 2014), shows expression patterns of genes involved in cell signalling, extracellular matrix remodelling and inflammatory responses; these include matrix metalloproteinases (MMPs), growth factor signalling proteins, collagens and SOX 9, amongst other common OA genes (Sato et al 2006;Geyer et al 2009). Fukui et al (2008) have separated the severity of degradation by grouping the samples (from the same OA patients' joint) into four distinct areas depending on the zones of the articular cartilage affected (preserved area, damaged with superficial, middle and deep zones present, damaged with middle and deep zones, damaged with deep zones only).…”

Section: Separating Initiation and Progression Phases Using Human Tismentioning

confidence: 99%

Models to define the stages of articular cartilage degradation in osteoarthritis development

Poulet

2017

Int J Experimental Path

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SummaryOsteoarthritis (OA) is a common chronic disorder that affects an increasing number of the ageing population. Despite the prevalence, there are currently no therapies. Defining new therapies that target specific pathogenic phases of disease development relies on the effective separation of the different stages of OA. This manuscript reviews the tissues and models that are being used to separate these stages of disease, in particular initiation and early and late progression. These models include human tissues with known initiating factors, the use of anatomical locations with defined relationships to the primary cartilage lesion area, timing of OA development in well‐described animal models and the versatility of a non‐invasive model of murine knee joint trauma.

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A gene expression study of normal and damaged cartilage in anteromedial gonarthrosis, a phenotype of osteoarthritis

Cited by 74 publications

References 45 publications

ADAMTS and ADAM metalloproteinases in osteoarthritis – looking beyond the ‘usual suspects’

ADAMTS and ADAM metalloproteinases in osteoarthritis – looking beyond the ‘usual suspects’

Intrauterine low‐functional programming of IGF1 by prenatal nicotine exposure mediates the susceptibility to osteoarthritis in female adult rat offspring

Models to define the stages of articular cartilage degradation in osteoarthritis development

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