Wnt/β‐catenin signaling of cartilage canal and osteochondral junction chondrocytes and full thickness cartilage in early equine osteochondrosis

Kinsley, Marc A.; Semevolos, Stacy A.; Duesterdieck-Zellmer, Katja F.

doi:10.1002/jor.22846

Cited by 20 publications

(21 citation statements)

References 30 publications

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“…On one hand, abnormal Wnt signalling in adult tissues may contribute to pathogenesis of musculoskeletal diseases, on the other, in embryonic tissue the same serves as an important regulator of chondrocyte development (Yates et al, 2005). The findings from this study in healthy rats are also in line with the previous study from Kinsley et al (2015). There were low levels of detection of Dkk1 activity in healthy rat tissues in comparison to the pathological (OVX) and necrotic tissues (inflammatory tissue).…”

Section: Discussionsupporting

confidence: 89%

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Differences in expression of Wnt antagonist Dkk1 in healthy versus pathological bone samples

Ray

Khassawna

Sommer

et al. 2016

Journal of Microscopy

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Wnt/β-catenin signalling components was shown to affect bone cells function including chondrocytes.Secreted Dkk1, a potent osteogenesis inhibiting factor mediates bone loss in diseased bones by suppressing the biological actions of Wnt proteins. In addition, increased Dkk1 signalling inhibits chondrogenesis in new bone formation. Recent findings also show there exists a cross-talk between the chondrocytes and the cells of the osteoblast lineage, which are the most affected cell types in muskuloskeletal disorders. This study investigated whether spatial expression of Dkk1 is confined to only osteoblasts, osteocytes or chondrocytes. The second objective was to detect a difference in the Dkk1 expression pattern in healthy subjects when compared to pathological state. To elucidate the cell specificity of Dickkopf-1 (Dkk1) in healthy bones, samples from female Sprague-Dawley rats were tested against two different antibodies with the two most widely accepted visualization system (ABC and Envision). The findings show Dkk1 specificity predominantly for osteoblasts, chondrocytes and osteocytes depending upon the antibody used. In addition, Dkk1 expression was evaluated in different cells of human osteoarthritis (OA) and rheumatoid arthritis (OA) patients. Its overexpression in pathologic state also suggests the role of Dkk1 in bone formation. This is scientifically and clinically important in studying the effect of Dkk1 in bone healing and in designing treatments for patients with compromised bone status. Taking into consideration the paradigm that cartilage and subchondral bone behave as an interconnected functional unit, normalization of cell behaviour in one compartment may have benefits in both tissues.

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Section: Discussionsupporting

confidence: 89%

“…The findings from this study in healthy rats are also in line with the previous study from Kinsley et al . (). There were low levels of detection of Dkk1 activity in healthy rat tissues in comparison to the pathological (OVX) and necrotic tissues (inflammatory tissue).…”

Section: Discussionmentioning

confidence: 97%

Differences in expression of Wnt antagonist Dkk1 in healthy versus pathological bone samples

Ray

Khassawna

Sommer

et al. 2016

Journal of Microscopy

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“…An increasing Wnt inhibitor expression (Wif-1, Axin1, Dkk-1) in femoropatellar joint cartilage of OC-affected foals in comparison to OC-non-affected foals [61] may influence the retonic acid signalling pathway and may have an inhibitory effect on chondrocyte maturation [62]. The role of PTH-rP, Wnt/b-catenin signalling and Ihh pathways was shown in several studies [59,61,63] and genes on these pathways partially correspond with OC-risk loci [54] (Supplementary Item 11).…”

Section: Ecamentioning

confidence: 93%

Genetic risk factors for osteochondrosis in various horse breeds

Naccache

Metzger

Distl

2018

Equine Veterinary Journal

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Osteochondrosis (OC) is an injury to cartilage canals with a following necrosis in the growth cartilage, from there it can develop to osteochondrosis dissecans (OCD). Due to its high impact in the equine industry, new insights into predisposing factors and potential high-risk genetic variants are warranted. This article reviews advancements in quantitative and molecular genetics in refining estimation of genetic parameters and identifying predisposing genetic loci. Heritabilities were highest for hock OC with estimates at 0.29-0.46 in Hanoverian warmblood and Norwegian trotters, whereas in Thoroughbreds only very low genetic variation seemed to be present in hock OC lesions. Whole genome scans using the Illumina Equine SNP50 or SNP70 Beadchip were performed in Thoroughbred, Standardbred, French and Norwegian trotter, Hanoverian and Dutch warmblood. Validation studies in Spanish Purebred and Hanoverian warmblood horses corroborated OC risk loci on ECA 3, 14, 27 and 29. Particularly, a strong association with hock-OCD was found for a single nucleotide polymorphism (SNP) on horse chromosome (ECA) 3 upstream to the LCORL gene. Gene expression and microRNA analyses may be helpful to understand pathophysiological processes in equine OC and to connect OCD-associated genomic regions with potential candidate genes. Furthermore progress in elucidating the underlying genetic variants and pathophysiological changes in OC may be expected from whole genome DNA and RNA next-generation sequencing studies.

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“…The information gained from this study thus fills a gap in our knowledge base by providing a description of molecular activity during this critical growth period. Samples used in this study contributed to several previous studies evaluating gene and protein expression in foals with and without osteochondrosis, which when evaluated together paint a much more comprehensive picture of the complex molecular events occurring during this process (Kinsley and Kinsley, 201510;Riddick et al, 2012;Semevolos et al, 2018) (Table 9, 10). To date, there is no current model for studies in endochondral ossification and osteochondrosis in children.…”

Section: Chapter 6: Conclusionmentioning

confidence: 99%