Potential diagnostic value of a type X collagen neo-epitope biomarker for knee osteoarthritis

He, Yi; Manon‐Jensen, Tina; Arendt-Nielsen, Lars; Petersen, Kristian Kjær; Christiansen, T.; Samuels, Jonathan; Abramson, Steven B.; Karsdal, Morten A.; Attur, Mukundan; Bay‐Jensen, Anne‐Christine

doi:10.1016/j.joca.2019.01.001

Cited by 42 publications

(29 citation statements)

References 38 publications

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“…It is highly expressed by hypertrophic chondrocytes as a marker of hypertrophic regeneration. In sections of human osteoarthritic cartilage, Col10 was found around hypertrophic chondrocyte clusters in the deep zone close to tidemark ( He et al., 2019 ). Besides the collagens, aggrecan, known as a cartilage-specific proteoglycan core protein, is another crucial component of cartilage ECM ( Hu et al., 2019 ).…”

Section: Discussionmentioning

confidence: 99%

Evaluation of Long-Time Decoction-Detoxicated Hei-Shun-Pian (Processed Aconitum carmichaeli Debeaux Lateral Root With Peel) for Its Acute Toxicity and Therapeutic Effect on Mono-Iodoacetate Induced Osteoarthritis

Zhang

Wang

et al. 2020

Front. Pharmacol.

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Background As a degenerative joint disease with severe cartilage destruction and pain, osteoarthritis (OA) has no satisfactory therapy to date. In traditional Chinese medicine (TCM), Aconitum carmichaeli Debeaux derived Hei-shun-pian ( Hsp ) has been developed for joint pain treatment. However, it causes adverse events in OA patients. Long-time decoction has been traditionally applied to reduce the aconite toxicity of Hsp and other aconite herbs, but its detoxifying effect is uncertain. Methods Hsp was extracted with dilute decoction times (30, 60, and 120 min) and evaluated by toxicological, chemical, pharmacological assays. Acute toxicity assay and chemical analysis were employed to determine the toxicity and chemoprofile of Hsp extracts, respectively. Since the detoxified Hsp (d Hsp ) was defined, its therapeutic effect was evaluated by using an OA rat model induced by monosodium iodoacetate. d Hsp at 14 g/kg was orally administered for 28 days, and the pain assessments (mechanical withdrawal threshold and thermal withdrawal latency) and histopathological analyses (HE and safranin-O staining) were performed. Real-time PCR (qPCR) was applied to determine the molecular actions of d Hsp on cartilage tissue and on chondrocytes. MTT assay was conducted to evaluate the effect of d Hsp on the cell viability of chondrocytes. The cellular and molecular assays were also conducted to analyze the functions of chemical components in d Hsp . Results The chemoprofile result showed that the contents of toxic alkaloids (aconitine, mesaconitine, and hypaconitine) were decreased but that of non-toxic alkaloids (benzoylaconitine, benzoylmesaconitine, and benzoylhypaconitine) were increased with increasing decoction time. Acute toxicity assay showed that only Hsp extract with 120 min decoction was non-toxic within the therapeutic dose range. Thus, it was defined as d Hsp for further experiment. In OA experiment, d Hsp significantly attenuated joint pain and prevented articular degeneration from MIA attack. qPCR data showed that d Hsp restored the abnormal expressions of Col10 , Mmp2 , Sox5 , Adamts4/5/9 , and up-regulated Col2 expression in rat cartilage. In vitro , d Hsp- containing serum significantly proliferated rat chondrocytes and regulated the gene expressions of Col2 , Mmp1 , Adamts9...

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Section: Discussionmentioning

confidence: 99%

Evaluation of Long-Time Decoction-Detoxicated Hei-Shun-Pian (Processed Aconitum carmichaeli Debeaux Lateral Root With Peel) for Its Acute Toxicity and Therapeutic Effect on Mono-Iodoacetate Induced Osteoarthritis

Zhang

Wang

et al. 2020

Front. Pharmacol.

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“…Mutant or abnormal human COL10A1 expression are often accompanied by abnormal chondrocyte hypertrophy, as seen in children and young adults with multiple skeletal dysplasia (Warman et al, 1993;Ikegawa et al, 1998;Bateman et al, 2005;Lu et al, 2014;Ain et al, 2018). Abnormal COL10A1 expression and chondrocyte hypertrophy are also observed in elderly individuals with osteoarthritis (OA), who show osteophyte formation involving a process mimicking the endochondral pathway (von der Mark et al, 1995;Girkontaite et al, 1996;Drissi et al, 2005;Lamas et al, 2010;Saito et al, 2010;Armiento et al, 2019;Gratal et al, 2019;He et al, 2019). Recent studies show that intact trimeric noncolla-genous 1 domain of type X collagen is a degradation by-product of endochondral ossification released into the circulation in proportion to the overall growth plate.…”

Section: Introductionmentioning

confidence: 99%

Expression Profiling and Functional Analysis of Candidate Col10a1 Regulators Identified by the TRAP Program

et al. 2021

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Hypertrophic chondrocytes and their specific marker, the type X collagen gene (Col10a1), are critical components of endochondral bone formation during skeletal development. We previously found that Runx2 is an indispensable mouse Col10a1 gene regulator and identified many other transcription factors (TFs) that potentially interact with the 150-bp Col10a1 cis-enhancer. However, the roles of these candidate TFs in Col10a1 expression and chondrocyte hypertrophy have not been elucidated. Here, we focus on 32 candidate TFs recently identified by analyzing the 150-bp Col10a1 enhancer using the transcription factor affinity prediction (TRAP) program. We found that 12 TFs (Hoxa3, Lsx, Evx2, Dlx5, S8, Pax2, Egr2, Mef2a, Barhl2, GKlf, Sox17, and Crx) were significantly upregulated and four TFs (Lhx4, Tbx5, Mef2c, and Hb9) were significantly downregulated in hypertrophic MCT cells, which show upregulation of Col10a1 expression. Most of the differential expression pattern of these TFs conformed with the results obtained from ATDC5 cell model and primary mouse chondrocytes. Notably, Tbx5 was downregulated upon Col10a1 upregulation, overexpression of Tbx5 decreased Col10a1 expression, and knock-down of Tbx5 increased Col10a1 expression in hypertrophic chondrocytes, suggesting that Tbx5 is a negative regulator of Col10a1. We further generated a stable Tbx5-overexpressing ATDC5 cell line and ColX-Tbx5 transgenic mice driven by Col10a1-specific enhancers and promoters. Tbx5 overexpression decreased Col10a1 expression in ATDC5 cells cultured as early as day 7 and in limb tissue on post-natal day 1. Slightly weaker alkaline phosphatase staining was also observed in cell culture on day 7 and in limb digits on embryonic day 17.5, indicating mildly delayed ossification. Further characterization of these candidate Col10a1 transcriptional regulators could help identify novel therapeutic targets for skeletal diseases associated with abnormal chondrocyte hypertrophy.

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“…In line with this, microarray studies of BML tissue isolates have shown increased expression of proteases, osteogenic and chondrogenic molecules such as matrix metalloproteinase (MMP) 13 and molecules associated with Wnt signaling, suggestive of local repair processes and heavy remodeling [75]. OA development is associated with changes in chondrocyte behavior, including matrix calcification and expression of hypertrophic markers such as MMP13 and type X collagen, which are both signs of hypertrophy [76,77]. These phenomena, in many cases, appear similar to the function of hypertrophic chondrocytes in the growth plate of long bones undergoing endochondral ossification during growth.…”

Section: Fibrodysplasia Ossificans Progressivathe Systemic Ossificatimentioning

confidence: 83%

“…The marker was also associated with increased severity defined by KL grade. Interestingly the level of Col10neo was higher in OA patients compared to RA patients suggesting that type X collagen expression and chondrocyte hypertrophy not surprisingly is more pronounced in OA compared to RA [76,107]. Although not a neo-epitope, the cartilage residing cartilage oligomeric protein (COMP) is increased in serum and synovial fluid of OA patients [102,103], and one study has shown that high baseline levels predict development of radiograph knee OA [104].…”

Section: Tissue Turnover Markers In Osteoarthritismentioning

confidence: 99%

Bone phenotypes in rheumatology – there is more to bone than just bone

Thudium

Nielsen

Sardar

et al. 2020

BMC Musculoskelet Disord

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Osteoarthritis, rheumatoid arthritis, psoriatic arthritis, and ankylosing spondylitis, all have one clear common denominator; an altered turnover of bone. However, this may be more complex than a simple change in bone matrix and mineral turnover. While these diseases share a common tissue axis, their manifestations in the area of pathology are highly diverse, ranging from sclerosis to erosion of bone in different regions. The management of these diseases will benefit from a deeper understanding of the local versus systemic effects, the relation to the equilibrium of the bone balance (i.e., bone formation versus bone resorption), and the physiological and pathophysiological phenotypes of the cells involved (e.g., osteoblasts, osteoclasts, osteocytes and chondrocytes). For example, the process of endochondral bone formation in chondrocytes occurs exists during skeletal development and healthy conditions, but also in pathological conditions. This review focuses on the complex molecular and cellular taxonomy of bone in the context of rheumatological diseases that alter bone matrix composition and maintenance, giving rise to different bone turnover phenotypes, and how biomarkers (biochemical markers) can be applied to potentially describe specific bone phenotypic tissue profiles.

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Potential diagnostic value of a type X collagen neo-epitope biomarker for knee osteoarthritis

Cited by 42 publications

References 38 publications

Evaluation of Long-Time Decoction-Detoxicated Hei-Shun-Pian (Processed Aconitum carmichaeli Debeaux Lateral Root With Peel) for Its Acute Toxicity and Therapeutic Effect on Mono-Iodoacetate Induced Osteoarthritis

Evaluation of Long-Time Decoction-Detoxicated Hei-Shun-Pian (Processed Aconitum carmichaeli Debeaux Lateral Root With Peel) for Its Acute Toxicity and Therapeutic Effect on Mono-Iodoacetate Induced Osteoarthritis

Expression Profiling and Functional Analysis of Candidate Col10a1 Regulators Identified by the TRAP Program

Bone phenotypes in rheumatology – there is more to bone than just bone

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