Hyaluronidase expression in cultured growth plate chondrocytes during differentiation

Tanimoto, Kotaro; Suzuki, Aya; Ohno, Shigeru; Honda, K.; Tanaka, Nobuaki; Doi, Takumi; Nakahara-Ohno, Maiko; Yoneno, Kiyoshi; Nakatani, Yuki; Ueki, M.; Yanagida, Tamami; Kitamura, Reiko; Tanne, Kazuo

doi:10.1007/s00441-004-0966-7

Cited by 17 publications

(11 citation statements)

References 27 publications

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“…Other studies show that HA released from rabbit growth plate chondrocytes during in vitro differentiation has a broad ranging 404 E. R. Bastow et al Synthesis and degradation of hyaluronan molecular mass [226]. Since hyal1 and hyal2 are expressed in the proliferative and hypertrophic zones of rabbit growth plate [227], these results suggest that HYALs, and synthases producing high M r HA, are active concurrently. Depolymerisation of HA by HYALs in growth plate cartilage will simultaneously depolymerise the HAaggrecan-link protein aggregates.…”

Section: Hyals and Hass In Longitudinal Bone Growthmentioning

confidence: 80%

Hyaluronan synthesis and degradation in cartilage and bone

Bastow

Byers

Golub

et al. 2007

Cell. Mol. Life Sci.

168

106

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Hyaluronan (HA) is a large but simple glycosaminoglycan composed of repeating D-glucuronic acid, beta1-3 linked to N-acetyl-D-glucosamine beta1-4, found in body fluids and tissues, in both intra- and extracellular compartments. Despite its structural simplicity, HA has diverse functions in skeletal biology. In development, HA-rich matrices facilitate migration and condensation of mesenchymal cells, and HA participates in joint cavity formation and longitudinal bone growth. In adult cartilage, HA binding to aggrecan immobilises aggrecan, retaining it at the high concentrations required for compressive resilience. HA also appears to regulate bone remodelling by controlling osteoclast, osteoblast and osteocyte behaviour. The functions of HA depend on its intrinsic properties, which in turn rely on the degree of polymerisation by HA synthases, depolymerisation by hyaluronidases, and interactions with HA-binding proteins. HA synthesis and degradation are closely regulated in skeletal tissues and aberrant synthetic or degradative activity causes disease. The role and regulation of HA synthesis and degradation in cartilage, bone and skeletal development is discussed.

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Section: Hyals and Hass In Longitudinal Bone Growthmentioning

confidence: 80%

Hyaluronan synthesis and degradation in cartilage and bone

Bastow

Byers

Golub

et al. 2007

Cell. Mol. Life Sci.

168

106

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“…Furthermore, future studies would ideally investigate NP and AF cells separately, although our own preliminary data on bovine NP and AF cells indicate marginal zonal differences in HYAL expression. Increased HYAL expression and/or activity have been described in numerous pathologies, such as during asthma (within the epithelium) [30], cartilage hypertrophy [52] or osteoarthritis and rheumatoid arthritis (within the knee synovium/synoviocytes) [53,54]. HYAL deficiency or knockdown/knockout have also been described to promote certain pathologies, leading, e.g., to swelling of the periarticular masses [55] as well as to progression of osteoarthritis [56,57].…”

Section: Discussionmentioning

confidence: 99%

Expression and activity of hyaluronidases HYAL-1, HYAL-2 and HYAL-3 in the human intervertebral disc

Krupková

Greutert

Boos³

et al. 2019

Eur Spine J

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Purpose Hyaluronic acid plays an essential role in water retention of the intervertebral disc (IVD) and thus provides flexibility and shock absorbance in the spine. Hyaluronic acid gets degraded by hyaluronidases (HYALs), and some of the resulting fragments were previously shown to induce an inflammatory and catabolic response in human IVD cells. However, no data currently exist on the expression and activity of HYALs in IVD health and disease. Methods Gene expression, protein expression and activity of HYALs were determined in human IVD biopsies with different degrees of degeneration (n = 50 total). Furthermore, freshly isolated human IVD cells (n = 23 total) were stimulated with IL-1β, TNF-α or H 2 O 2 , followed by analysis of HYAL-1, HYAL-2 and HYAL-3 gene expression. Results Gene expression of HYAL-1 and protein expression of HYAL-2 significantly increased in moderate/severe disc samples when compared to samples with no or low IVD degeneration. HYAL activity was not significantly increased due to high donor-donor variation, but seemed overall higher in the moderate/severe group. An inflammatory environment, as seen during IVD disease, did not affect HYAL-1, HYAL-2 or HYAL-3 expression, whereas exposure to oxidative stress (100 µM H 2 O 2) upregulated HYAL-2 expression relative to untreated controls. Conclusion Although HYAL-1, HYAL-2 and HYAL-3 are all expressed in the IVD, HYAL-2 seems to have the highest pathophysiological relevance. Nonetheless, further studies will be needed to comprehensively elucidate its significance and to determine its potential as a therapeutic target.

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“…HYAL3 which belongs to the Hyaluronan family, the major component of the extracellular matrix of cartilage, contributes to its structural and functional integrity. Tanimoto et al demonstrated that the selective expression of HYALs is essential for extracellular HA metabolism during chondrocyte differentiation 20…”

Section: Discussionmentioning

confidence: 99%

“…Tanimoto et al demonstrated that the selective expression of HYALs is essential for extracellular HA metabolism during chondrocyte differentiation. 20 Other genes related to the immune system are modulated. This mechanism could be related to the osseointegration process: indeed the inserted material has to be recognized as ''self'' by the immune system.…”

Section: Discussionmentioning

confidence: 99%

Genetic effect of anatase on osteoblast‐like cells

et al. 2007

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Titanium is the gold standard among materials used for prosthetic devices, because of its good mechanical and chemical properties. When exposed to oxygen, titanium becomes an oxide that is biocompatible and able to induce osseointegration. Three allotropic forms of titanium dioxide exist, that is brookite, rutile, and anatase. Anatase can be prepared as a colloidal suspension and then used to coat surfaces. Anatase coating (AC) can potentially have specific biological effects. Here we are testing the effect of AC on osteoblast-like cells (MG63) by using microarray techniques to identify genes that are differently regulated in osteoblasts exposed to AC. By using DNA microarrays containing 20,000 genes, we identified in osteoblast-like cell lines (MG-63) cultured on AC, several genes whose expression was significantly up- or downregulated. They cover a broad range of functional activities: signaling transduction, immunity, cell cycle regulation, lysosomes composition and vesicular transport, cell adhesion, cytoskeleton and extracellular matrix components, proliferation, and apoptosis. The data reported constitute, to our knowledge, the first genetic portrait of AC effects. They can be relevant to a better understanding of the molecular mechanism of bone regeneration and as a model for comparing other materials with similar clinical effects.

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Hyaluronidase expression in cultured growth plate chondrocytes during differentiation

Cited by 17 publications

References 27 publications

Hyaluronan synthesis and degradation in cartilage and bone

Hyaluronan synthesis and degradation in cartilage and bone

Expression and activity of hyaluronidases HYAL-1, HYAL-2 and HYAL-3 in the human intervertebral disc

Genetic effect of anatase on osteoblast‐like cells

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