Mechanical loading stimulates chondrogenesis via the PKA/CREB-Sox9 and PP2A pathways in chicken micromass cultures

Juhász, Tamás; Matta, Csaba; Somogyi, Csilla; Katona, Éva; Takács, Roland; Soha, Rudolf Ferenc; Szabó, I.A.; Cserháti, Csaba; Sződy, Róbert; Karácsonyi, Zoltán; Bakó, Éva; Gergely, Pál; Zákány, Róza

doi:10.1016/j.cellsig.2013.12.001

Cited by 94 publications

(91 citation statements)

References 66 publications

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“…Sox9 promoter is known to be regulated by the CREB that binds to a CRE site upstream of Sox9 [30]. We have demonstrated that Sox9 and CREB transcription factors are phosphorylated by PKA during cartilage formation [31,32]. Moreover, a quite complex regulatory mechanism and synergism between Sox9 function and the cAMP-PKA-CREB pathway has been published in both mature and differentiating chondrocytes which includes BMP pathway connections [33].…”

Section: Regulation Of Chondrogenesis Focused On Vip and Pacapmentioning

confidence: 98%

PACAP and VIP signaling in chondrogenesis and osteogenesis

et al. 2015

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Section: Regulation Of Chondrogenesis Focused On Vip and Pacapmentioning

confidence: 98%

PACAP and VIP signaling in chondrogenesis and osteogenesis

et al. 2015

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“…Indeed, the addition of PACAP1-38 during oxidative stress prevented the inhibition of cartilage matrix production by normalizing the phosphorylation of Sox9 and CREB in chicken chondrogenic cells [ 13 ]. Recently, the involvement of PACAP or VIP signalling activation in mechanotransduction of developing articular cartilage has been proved by our group [ 68 ] and the importance of PKA in mechanical cellular response was proposed [ 34 ]. Mechanical load of in vitro chondrogenic cell cultures resulted in an increased PAC1 receptor and PACAP expression, and supported the undifferentiated stage of chondroblasts.…”

Section: Pacap and Vip Regulates Chondrogenic Differentiationmentioning

confidence: 98%

Role of PACAP and VIP Signalling in Regulation of Chondrogenesis and Osteogenesis

Juhász

Tamás

Zákány

et al. 2016

Current Topics in Neurotoxicity

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Pituitary adenylate cyclase activating polypeptide (PACAP) and vasoactive intestinal peptide (VIP) are multifunctional proteins that can regulate diverse physiological processes. These are also regarded as neurotrophic and antiinfl ammatory substances in the CNS, and PACAP is reported to prevent harmful effects of oxidative stress. In the last decade more and more data accumulated on the similar function of PACAP in various tissues, but its cartilage-and bone-related presence and functions have not been widely investigated yet. In this summary we plan to verify the presence and function of PACAP and VIP signalling tool kit during cartilage differentiation and bone formation. We give evidence about the protective function of PACAP in cartilage regeneration with oxidative or mechanically stress and also with the modulation of PACAP signalling in vitro in osteogenic cells. Our observations imply the therapeutic perspective that PACAP might be applicable as a natural agent exerting protecting effect during joint infl ammation and/or may promote cartilage regeneration during degenerative diseases of articular cartilage.

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“…A moderate level of cyclic mechanical stimulus increases the production of cartilage ECM components and promotes cartilage thickening, 25,26 whereas high levels of mechanical loading induce inflammatory responses, accelerate cartilage degradation, and eventually lead to OA. [27][28][29] In this study, expression of the genes encoding aggrecan and type I and type II collagens were upregulated at cyclic loads of 30-40 psi, but downregulated at 60 and 120 psi (Figure 2(a) and (b)).…”

Section: Discussionmentioning

confidence: 99%

A novel compressive stress-based osteoarthritis-like chondrocyte system

Young

Chuang

Gefen

et al. 2017

Exp Biol Med (Maywood)

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The lack of an effective treatment for osteoarthritis (OA) reflects the great need for alternative therapies and drug discovery. Disease models can be used for earlystage compound screening and disease studies. Chondrocytes are solely responsible for the maintenance of the articular cartilage extracellular matrix. Our strategy involved the generation of a cell-based model of OA, a more readily studied disease. Instead of using animal cartilage explants, we incorporated isolated porcine chondrocytes with hydrogel to form threedimensional assemblies. We could identify the specific magnitude-dependent metabolic responses of chondrocytes by applying a series of static and cyclic compression, and therefore successfully generated a novel OA-like cell-based model for drug screening. AbstractMechanical stress damage and insufficient self-repair can contribute to osteoarthritis (OA) in the affected joint. As the effects of stress on chondrocyte metabolism can regulate cartilage homeostasis, the specific stress-response condition is therefore a key to the generation of an OA disease model. We aimed to produce a specific stress-and cell-based OA model after evaluating the metabolic responses of chondrocytes in response to a series of static and cyclic compression stressors. A static load exceeding 40 psi initiated extracellular matrix (ECM) degradation through a decrease in the sulphated-glycosaminoglycan (GAG) content, upregulation of catabolic matrix metalloproteinase (MMP)-13 encoding gene expression, and downregulation of the ECM-related aggrecan and type II collagen encoding genes within 24 h. Indicators of pro-inflammatory events and oxidative stress were found to correlate with increased IL-6 expression and reactive oxygen species (ROS) production, respectively. However, chondrocytes stimulated by moderate cyclic loading (30-40 psi) exhibited increased ECM-related gene expression without significant changes in catabolic and pro-inflammatory gene expression. BMP-7 expression increased at cyclic loading levels above 30-60 psi. These results demonstrated that static compression exceeding 60 psi is sufficient to produce OA-like chondrocytes that exhibit signs of ECM degradation and inflammation. These OA-like chondrocytes could therefore be used as a novel cell-based drug screening system.

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Mechanical loading stimulates chondrogenesis via the PKA/CREB-Sox9 and PP2A pathways in chicken micromass cultures

Cited by 94 publications

References 66 publications

PACAP and VIP signaling in chondrogenesis and osteogenesis

PACAP and VIP signaling in chondrogenesis and osteogenesis

Role of PACAP and VIP Signalling in Regulation of Chondrogenesis and Osteogenesis

A novel compressive stress-based osteoarthritis-like chondrocyte system

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