Articular chondrocyte network mediated by gap junctions: role in metabolic cartilage homeostasis

Mayán, M.D.; Gago-Fuentes, Raquel; Carpintero-Fernández, Paula; Fernández-Puente, Patricia; Filgueira-Fernández, P.; Goyanes, N.; Valiūnas, Virginijus; Brink, Peter R.; Goldberg, Gary S.; Blanco, Francisco J.

doi:10.1136/annrheumdis-2013-204244

Cited by 69 publications

(86 citation statements)

References 47 publications

(38 reference statements)

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“…13,14 While the first two molecules disappear in the course of chondrogenesis, 13 gap junctions can still be found in mature cartilage. 15 Gap junctions are intercellular channels formed by connexins that allow for rapid exchange of ions, metabolites, and other small-molecule messengers. 16 They are expressed in virtually all tissues and are involved in various cellular functions, including cell growth, differentiation, and death.…”

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confidence: 99%

The Importance of Connexin Hemichannels During Chondroprogenitor Cell Differentiation in Hydrogel Versus Microtissue Culture Models

Schrobback

Woodfield

2015

Tissue Engineering Part A

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Appropriate selection of scaffold architecture is a key challenge in cartilage tissue engineering. Gap junctionmediated intercellular contacts play important roles in precartilage condensation of mesenchymal cells. However, scaffold architecture could potentially restrict cell-cell communication and differentiation. This is particularly important when choosing the appropriate culture platform as well as scaffold-based strategy for clinical translation, that is, hydrogel or microtissues, for investigating differentiation of chondroprogenitor cells in cartilage tissue engineering. We, therefore, studied the influence of gap junction-mediated cell-cell communication on chondrogenesis of bone marrow-derived mesenchymal stromal cells (BM-MSCs) and articular chondrocytes. Expanded human chondrocytes and BM-MSCs were either (re-) differentiated in micromass cell pellets or encapsulated as isolated cells in alginate hydrogels. Samples were treated with and without the gap junction inhibitor 18-a glycyrrhetinic acid (18aGCA). DNA and glycosaminoglycan (GAG) content and gene expression levels (collagen I/II/X, aggrecan, and connexin 43) were quantified at various time points. Protein localization was determined using immunofluorescence, and adenosine-5¢-triphosphate (ATP) was measured in conditioned media. While GAG/DNA was higher in alginate compared with pellets for chondrocytes, there were no differences in chondrogenic gene expression between culture models. Gap junction blocking reduced collagen II and extracellular ATP in all chondrocyte cultures and in BM-MSC hydrogels. However, differentiation capacity was not abolished completely by 18aGCA. Connexin 43 levels were high throughout chondrocyte cultures and peaked only later during BM-MSC differentiation, consistent with the delayed response of BM-MSCs to 18aGCA. Alginate hydrogels and microtissues are equally suited culture platforms for the chondrogenic (re-)differentiation of expanded human articular chondrocytes and BM-MSCs. Therefore, reducing direct cell-cell contacts does not affect in vitro chondrogenesis. However, blocking gap junctions compromises cell differentiation, pointing to a prominent role for hemichannel function in this process. Therefore, scaffold design strategies that promote an increasing distance between single chondroprogenitor cells do not restrict their differentiation potential in tissue-engineered constructs.

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confidence: 99%

The Importance of Connexin Hemichannels During Chondroprogenitor Cell Differentiation in Hydrogel Versus Microtissue Culture Models

Schrobback

Woodfield

2015

Tissue Engineering Part A

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“…In addition, caldesmon plays important roles in the migration of nonmuscle cells via regulating the actin-myosin system (82), and caldesmon binding to myosin has been reported to result in the enhancement of axon extension (83). Interestingly, we have found that chondrocytes from OA patients contain longer cellular extensions (more than 200 m in length) when compared with chondrocytes in healthy cartilage (7). Further studies will be necessary to reveal the role of Cx43 in these processes and to discern its function in OA chondrocytes.…”

Section: Fig 2 Cx43-nuclear and Perinuclear Interactorsmentioning

confidence: 72%

“…In fact, the eye lens and articular cartilage of adults are avascular organs, and because no blood supply reaches these tissues, it has been reported that cells in these tissues are maintained by the movement of fluids, ions, nutrients (e.g. glucose), and metabolites through a network of GJs (7,54,55). In addition, results from different reports strongly suggest that inhibition of GJIC modifies glucose uptake and that glucose levels modify Cx43 gene expression (56).…”

Section: Fig 2 Cx43-nuclear and Perinuclear Interactorsmentioning

confidence: 99%

“…Our group is interested in investigating the physiopathological mechanism that is associated with osteoarthritis (OA). Recent results suggest a direct role of Cx43 in the development of OA that is not necessary related to its channel function (7,23,24). For instance, only a few connexin-interacting proteins have been described to date, and previous studies have used artificial systems, such as yeast two-hybrid screens or Cx43-domain fusion proteins.…”

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confidence: 99%

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Proteomic Analysis of Connexin 43 Reveals Novel Interactors Related to Osteoarthritis

Gago-Fuentes

Fernández-Puente

Megı́as

et al. 2015

Molecular & Cellular Proteomics

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We have previously reported that articular chondrocytes in tissue contain long cytoplasmic arms that physically connect two distant cells. Cell-to-cell communication occurs through connexin channels termed Gap Junction (GJ) channels, which achieve direct cellular communication by allowing the intercellular exchange of ions, small RNAs, nutrients, and second messengers. The Cx43 protein is overexpressed in several human diseases and inflammation processes and in articular cartilage from patients with osteoarthritis (OA). An increase in the level of Cx43 is known to alter gene expression, cell signaling, growth, and cell proliferation. The interaction of proteins with the C-terminal tail of connexin 43 (Cx43) directly modulates GJ-dependent and -independent functions. Here, we describe the isolation of Cx43 complexes using mild extraction conditions and immunoaffinity purification. Cx43 complexes were extracted from human primary articular chondrocytes isolated from healthy donors and patients with OA. The proteomic content of the native complexes was determined using LC-MS/MS, and protein associations with Cx43 were validated using Western blot and immunolocalization experiments. We identified >100 Cx43-associated proteins including previously uncharacterized proteins related to nucleolar functions, RNA transport, and translation. We also identified several proteins involved in human diseases, cartilage structure, and OA as novel functional Cx43 interactors, which emphasized the importance of Cx43 in the normal physiology and structural and functional integrity of chondrocytes and articular cartilage. Gene Ontology (GO) terms of the proteins identified in the OA samples showed an enrichment of Cx43-interactors related to cell adhesion, calmodulin binding, the nucleolus, and the cytoskeleton in OA samples compared with healthy samples. However, the mitochondrial proteins SOD2 and ATP5J2 were identified only in samples from healthy donors. The identification of Cx43 interactors will provide clues to the functions of Cx43 in human cells and its roles in the development of several diseases, including OA. Molecular & Cellular

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“…Direct cell-to-cell communication has been shown in the superficial zone of articular chondrocytes [155]. A paradigm challenging study has even shown that chondrocytes in situ may form long cell processes, 5 to 150 microns in length, that permit communication through gap junction channels [156]. Increased presence of gap junction plaques and Cx43 expression have been found in synovial lining cells obtained from the knee of patients with osteoarthritis [157].…”

Section: Connexins In Cartilage Ligaments and Tendonsmentioning

confidence: 99%

Connexins and pannexins in the skeleton: gap junctions, hemichannels and more

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Stains

2015

Cell. Mol. Life Sci.

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Regulation of bone homeostasis depends on the concerted actions of bone-forming osteoblasts and bone-resorbing osteoclasts, controlled by osteocytes, cells derived from osteoblasts surrounded by bone matrix. The control of differentiation, viability and function of bone cells relies on the presence of connexins. Connexin43 regulates the expression of genes required for osteoblast and osteoclast differentiation directly or by changing the levels of osteocytic genes, and connexin45 may oppose connexin43 actions in osteoblastic cells. Connexin37 is required for osteoclast differentiation and its deletion results in increased bone mass. Less is known on the role of connexins in cartilage, ligaments and tendons. Connexin43, connexin45, connexin32, connexin46 and connexin29 are expressed in chondrocytes, while connexin43 and connexin32 are expressed in ligaments and tendons. Similarly, although the expression of pannexin1, pannexin2 and pannexin3 has been demonstrated in bone and cartilage cells, their function in these tissues is not fully understood.

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Articular chondrocyte network mediated by gap junctions: role in metabolic cartilage homeostasis

Cited by 69 publications

References 47 publications

The Importance of Connexin Hemichannels During Chondroprogenitor Cell Differentiation in Hydrogel Versus Microtissue Culture Models

The Importance of Connexin Hemichannels During Chondroprogenitor Cell Differentiation in Hydrogel Versus Microtissue Culture Models

Proteomic Analysis of Connexin 43 Reveals Novel Interactors Related to Osteoarthritis

Connexins and pannexins in the skeleton: gap junctions, hemichannels and more

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