High Bone Mass in Mice Lacking Cx37 Because of Defective Osteoclast Differentiation

dc.contributorIndiana Univ Sch Med
dc.contributorUniversidade Federal de São Paulo (UNIFESP)
dc.contributorIndiana Univ
dc.creatorCosta, Rafael Pacheco da [UNIFESP]
dc.creatorHassan, Iraj
dc.creatorReginato, Rejane Daniele [UNIFESP]
dc.creatorDavis, Hannah M.
dc.creatorBruzzaniti, Angela
dc.creatorAllen, Matthew R.
dc.creatorPlotkin, Lilian I.
dc.date.accessioned2016-01-24T14:35:27Z
dc.date.accessioned2022-10-07T20:29:08Z
dc.date.available2016-01-24T14:35:27Z
dc.date.available2022-10-07T20:29:08Z
dc.date.created2016-01-24T14:35:27Z
dc.date.issued2014-03-21
dc.identifierJournal of Biological Chemistry. Bethesda: Amer Soc Biochemistry Molecular Biology Inc, v. 289, n. 12, p. 8508-8520, 2014.
dc.identifier0021-9258
dc.identifierhttp://repositorio.unifesp.br/handle/11600/37554
dc.identifier10.1074/jbc.M113.529735
dc.identifierWOS:000333157500042
dc.identifier.urihttp://repositorioslatinoamericanos.uchile.cl/handle/2250/4018653
dc.description.abstractBackground: Connexin proteins are essential for cell differentiation, function, and survival. Results: Global deletion of Cx37 results in increased bone mass caused by reduced osteoclast maturation. Conclusion: Our findings demonstrate a previously unrecognized role of Cx37 in bone homeostasis in vivo. Significance: Therapeutic approaches to increase bone mass might be developed by interfering with Cx37 function.Connexin (Cx) proteins are essential for cell differentiation, function, and survival in all tissues with Cx43 being the most studied in bone. We now report that Cx37, another member of the connexin family of proteins, is expressed in osteoclasts, osteoblasts, and osteocytes. Mice with global deletion of Cx37 (Cx37(-/-)) exhibit higher bone mineral density, cancellous bone volume, and mechanical strength compared with wild type littermates. Osteoclast number and surface are significantly lower in bone of Cx37(-/-) mice. in contrast, osteoblast number and surface and bone formation rate in bones from Cx37(-/-) mice are unchanged. Moreover, markers of osteoblast activity ex vivo and in vivo are similar to those of Cx37(+/+) littermates. sRANKL/M-CSF treatment of nonadherent Cx37(-/-) bone marrow cells rendered a 5-fold lower level of osteoclast differentiation compared with Cx37(+/+) cell cultures. Further, Cx37(-/-) osteoclasts are smaller and have fewer nuclei per cell. Expression of RANK, TRAP, cathepsin K, calcitonin receptor, matrix metalloproteinase 9, NFATc1, DC-STAMP, ATP6v0d1, and CD44, markers of osteoclast number, fusion, or activity, is lower in Cx37(-/-) osteoclasts compared with controls. in addition, nonadherent bone marrow cells from Cx37(-/-) mice exhibit higher levels of markers for osteoclast precursors, suggesting altered osteoclast differentiation. the reduction of osteoclast differentiation is associated with activation of Notch signaling. We conclude that Cx37 is required for osteoclast differentiation and fusion, and its absence leads to arrested osteoclast maturation and high bone mass in mice. These findings demonstrate a previously unrecognized role of Cx37 in bone homeostasis that is not compensated for by Cx43 in vivo.
dc.languageeng
dc.publisherAmer Soc Biochemistry Molecular Biology Inc
dc.relationJournal of Biological Chemistry
dc.rightsAcesso aberto
dc.subjectBone
dc.subjectGap Junctions
dc.subjectOsteoblasts
dc.subjectOsteoclast
dc.subjectOsteocyte
dc.subjectCx37
dc.titleHigh Bone Mass in Mice Lacking Cx37 Because of Defective Osteoclast Differentiation
dc.typeArtigo


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