CD735’-ecto-nucleotidase acts as a regulatory factor in osteo-chondrogenic differentiation of mechanically stimulated mesenchym.docx
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1、A Ode et al.CD73 controls differentiation ofMSCsEuropean A Ode et Cells”/, and Materials Vol. 25 2013 (pages37-47)CD735,-ECTO-NUCLEOTIDASE ACTS AS A REGULATORY FACTOR INOSTEO-CHONDROGENIC DIFFERENTIATION OF MECHANICALLYSTIMULATED MESENCHYMAL STROMAL CELLSAndrea Ode *, Janosch Schoon , nnctt Kurtz ,
2、Marcel Gactjcn , Jan E. Ode , Sven Geissler , Georg N. Duda1.21,2111L21.2,Julius Wolff Institute and Musculoskeletal Research Center Berlin, Charitc-Univcrsitatsmcdzin, Berlin, Germany2 Berlin-Brandenburg Center fbr Regenerative Therapies, Berlin, GermanyAbstractIntroduction38www.ecnjournaLorgBone r
3、egeneration is influenced by mesenchymal stromalcells (MSCs) and mechanical conditions. How healingoutcome and mechanical stability arc linked on the cellularlevel, however, remains elusive. Cyclic-comprcssivcloading of MSCs accts the expression of moleculesinvolved in angiogenesis and matrix assemb
4、ly, but alsoreduces the expression of CD73, an ccto-5-nucleotidase,which plays a crucial role in extracellular adenosinegeneration. Although, fbr almost 20 years, CD73 has beena major cell surface marker defining MSCs, little is knownabout its function in these cells. Therefore, the aim of thisstudy
5、 was to determine the putative involvement of CD73in MSC differentiation after cyclic-comprcssivc loading.After cultivation in appropriate differentiation media,chondrogcnic differentiation ability was significantlyincreased in loaded MSCs, hence following current models.Through treatment with the C
6、D73 inhibitor adenosine5-(, -methylene) diphosphate, chondrogenic matrixdeposition was further increased; in contrast, mineralmatrix deposition and expression of osteogenic markers wasreduced. One major signal transduction pathway, which isactivated via CD73-mcdiatcd adenosine, is the adenosinerecep
7、tor pathway. Thus, the adenosine receptor expressionpattern was investigated. MSCs expressed the four knownadenosine receptors at the mRNA level. After mechanicalstimulation ofMSCs, Adora2a was down-regulated. Thesedata point towards a role of CD73 in MSC differentiationpossibly vA2R signalling, whi
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