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1 Department of Orthopaedics, 2 Department of Pathology, and 3 Department of Physiology and Biophysics, Case Western Reserve University and University Hospitals of Cleveland, Cleveland, Ohio 44106-5000
Conditionally immortalized
murine calvarial (CIMC) cells that support differentiation of
precursors into mature osteoclasts were isolated. All six CIMC cell
lines supported osteoclast differentiation in response to
1,25-dihydroxyvitamin D3 or interleukin (IL)-11. CIMC-4
cells also supported osteoclast differentiation in response to tumor
necrosis factor (TNF)-
, IL-1
, or IL-6. The resultant multinucleated cells expressed tartrate-resistant acid phosphatase and
formed resorption lacunae on mineralized surfaces. CIMC-4 cells,
therefore, establish an osteoclast differentiation assay that is
responsive to many cytokines and does not rely on isolation of primary
stromal support cells. Low concentrations of the cytokines synergistically stimulated differentiation when osteoclast precursors were cocultured with either CIMC-4 cells or primary calvarial cells.
Osteoclast differentiation induced by all stimuli other than
TNF-
was completely blocked by osteoprotegerin, whether the
stimulators were examined alone or in combination. Moreover, study of
precursors that lack TNF-
receptors showed that TNF-
induces
osteoclast differentiation primarily through direct actions on
osteoclast precursors, which is a distinct mechanism from that used by
the other bone-resorptive agents examined in this study.
conditionally immortalized murine calvarial (CIMC-4) cells; cytokines; osteoclast differentiation; RANKL; tumor necrosis factor-
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