c-Fos: a Key Regulator of Osteoclast-Macrophage Lineage Determination and Bone Remodeling

Agamemnon E. Grigoriadis; Zhao‐Qi Wang; Marco Cecchini; Willy Hofstetter; R. Felix; H. Fleisch; Erwin F. Wagner

doi:10.1126/science.7939685

c-Fos: a Key Regulator of Osteoclast-Macrophage Lineage Determination and Bone Remodeling

Agamemnon E. Grigoriadis(Research Institute of Molecular Pathology), Zhao‐Qi Wang(Research Institute of Molecular Pathology), Marco Cecchini(Ion Beam Applications (France)), Willy Hofstetter(Ion Beam Applications (France)), R. Felix(Ion Beam Applications (France)), H. Fleisch(Ion Beam Applications (France)), Erwin F. Wagner(Research Institute of Molecular Pathology)

Science

October 21, 1994

10.1126/science.7939685

Cited by 1,282

Abstract

Mice lacking the proto-oncogene c-fos develop the bone disease osteopetrosis. Fos mutant mice were found to have a block in the differentiation of bone-resorbing osteoclasts that was intrinsic to hematopoietic cells. Bone marrow transplantation rescued the osteopetrosis, and ectopic c-fos expression overcame this differentiation block. The lack of Fos also caused a lineage shift between osteoclasts and macrophages that resulted in increased numbers of bone marrow macrophages. These results identify Fos as a key regulator of osteoclast-macrophage lineage determination in vivo and provide insights into the molecular mechanisms underlying metabolic bone diseases.

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