1. v-ATPase V0 subunit d2-deficient mice exhibit impaired osteoclast fusion and increased bone formation
- Author
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Ju Seob Kang, Nacksung Kim, Toshio Suda, Daewon Jeong, Seoung Hoon Lee, Takeshi Miyamoto, Jai Yoon Sul, Joseph A. Lorenzo, Sun-Kyeong Lee, Robert J. Pignolo, Boguslawa Koczon-Jaremko, Taesoo Kim, Yongwon Choi, and Jaerang Rho
- Subjects
musculoskeletal diseases ,Vacuolar Proton-Translocating ATPases ,Myeloid ,Osteoclasts ,Osteoclast fusion ,Biology ,General Biochemistry, Genetics and Molecular Biology ,Bone resorption ,Osteoclast maturation ,Cell Fusion ,Mice ,Multinucleate ,Osteogenesis ,medicine ,V-ATPase ,Animals ,Humans ,Protein Isoforms ,Cells, Cultured ,Mice, Knockout ,Cell fusion ,Macrophage Colony-Stimulating Factor ,RANK Ligand ,Cell Differentiation ,General Medicine ,Proton Pumps ,Cell biology ,Protein Structure, Tertiary ,Mice, Inbred C57BL ,Haematopoiesis ,medicine.anatomical_structure ,Immunology - Abstract
Matrix-producing osteoblasts and bone-resorbing osteoclasts maintain bone homeostasis. Osteoclasts are multinucleated, giant cells of hematopoietic origin formed by the fusion of mononuclear pre-osteoclasts derived from myeloid cells. Fusion-mediated giant cell formation is critical for osteoclast maturation; without it, bone resorption is inefficient. To understand how osteoclasts differ from other myeloid lineage cells, we previously compared global mRNA expression patterns in these cells and identified genes of unknown function predominantly expressed in osteoclasts, one of which is the d2 isoform of vacuolar (H(+)) ATPase (v-ATPase) V(0) domain (Atp6v0d2). Here we show that inactivation of Atp6v0d2 in mice results in markedly increased bone mass due to defective osteoclasts and enhanced bone formation. Atp6v0d2 deficiency did not affect differentiation or the v-ATPase activity of osteoclasts. Rather, Atp6v0d2 was required for efficient pre-osteoclast fusion. Increased bone formation was probably due to osteoblast-extrinsic factors, as Atp6v02 was not expressed in osteoblasts and their differentiation ex vivo was not altered in the absence of Atp6v02. Our results identify Atp6v0d2 as a regulator of osteoclast fusion and bone formation, and provide genetic data showing that it is possible to simultaneously inhibit osteoclast maturation and stimulate bone formation by therapeutically targeting the function of a single gene.
- Published
- 2006