Bone morphogenetic protein-3 is a negative regulator of bone density

Daluiski, Aaron; Engstrand, Thomas; Bahamonde, ME; Gamer, LW; Agius, Eric; Stevenson, SL; Cox, Karen; Rosen,; Lyons, KM

doi:10.1038/83810

Cited by 378 publications

(279 citation statements)

References 29 publications

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“…Key genes for the regulation of embryonic organogenesis (Hoxa5, Hoxa9, Foxc1 and Foxf2) and the commitment of immature cells to multiple lineages (Pparg, Cebpa, Plxnd1, Egfl7, Mgp, Plxdc2, Ebf1 and Tcf3) were expressed at higher levels in AO cells than in AX cells, suggesting that AO cells have characteristics of immature mesenchymal cells (Wang and Reed, 1993;Luo et al, 1997;Wu et al, 1999;Rosen et al, 2000;Parker et al, 2004;Torres-Vazquez et al, 2004;Miller et al, 2007;Cole et al, 2008). The profile of AX cells, on the other hand, was indicative of both cells that are committed to the osteocyte lineage (Dlx3, Sp7, Dkk1, Ostn and Bmp3) and cells that are inclined to tumorigenesis in vivo (Cd276, Ptgs2, Vegfa, Epha2, Frzb and Sfrp1) (Kim et al, 1993;Daluiski et al, 2001;Dannenberg et al, 2001;Thomas et al, 2003;Lee et al, 2004 Zang et al, 2007;Brantley-Sieders et al, 2008;Engin et al, 2008;Li et al, 2008).…”

Section: Ao and Ax Cells Differ In Their Gene Expression Profilesmentioning

confidence: 98%

c-MYC overexpression with loss of Ink4a/Arf transforms bone marrow stromal cells into osteosarcoma accompanied by loss of adipogenesis

et al. 2010

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The development of cancer is due to the growth and proliferation of transformed normal cells. Recent evidence suggests that the nature of oncogenic stress and the state of the cell of origin critically affect both tumorigenic activity and tumor histological type. However, this mechanistic relationship in mesenchymal tumors is currently largely unexplored. To clarify these issues, we established a mouse osteosarcoma (OS) model through overexpression of c-MYC in bone marrow stromal cells (BMSCs) derived from Ink4a/Arf (À/À) mice. Single-cell cloning revealed that c-MYC-expressing BMSCs are composed of two distinctly different clones: highly tumorigenic cells, similar to bipotent-committed osteochondral progenitor cells, and low-tumorigenic tripotent cells, similar to mesenchymal stem cells (MSCs). It is noteworthy that both bipotent and tripotent cells were capable of generating histologically similar, lethal OS, suggesting that both committed progenitor cells and MSCs can become OS cells of origin. Shifting mesenchymal differentiation by depleting PPARc in tripotent MSC-like cells and overexpressing PPARc in bipotent cells affected cell proliferation and tumorigenic activity. Our findings indicate that differentiation potential has a key role in OS tumorigenic activity, and that the suppression of adipogenic ability is a critical factor for the development of OS.

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Section: Ao and Ax Cells Differ In Their Gene Expression Profilesmentioning

confidence: 98%

c-MYC overexpression with loss of Ink4a/Arf transforms bone marrow stromal cells into osteosarcoma accompanied by loss of adipogenesis

et al. 2010

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“…Similarly Bmp4 CKO mice (Col1-Cre mice were used) also showed defects in bone development and postnatal bone formation (Guo et al, 2004). In contrast, Bmp3 KO mice show increased bone mass, suggesting that endogenous BMP3 antagonizes BMP signaling in vivo (Daluiski et al, 2001). Bmp6-deficient mice are viable and fertile and show no overt defects in tissues known to express Bmp6 mRNA (Solloway et al, 1998).…”

Section: Knockout Of Bmp Bmpr and Smad Genesmentioning

confidence: 99%

The BMP signaling and in vivo bone formation

Cao

Chen

2005

Gene

268

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Bone morphogenetic proteins (BMPs) are multi-functional growth factors that belong to the transforming growth factor β(TGFβ) superfamily. The roles of BMPs in embryonic development and cellular functions in postnatal and adult animals have been extensively studied in recent years. Signal transduction studies have revealed that Smads 1, 5 and 8 are the immediate downstream molecules of BMP receptors and play a central role in BMP signal transduction. Studies from transgenic and knockout mice and from animals and humans with naturally occurring mutations in BMPs and their signaling molecules have shown that BMP signaling plays critical roles in bone and cartilage development and postnatal bone formation. BMP activities are regulated at different molecular levels. Tissue-specific knockout of a specific BMP ligand, a subtype of BMP receptors or a specific signaling molecule is required to further determine the specific role of a BMP ligand, receptor or signaling molecule in a particular tissue.

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“…Most of the BMPs are expressed in skeletal tissue, and many are detectable in osteoblasts as well (Anderson et al, 2000). While the majority are recognized for promotion of bone formation, BMP-3, for example, is a negative regulator of bone formation (Daluiski et al, 2001). Transforming growth factor-/S (TGF-/3) is a major player in bone biology, directly inducing effects in both osteoclasts and osteoblasts.…”

Section: Systemic and Local Factors Affecting Bone Remodelingmentioning

confidence: 99%