TGFβ alters growth and differentiation related gene expression in proliferating osteoblasts in vitro, preventing development of the mature bone phenotype

Breen, Ellen C.; Ignotz, Ronald A.; McCabe, Laura R.; Stein, Janet L.; Stein, Gary S.; Lian, Jane B.

doi:10.1002/jcp.1041600214

Cited by 129 publications

(100 citation statements)

References 69 publications

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“…This pattern, similar to AP activity, may be the response of PLA cell subpopulations at distinct developmental stages to osteogenic induction. In support of this, several other induction agents have been shown to stage-specific effects on osteogenesis, including TGF␤ (Breen et al, 1994). Finally, OC expression by induced PLA cells was dependent upon osteogenic agent as OC expression was inhibited upon dexamethasone exposure, an effect not observed in MSC controls.…”

Section: Osteogenesismentioning

confidence: 74%

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Zuk

Zhu

Ashjian

et al. 2002

MBoC

5,915

144

4,635

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Much of the work conducted on adult stem cells has focused on mesenchymal stem cells (MSCs) found within the bone marrow stroma. Adipose tissue, like bone marrow, is derived from the embryonic mesenchyme and contains a stroma that is easily isolated. Preliminary studies have recently identified a putative stem cell population within the adipose stromal compartment. This cell population, termed processed lipoaspirate (PLA) cells, can be isolated from human lipoaspirates and, like MSCs, differentiate toward the osteogenic, adipogenic, myogenic, and chondrogenic lineages. To confirm whether adipose tissue contains stem cells, the PLA population and multiple clonal isolates were analyzed using several molecular and biochemical approaches. PLA cells expressed multiple CD marker antigens similar to those observed on MSCs. Mesodermal lineage induction of PLA cells and clones resulted in the expression of multiple lineage-specific genes and proteins. Furthermore, biochemical analysis also confirmed lineage-specific activity. In addition to mesodermal capacity, PLA cells and clones differentiated into putative neurogenic cells, exhibiting a neuronal-like morphology and expressing several proteins consistent with the neuronal phenotype. Finally, PLA cells exhibited unique characteristics distinct from those seen in MSCs, including differences in CD marker profile and gene expression.

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Section: Osteogenesismentioning

confidence: 74%

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Zuk

Zhu

Ashjian

et al. 2002

MBoC

5,915

144

4,635

View full text Add to dashboard Cite

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“…The resulting dimers can bind to DNA at a consensus AP1 binding site termed the TPA response element (TRE), thereby transactivating the expression of AP1-responsive genes (St-Arnaud and Quelo, 1998). Experiments where fos and jun expression in the bone was modulated by steroid hormone treatment or by overexpression or ablation of fos or jun genes suggest that the Fos and Jun proteins are important in the regulation of bone formation (Clohisy et al, 1992;Breen et al, 1994). This suggestion is supported by a study by McCabe et al (1996), who showed that the developmental expression and activity of particular Fos and Jun proteins are functionally related to osteoblast maturation.…”

Section: Introductionmentioning

confidence: 99%

Erk pathway and activator protein 1 play crucial roles in FGF2‐stimulated premature cranial suture closure

Kim

Lee

Park

et al. 2003

Developmental Dynamics

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Cranial sutures are an important growth center of the cranial bones, and the suture space must be maintained to permit the cranial adjustments needed to accommodate brain growth. Craniosynostosis, characterized by premature suture closure, mainly results from mutations that generate constitutively active fibroblast growth factor (FGF) receptors. FGF signaling, thus, is responsible for the pathogenesis of craniosynostosis. Even though FGF activates many different signaling pathways, the one involved in premature suture closure has not been defined. We observed that placing FGF2-soaked bead on the osteogenic fronts of cultured mouse calvaria accelerates cranial suture closure and strongly induces the expression of osteopontin, an early marker of differentiated osteoblasts. FGF2 treatment also induced fos and jun mRNAs and later increased the nuclear levels of activator protein 1 (AP1).

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“…It is becoming clear that the TGF-fl supergene family plays an instrumental role for the osteoblastic cell lineage to display its full catalogue of phenotypic characteristics during osteogenesis. In various experimental systems for studying bone formation, contradictory results have been obtained on whether TGF-fll enhances or inhibits bone matrix formation, mineralization and the expression of bone marker proteins [4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22]. This has in part been explained by differences in the source and type of cells, stage of osteoblastic maturation, culture conditions and presence of other cytokines and their receptors.…”

Section: K Iba Et Al/febs Letters 373 (1995) 1~1mentioning

confidence: 99%

“…Based on all these in vitro and in vivo studies, several authors suggested that, while TGF-fll initiates the proliferation, differentiation and extracellular matrix synthesis of bone cells, TGF-fll may be less involved in or actually inhibit the later phases of osteogenesis, i.e. mineralization [17,20,21]. The biological responses to TGF-fl may be mediated by the retinoblastoma gene product [38], which binds to the SV-40 T antigen, and therefore the effect of T antigen expression by the SV-HFO cells on the TGF-fll signal transduction pathway will require further analysis.…”

Section: K Iba Et Al/febs Letters 373 (1995) 1~1mentioning

confidence: 99%

“…Bone is an abundant source of TGFofll [1,2] and in vivo studies have shown that TGF-fll is a local regulator of bone formation. In osteoblast cell culture systems, TGF-fll regulates the mineralization process and the expression of osteoblastic markers, including alkaline phosphatase, c~1 (I) procollagen, osteopontin, osteonectin and osteocalcin [4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22].…”

Section: Introductionmentioning

confidence: 99%

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Transforming growth factor‐β₁ downregulates dexamethasone‐indunced tetranectin gene expression during the in vitro mineralization of the human osteoblastic cell line SV‐HFO

et al. 1995

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In the present study, we examined the regulation of tetranectin gene expression using a human osteoblastic cell line, SV-HFO, that undergoes mineralization upon treatment with dexamethasone. We found that the expression of tetranectin and alkaline phosphatase mRNA was induced by dexamethasone treatment as evidenced by Northern blotting. When transforming growth factor-/] 1 (TGF-/] 0 was added together with dexamethasone to the SV-HFO cell cultures, the mineralization process was markedly suppressed and the expression of tetra nectin and alkaline phosphatase was downregulated in a dosedependent manner. These results demonstrate that the expression of tetranectin in these osteoblastic cells is regulated by dexamethasone and TGF-/] 1 and that tetranectin expression is tightly linked to the process of mineralization.of both alkaline phosphatase and osteocalcin [24]. More recently, we have shown that the cells undergo mineralization upon treatment with glucocorticoids [25]. In the present study, we used this human osteoblastic in vitro model system to begin analysing the regulation of tetranectin gene expression during mineralization. Tetranectin is a protein originally isolated from plasma [26] that was found to be expressed in bone at a time and space coincident with mineralization in vivo and in vitro [27]. We report that dexamethasone treatment induced the expression of tetranectin mRNA and that TGF-fl~ inhibited mineralization and the induction of tetranectin mRNA. Materials and methods

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TGFβ alters growth and differentiation related gene expression in proliferating osteoblasts in vitro, preventing development of the mature bone phenotype

Cited by 129 publications

References 69 publications

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Erk pathway and activator protein 1 play crucial roles in FGF2‐stimulated premature cranial suture closure

Transforming growth factor‐β₁ downregulates dexamethasone‐indunced tetranectin gene expression during the in vitro mineralization of the human osteoblastic cell line SV‐HFO

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TGFβ alters growth and differentiation related gene expression in proliferating osteoblasts in vitro, preventing development of the mature bone phenotype

Cited by 129 publications

References 69 publications

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Human Adipose Tissue Is a Source of Multipotent Stem Cells

Erk pathway and activator protein 1 play crucial roles in FGF2‐stimulated premature cranial suture closure

Transforming growth factor‐β1 downregulates dexamethasone‐indunced tetranectin gene expression during the in vitro mineralization of the human osteoblastic cell line SV‐HFO

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Transforming growth factor‐β₁ downregulates dexamethasone‐indunced tetranectin gene expression during the in vitro mineralization of the human osteoblastic cell line SV‐HFO