Your search keyword '"Frediani, Uliana"' showing total 3 results

1. Bone endothelial cells as estrogen targets

Author

Brandi, Maria Luisa, Crescioli, Clara, Tanini, Annalisa, Frediani, Uliana, Agnusdei, Donato, and Gennari, Carlo

Abstract

Summary In the present study, we investigated the effects of estrogens on bone endothelial cell metabolism and the presence of estrogen binding sites in the same cells. For these studies, we have used a continuous cell line of clonal bovine bone endothelial cells for evidence of a direct response to estrogensin vitro. Receptor analysis to intact viable cells was steroid specific and saturable, with an apparent dissociation constant of 17.2 nM and a Bmax of 3.2 × 104 sites/cell. Northern blot analysis revealed a 6.5-kilobase mRNA that hybridized with a cDNA to human estrogen receptor. The 6.5-kilobase size is in close agreement with the reported size of the human estrogen receptor mRNA.In vitro estrogen responses of bone endothelial cells included a stimulation of cell proliferation as well as an inhibition of parathyroid hormone responsiveness. These findings clearly demonstrate the presence of functional estrogen receptors in bone endothelial cellsin vitro, suggesting a role of estrogens in bone angiogenesis and in the entire process of bone remodeling.

Published

1993

2. Heterogeneity of Binding Sites and Bioeffects of Raloxifene on the Human Leukemic Cell Line FLG 29.1

Author

Fiorelli, Gianna, Martineti, Valentina, Gori, Francesca, Benvenuti, Susanna, Frediani, Uliana, Formigli, Lucia, Zecchi, Sandra, and Brandi, Maria Luisa

Abstract

The benzothiophene divarative raloxifene is known to mimic estrogen in human bone remodeling. To investigate the “in vitro” properties of raloxifene on osteoclast precursors, the human leukemic cell line FLG 29.1, which differentiates toward the osteoclastic phenotype, was examined for raloxifene binding and for evidence of its bioeffects. Scatchard and Hill analysis of binding data with the tritiated raloxifene demonstrated the presence of two classes of binding sites in both nuclear and cytosol fractions with Kd values of ∼ 1 nM and ∼ 5 nM, respectively. In addition, analysis of binding data using tritiated 17βE2as ligand at high concentrations (10 - 40 nM) and either unlabeled 17βE2or raloxifene as competitors gave similar results demonstrating the presence of type II EBS in these cells. Picomolar concentrations of raloxifene significantly (p<0.05) inhibited cell proliferation. Moreover, the compound at nanomolar concentrations induced a significant dose- and time-dependent increase of progesterone receptor, and activated apoptotic cell death. These findings clearly demonstrate that raloxifene acts as an estrogen agonist in FLG 29.1 cells, acting through the estrogen receptor and, possibly, via multiple cooperative binding component(s).

Published

1997

3. Effects of ipriflavone and its metabolites on a clonal osteoblastic cell line

Author

Benvenuti, Susanna, Tanini, Annalisa, Frediani, Uliana, Bianchi, Sandro, Masi, Laura, Casano, Rosaria, Bufalino, Lidia, Serio, Mario, and Dr. Brandi, Maria Luisa

Abstract

Protective effects of ipriflavone, an isoflavone derivative, in osteoporosis are believed to be caused by the inhibitory action on bone resorption. A direct effect of ipriflavone on bone formation is as yet unknown. Ipriflavone and four of its metabolites (I, II, III, and V) were examined for their effects on parathyroid hormone response, collagen synthesis, alkaline phosphatase activity, and cell proliferation in a clonal cell population of rat osteoblastic cells. Pretreatment of osteoblasts with high concentrations of ipriflavone for 48 h significantly inhibited the cAMP response to parathyroid hormone, producing a shift in the dose‐response curve; at lower concentrations metabolites II and III potentiated the cAMP accumulation induced by low doses of parathyroid hormone. The 48 h treatment with metabolite V at the 1 nM dose significantly stimulated collagen synthesis in osteoblastic cells. Ipriflavone and metabolite I showed a biphasic stimulatory action on the alkaline phosphatase activity of osteoblasts, with a maximal effect at the 0.1 and 1 nM doses, respectively. A similar biphasic response was observed with ipriflavone and metabolite I on osteoblastic cell growth, with a maximal effect at the 0.1 nM concentration. These results suggest a direct role of ipriflavone in modulating the synthetic and growth properties of osteoblast‐like cells.

Published

1991