biostudies-literature00650Kumar ANIA NIH HHS254-63https://www.ebi.ac.uk/biostudies/studies/S-EPMC3249674biostudies-literatureUnknown153(1)In the bone marrow cavity, adipocyte numbers increase, whereas osteoblast progenitor numbers decrease with aging. Because adipocytes and osteoblasts share a common progenitor, it is possible that this shift is due to an increase in adipocyte-lineage cells at the expense of osteoblast-lineage commitment. Estrogens inhibit adipocyte differentiation, and in both men and women, circulating estrogens correlate with bone loss with aging. In bone cells, estrogens stimulate expression of TGF-? and suppress mesenchymal cell adipogenesis. Using a tripotential mesenchymal cell line, we have examined whether estradiol suppression of adipocyte differentiation is due to stimulation of TGF-? and the mechanism by which TGF-? suppresses adipogenesis. We observed that estradiol-mediated suppression of adipogenic gene expression required at least 48 h treatment. TGF-? expression increased within 24 h of estradiol treatment, and TGF-? inhibition reversed estradiol influences on adipogenesis and adipocyte gene expression. Connective tissue growth factor (CTGF) mediates TGF-? suppression of adipogenesis in mouse 3T3-L1 cells. CTGF expression was induced within 24 h of TGF-? treatment, whereas estradiol-mediated induction required 48 h treatment. Moreover, estradiol-mediated induction of CTGF was abrogated by TGF-? inhibition. These data support that estradiol effects on adipogenesis involves TGF-? induction, which then induces CTGF to suppress adipogenesis.EndocrinologyTGF-? mediates suppression of adipogenesis by estradiol through connective tissue growth factor induction.PMC3249674R01 AG028936P01 AG004875Syed FClifton KRuan MKhosla SOursler MJKumar A65falseTGF-? mediates suppression of adipogenesis by estradiol through connective tissue growth factor induction.In the bone marrow cavity, adipocyte numbers increase, whereas osteoblast progenitor numbers decrease with aging. Because adipocytes and osteoblasts share a common progenitor, it is possible that this shift is due to an increase in adipocyte-lineage cells at the expense of osteoblast-lineage commitment. Estrogens inhibit adipocyte differentiation, and in both men and women, circulating estrogens correlate with bone loss with aging. In bone cells, estrogens stimulate expression of TGF-? and suppress mesenchymal cell adipogenesis. Using a tripotential mesenchymal cell line, we have examined whether estradiol suppression of adipocyte differentiation is due to stimulation of TGF-? and the mechanism by which TGF-? suppresses adipogenesis. We observed that estradiol-mediated suppression of adipogenic gene expression required at least 48 h treatment. TGF-? expression increased within 24 h of estradiol treatment, and TGF-? inhibition reversed estradiol influences on adipogenesis and adipocyte gene expression. Connective tissue growth factor (CTGF) mediates TGF-? suppression of adipogenesis in mouse 3T3-L1 cells. CTGF expression was induced within 24 h of TGF-? treatment, whereas estradiol-mediated induction required 48 h treatment. Moreover, estradiol-mediated induction of CTGF was abrogated by TGF-? inhibition. These data support that estradiol effects on adipogenesis involves TGF-? induction, which then induces CTGF to suppress adipogenesis.2012-01-01T00:00:00Z2012 Jan2020-10-01T07:21:04Z2019-03-27T00:47:33ZS-EPMC32496742206731410.1210/en.2011-1169