The small GTP-binding protein Rho links G protein-coupled receptors and Gα
            <sub>12</sub>
            to the serum response element and to cellular transformation

Fromm, C; Coso, Omar A.; Montaner, Silvia; Xu, Ningzhi; Gutkind, J. Silvio

doi:10.1073/pnas.94.19.10098

Cited by 208 publications

(252 citation statements)

References 41 publications

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“…Right panel: C3 transferase functions in Ishikawa cells to inhibit activation of the serum response element (SRE) reporter by RhoA, but not by Cdc42Hs. Transfections were performed with constituitively activating mutants, RhoQL (400 ng) and Cdc42QL (400 ng) (Coso et al, 1995) and SRE-luciferase reporter (1 mg) in the presence (+) or 100 ng pCEV-C3 transferase (C3) (Fromm et al, 1997). pCEV-0 at 100 ng was used as a control (7).…”

Section: Discussionmentioning

confidence: 99%

“…Control expression vector (pCEV-0) was added to give a total of 500 ng of plasmid per well. pCEV-C3 transferase expression plasmid was prepared as described in Fromm et al, 1997. Ishikawa cells were stably transfected with either a FLAG epitope-tagged Brx expression plasmid, or control plasmid encoding Neomycin resistance (pBK-RSV).…”

Section: Cell Culture and Transient Transfectionmentioning

confidence: 99%

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Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

et al. 1998

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Regulation of gene activation by the estrogen receptor (ER) is complex and involves co-regulatory proteins, oncoproteins (such as Fos and Jun), and phosphorylation signaling pathways. Here we report the cloning and initial characterization of a novel protein, Brx, that contains a region of identity to the oncogenic Rhoguanine nucleotide exchange (Rho-GEF) protein Lbc, and a unique region capable of binding to nuclear hormone receptors, including the ER. Western and immunohistochemistry studies showed Brx to be expressed in estrogen-responsive reproductive tissues, including breast ductal epithelium. Brx bound speci®cally to the ER via an interaction that required distinct regions of ER and Brx. Furthermore, overexpression of Brx in transfection experiments using an estrogenresponsive reporter revealed that Brx augmented gene activation by the ER in an element-speci®c and liganddependent manner. Moreover, activation of ER by Brx could be speci®cally inhibited by a dominant-negative mutant of Cdc42Hs, but not by dominant negative mutants of RhoA or Rac1. Taken together, these data suggest that Brx represents a novel modular protein that may integrate cytoplasmic signaling pathways involving Rho family GTPases and nuclear hormone receptors.

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Section: Discussionmentioning

confidence: 99%

Section: Cell Culture and Transient Transfectionmentioning

confidence: 99%

Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

et al. 1998

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“…Furthermore, the expression of the Ga 12 QL has been shown to stimulate DNA synthesis in several other cell-types such as 1321N1 astrocytoma cells (Aragay et al, 1995). Studies from several laboratories including ours have shown that the proliferative pathway regulated by Ga 12 includes the Ras/Rac mediated activation of JNKs (Vara Prasad et al, 1995;Collins et al, 1996;Voyno-Yasenetskaya et al, 1996), Rho-dependent activation of cytoskeletal changes (Buhl et al, 1995;Hooley et al, 1996;Needham and Rozengurt, 1998), Rho-dependent activation of speci®c transcription factors (Fromm et al, 1997), Rac/MEKK1-mediated activation of AP-1 complex (Collins et al, 1996), and Ras/Rac/Rhodependent cell transformation (Zhang et al, 1996;Tolkacheva et al, 1997;Fromm et al, 1997). In addition, it has been shown that serum-induced phospholipase A 2 (PLA 2 ) activity was potentiated by Ga 12 QL in NIH3T3 cells, suggesting a role for eicosanoids in Ga 12 QL signaling (Xu et al, 1993).…”

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confidence: 87%

Oncogenic mutant of Gα12 stimulates cell proliferation through cycloxygenase-2 signaling pathway

et al. 1999

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Expression of the GTPase-de®cient, activated mutant asubunit of the heterotrimeric G protein G12 (Ga 12 QL) leads to the neoplastic transformation of ®broblast cell lines. The mitogenic pathway regulated by Ga 12 QL includes an extensive signaling network involving several small GTPases and various kinases. In addition, Ga 12 QL has been shown to potentiate the serum-induced phospholipase-A 2 activity in NIH3T3 cells. In the present study, we demonstrate that cycloxygenase-2 (COX-2) pathway is involved in the mitogenic pathway activated by Ga 12 QL. Expression of Ga 12 QL and not Ga 13 QL, stimulates the serum-induced release of arachidonic acid in NIH3T3 cells. Furthermore, expression of Ga 12 QL or the stimulation of wild-type Ga 12 induces the expression of COX-2. Our results also indicate that the COX-2 inhibitor acutely disrupts the DNA-synthesis stimulated by Ga 12 QL in NIH3T3 cells. These studies, for the ®rst time, identify the crucial role of COX-2 in Ga 12 -mediated regulation of cell proliferation and suggest a role for prostaglandin-derived autocrine loop in Ga 12 -mediated signaling pathways.

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“…NIH3T3 cells transformed with Ga 12 QL or Ga 13 QL indicated that conventional secondary messenger pathways involving cAMP, Ca 2+ , or IP 3 were not altered in these cells (Chan et al, 1993;Xu et al, 1993;Jiang et al, 1993Vara Prasad et al, 1994;VoynaYasenetskaya et al, 1994). However, speci®c sets of primary respose genes appear to be activated in Ga 12 QL-and Ga 13 QL-transformed NIH3T3 cells (Fromm et al, 1997;Vara Prasad et al, 1994). Ga 12 QL has been shown to activate SRFs through a Rho-dependent pathway (Fromm et al, 1997).…”

Section: Ga 12/13 : the Gep Oncogenes?mentioning

confidence: 99%

“…However, speci®c sets of primary respose genes appear to be activated in Ga 12 QL-and Ga 13 QL-transformed NIH3T3 cells (Fromm et al, 1997;Vara Prasad et al, 1994). Ga 12 QL has been shown to activate SRFs through a Rho-dependent pathway (Fromm et al, 1997). Ga 13 QL has been shown to activate the transcription of Egr-1 a primary response gene implicated in cell proliferation as well as di erentiation .…”

Section: Ga 12/13 : the Gep Oncogenes?mentioning

confidence: 99%

Regulation of cell proliferation by G proteins

Dhanasekaran

Tsim²,

Dermott³

et al. 1998

Oncogene

136

107

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G Proteins provide signal transduction mechanisms to seven transmembrane receptors. Recent studies have indicated that the a-subunits as well as the bg-subunits of these proteins regulate several critical signaling pathways involved in cell proliferation, di erentiation and apoptosis. Of the 17 a-subunits that have been cloned, at least ten of them have been shown to couple mitogenic signaling in ®broblast cells. Activating mutations in Ga s , Ga i2 , and Ga 12 have been correlated with di erent types of tumors. In addition, the ability of the bg-subunits to activate mitogenic pathways in di erent cell-types has been de®ned. The present review brie¯y summarizes the diverse and novel signaling pathways regulated by the a-as well as the bg-subunits of G proteins in regulating cell proliferation.

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The small GTP-binding protein Rho links G protein-coupled receptors and Gα ₁₂ to the serum response element and to cellular transformation

Cited by 208 publications

References 41 publications

Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

Oncogenic mutant of Gα12 stimulates cell proliferation through cycloxygenase-2 signaling pathway

Regulation of cell proliferation by G proteins

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The small GTP-binding protein Rho links G protein-coupled receptors and Gα 12 to the serum response element and to cellular transformation

Cited by 208 publications

References 41 publications

Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

Characterization of Brx, a novel Dbl family member that modulates estrogen receptor action

Oncogenic mutant of Gα12 stimulates cell proliferation through cycloxygenase-2 signaling pathway

Regulation of cell proliferation by G proteins

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The small GTP-binding protein Rho links G protein-coupled receptors and Gα ₁₂ to the serum response element and to cellular transformation