Molecular and Cellular Biology
 2006
DOI: 10.1128/mcb.26.1.50-62.2006
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Transactivation of Platelet-Derived Growth Factor Receptor α by the GTPase-Deficient Activated Mutant of Gα12

Rashmi N. Kumar
1
,
Ji Hee Ha
2
,
R. Radhakrishnan
3
et al.

Abstract: Heterotrimeric G proteins regulate diverse cellular responses by coupling heptahelical receptors to intracellular effectors (11,25,35). Of the different ␣-subunits that have been analyzed thus far, the ␣-subunit of the heterotrimeric G protein G12 (G␣ 12 ) shows the most potent mitogenic and oncogenic activities (5, 35). The initial identification of G␣ 12 as the transforming oncogene in Ewing's sarcoma cell lines indicated the critical role of G␣ 12 in oncogenic signaling (5). Consistent with these observat… Show more

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Cited by 25 publications
(46 citation statements)
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References 44 publications
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“…Downstream signaling through Gα13/Rho has been associated with muscle hypertrophy in pressure-overloaded cardiac muscle (10), supporting the concept that Gα12/13 is a mechanosensitive anabolic pathway. Moreover, Gα12 signaling has been shown to activate the PI3K/Akt pathway in 3T3 cells (22), supporting our findings and confirming the Gα12/13 signaling as a regulatory pathway for mTOR. The loss of GPR56 could limit activation of Gα12/13 signaling during overload and prevent full activation of mTOR, similar to our observations in overloaded Gpr56-KO muscle (see model in Fig.…”
Section: Discussionsupporting
confidence: 89%

G protein-coupled receptor 56 regulates mechanical overload-induced muscle hypertrophy

White
1
,
Wrann
2
,
Rao
3
et al. 2014
Proc. Natl. Acad. Sci. U.S.A.
103
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100
0
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“…Downstream signaling through Gα13/Rho has been associated with muscle hypertrophy in pressure-overloaded cardiac muscle (10), supporting the concept that Gα12/13 is a mechanosensitive anabolic pathway. Moreover, Gα12 signaling has been shown to activate the PI3K/Akt pathway in 3T3 cells (22), supporting our findings and confirming the Gα12/13 signaling as a regulatory pathway for mTOR. The loss of GPR56 could limit activation of Gα12/13 signaling during overload and prevent full activation of mTOR, similar to our observations in overloaded Gpr56-KO muscle (see model in Fig.…”
Section: Discussionsupporting
confidence: 89%

G protein-coupled receptor 56 regulates mechanical overload-induced muscle hypertrophy

White
1
,
Wrann
2
,
Rao
3
et al. 2014
Proc. Natl. Acad. Sci. U.S.A.
103
0
100
0
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“…This would corroborate the idea that the PDGF-AA and PDGF-BB we detected in the bone marrow aspirates provide a negligible contribution to the activation of a-PDGFR in bone-metastatic prostate cells, and therefore confirm the concept of a-PDGFR transactivation. The neutralization of a-PDGFR in the absence of internalization would also exclude that additional isoforms of PDGF (i.e., PDGF-AB and PDGF-CC) could be present in the bone marrow aspirates and activate a-PDGFR in PC3-ML cells as well as rule out the possibility of an autocrine stimulation loop, which has previously been shown as a mechanism of a-PDGFR transactivation (19).…”
Section: Resultsmentioning
confidence: 99%

Human Bone Marrow Activates the Akt Pathway in Metastatic Prostate Cells through Transactivation of the α-Platelet–Derived Growth Factor Receptor

Dolloff
1
,
Russell2,
Loizos3
et al. 2007
Cancer Research
37
3
37
0
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“…Our results indicate that LPA specifically stimulates the proliferation of ovarian cancer cell lines but not the nonmalignant IOSE or HOSE cell lines. Such LPA-mediated proliferation of ovarian cancer cells is inhibited by the expression of a competitively inhibitory minigene of Gα 12 that is known to disrupt receptor-Gα gep proto-oncogene family, 7 in transmitting LPA-mediated proliferation signals to ovarian cancer cells. Thus, our studies establish for the first time an unequivocal role for LPA and Gα 12 signaling axis in ovarian cancer cell proliferation.…”
Section: Introductionmentioning
confidence: 99%

Lysophosphatidic Acid Stimulates the Proliferation of Ovarian Cancer Cells via the gep Proto-Oncogene G 12

Goldsmith
1
,
Ha2,
Jayaraman
3
et al. 2011
Genes & Cancer
38
8
59
0
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