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Science 1 June 2001: Vol. 292. no. 5522, pp. 1718 - 1722 DOI: 10.1126/science.1060100
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Reports
G Protein Signaling from Activated Rat Frizzled-1 to the -Catenin-Lef-Tcf Pathway
Tong Liu,1
Anthony J. DeCostanzo,1
Xunxian Liu,1
Hsien-yu Wang,2
Sarah Hallagan,3
Randall T. Moon,3
Craig C. Malbon1*
The frizzled receptors, which mediate
development and display seven hydrophobic, membrane-spanning segments,
are cell membrane-localized. We constructed a chimeric receptor with
the ligand-binding and transmembrane segments from the
2-adrenergic receptor ( 2AR) and the
cytoplasmic domains from rat Frizzled-1 (Rfz1). Stimulation of mouse F9
clones expressing the chimera ( 2AR-Rfz1) with the -adrenergic agonist isoproterenol stimulated stabilization of -catenin, activation of a -catenin-sensitive promoter,
and formation of primitive endoderm. The response was blocked by
inactivation of pertussis toxin-sensitive, heterotrimeric guanine
nucleotide-binding proteins (G proteins) and by depletion of G q and
G o. Thus, G proteins are elements of Wnt/Frizzled-1 signaling to the
-catenin-lymphoid-enhancer factor (LEF)-T cell factor
(Tcf) pathway.
1 Department of Molecular Pharmacology and
2 Department of Physiology, Diabetes and Metabolic
Diseases Research Center, University Medical Center, State University
of New York at Stony Brook, Stony Brook, NY 11794-8651, USA.
3 Howard Hughes Medical Institute, Department of
Pharmacology and Center for Developmental Biology, University of
Washington School of Medicine, Seattle, WA 98195, USA.
*
To whom correspondence should be addressed. E-mail:
craig{at}pharm.som.sunysb.edu
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