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Randall T. Moon

Researcher at University of Washington

Publications -  305
Citations -  54792

Randall T. Moon is an academic researcher from University of Washington. The author has contributed to research in topics: Wnt signaling pathway & Signal transduction. The author has an hindex of 119, co-authored 305 publications receiving 51964 citations. Previous affiliations of Randall T. Moon include Marine Biological Laboratory & Howard Hughes Medical Institute.

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Ca2+/Calmodulin-dependent Protein Kinase II Is Stimulated by Wnt and Frizzled Homologs and Promotes Ventral Cell Fates in Xenopus

TL;DR: The hypothesis that Ca2+/calmodulin-dependent protein kinase II (CamKII) is activated by some Wnt and Frizzled homologs is tested, revealing that CamKII contributes to a ventral cell fate in the early embryo.
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Injected Wnt RNA induces a complete body axis in Xenopus embryos.

TL;DR: The results show that Wnt-1 and Xwnt-8 can induce a new and complete dorsal axis and can rescue the development of axis-deficient, UV-irradiated embryos.
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A frizzled homolog functions in a vertebrate Wnt signaling pathway

TL;DR: The results demonstrate that a vertebrate frizzled homolog is involved in Wnt signaling in a manner which discriminates between functionally distinct Wnts, which involves translocation of the dishevelled protein to the plasma membrane, and which works in a synergistic manner with WNTs to induce gene expression.
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Protein kinase C is differentially stimulated by Wnt and Frizzled homologs in aG-protein-dependent manner

TL;DR: It is demonstrated that some but not all Wnt and Frizzled signals modulate PKC localization and stimulate PKC activity via a G-protein-dependent mechanism, and these data support the existence of multiple Wnt/Frizzled signaling pathways in vertebrates.
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Control of neural crest cell fate by the Wnt signalling pathway

TL;DR: The role of Wnt signals in modulating the fate of neural crest by injecting messenger RNAs into single, premigratory neural crest cells of zebrafish is determined and endogenous Wnt signalling normally promotes pigment-cell formation by medial crest cells and thereby contributes to the diversity of Neural crest cell fates.