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XB-ART-8580
J Biol Chem 2001 Oct 12;27641:37769-78. doi: 10.1074/jbc.M104774200.
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Fucosylation of Cripto is required for its ability to facilitate nodal signaling.

Schiffer SG , Foley S , Kaffashan A , Hronowski X , Zichittella AE , Yeo CY , Miatkowski K , Adkins HB , Damon B , Whitman M , Salomon D , Sanicola M , Williams KP .


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O-linked fucose modification is rare and has been shown to occur almost exclusively within epidermal growth factor (EGF)-like modules. We have found that the EGF-CFC family member human Cripto-1 (CR) is modified with fucose and through a combination of peptide mapping, mass spectrometry, and sequence analysis localized the site of attachment to Thr-88. The identification of a fucose modification on human CR within its EGF-like domain and the presence of a consensus fucosylation site within all EGF-CFC family members suggest that this is a biologically important modification in CR, which functionally distinguishes it from the EGF ligands that bind the type 1 erbB growth factor receptors. A single CR point mutation, Thr-88 --> Ala, results in a form of the protein that is not fucosylated and has substantially weaker activity in cell-based CR/Nodal signaling assays, indicating that fucosylation is functionally important for CR to facilitate Nodal signaling.

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Species referenced: Xenopus
Genes referenced: cripto.3 egf egfr nodal nodal1 ptpn11