Literature DB >> 28334865

Structure of human POFUT1, its requirement in ligand-independent oncogenic Notch signaling, and functional effects of Dowling-Degos mutations.

Brian J McMillan1, Brandon Zimmerman1, Emily D Egan1, Michael Lofgren1, Xiang Xu1, Anthony Hesser1, Stephen C Blacklow1,2.   

Abstract

Protein O-fucosyltransferase-1 (POFUT1), which transfers fucose residues to acceptor sites on serine and threonine residues of epidermal growth factor-like repeats of recipient proteins, is essential for Notch signal transduction in mammals. Here, we examine the consequences of POFUT1 loss on the oncogenic signaling associated with certain leukemia-associated mutations of human Notch1, report the structures of human POFUT1 in free and GDP-fucose bound states, and assess the effects of Dowling-Degos mutations on human POFUT1 function. CRISPR-mediated knockout of POFUT1 in U2OS cells suppresses both normal Notch1 signaling, and the ligand-independent signaling associated with leukemogenic mutations of Notch1. Normal and oncogenic signaling are rescued by wild-type POFUT1 but rescue is impaired by an active-site R240A mutation. The overall structure of the human enzyme closely resembles that of the Caenorhabditis elegans protein, with an overall backbone RMSD of 0.93 Å, despite primary sequence identity of only 39% in the mature protein. GDP-fucose binding to the human enzyme induces limited backbone conformational movement, though the side chains of R43 and D244 reorient to make direct contact with the fucose moiety in the complex. The reported Dowling-Degos mutations of POFUT1, except for M262T, fail to rescue Notch1 signaling efficiently in the CRISPR-engineered POFUT1-/- background. Together, these studies identify POFUT1 as a potential target for cancers driven by Notch1 mutations and provide a structural roadmap for its inhibition.

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Year:  2017        PMID: 28334865      PMCID: PMC5881682          DOI: 10.1093/glycob/cwx020

Source DB:  PubMed          Journal:  Glycobiology        ISSN: 0959-6658            Impact factor:   4.313


  38 in total

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2.  Structural basis for autoinhibition of Notch.

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Review 5.  Fringe benefits: functional and structural impacts of O-glycosylation on the extracellular domain of Notch receptors.

Authors:  Nadia A Rana; Robert S Haltiwanger
Journal:  Curr Opin Struct Biol       Date:  2011-09-15       Impact factor: 6.809

Review 6.  Significance of glycosylation in Notch signaling.

Authors:  Hideyuki Takeuchi; Robert S Haltiwanger
Journal:  Biochem Biophys Res Commun       Date:  2014-06-06       Impact factor: 3.575

7.  Fringe-mediated extension of O-linked fucose in the ligand-binding region of Notch1 increases binding to mammalian Notch ligands.

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10.  Effects of S1 cleavage on the structure, surface export, and signaling activity of human Notch1 and Notch2.

Authors:  Wendy R Gordon; Didem Vardar-Ulu; Sarah L'Heureux; Todd Ashworth; Michael J Malecki; Cheryll Sanchez-Irizarry; Debbie G McArthur; Gavin Histen; Jennifer L Mitchell; Jon C Aster; Stephen C Blacklow
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Authors:  Bernadette C Holdener; Robert S Haltiwanger
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6.  Variant in human POFUT1 reduces enzymatic activity and likely causes a recessive microcephaly, global developmental delay with cardiac and vascular features.

Authors:  Hideyuki Takeuchi; Derek Wong; Michael Schneider; Hudson H Freeze; Megumi Takeuchi; Steven J Berardinelli; Atsuko Ito; Hane Lee; Stanley F Nelson; Robert S Haltiwanger
Journal:  Glycobiology       Date:  2018-05-01       Impact factor: 4.313

Review 7.  Multiple roles for O-glycans in Notch signalling.

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10.  POFUT1 promotes colorectal cancer development through the activation of Notch1 signaling.

Authors:  Yuheng Du; Daojiang Li; Nanpeng Li; Chen Su; Chunxing Yang; Changwei Lin; Miao Chen; Runliu Wu; Xiaorong Li; Gui Hu
Journal:  Cell Death Dis       Date:  2018-09-24       Impact factor: 8.469

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