Literature DB >> 29593094

Distinct human α(1,3)-fucosyltransferases drive Lewis-X/sialyl Lewis-X assembly in human cells.

Nandini Mondal1, Brad Dykstra1, Jungmin Lee2, David J Ashline3, Vernon N Reinhold3, Derrick J Rossi2, Robert Sackstein4.   

Abstract

In humans, six α(1,3)-fucosyltransferases (α(1,3)-FTs: FT3/FT4/FT5/FT6/FT7/FT9) reportedly fucosylate terminal lactosaminyl glycans yielding Lewis-X (LeX; CD15) and/or sialyl Lewis-X (sLeX; CD15s), structures that play key functions in cell migration, development, and immunity. Prior studies analyzing α(1,3)-FT specificities utilized either purified and/or recombinant enzymes to modify synthetic substrates under nonphysiological reaction conditions or molecular biology approaches wherein α(1,3)-FTs were expressed in mammalian cell lines, notably excluding investigations using primary human cells. Accordingly, although significant insights into α(1,3)-FT catalytic properties have been obtained, uncertainty persists regarding their human LeX/sLeX biosynthetic range across various glycoconjugates. Here, we undertook a comprehensive evaluation of the lactosaminyl product specificities of intracellularly expressed α(1,3)-FTs using a clinically relevant primary human cell type, mesenchymal stem cells. Cells were transfected with modified mRNA encoding each human α(1,3)-FT, and the resultant α(1,3)-fucosylated lactosaminyl glycoconjugates were analyzed using a combination of flow cytometry and MS. The data show that biosynthesis of sLeX is driven by FTs-3, -5, -6, and -7, with FT6 and FT7 having highest potency. FT4 and FT9 dominantly biosynthesize LeX, and, among all FTs, FT6 holds a unique capacity in creating sLeX and LeX determinants across protein and lipid glycoconjugates. Surprisingly, FT4 does not generate sLeX on glycolipids, and neither FT4, FT6, nor FT9 synthesizes the internally fucosylated sialyllactosamine VIM-2 (CD65s). These results unveil the relevant human lactosaminyl glycans created by human α(1,3)-FTs, providing novel insights on how these isoenzymes stereoselectively shape biosynthesis of vital glycoconjugates, thereby biochemically programming human cell migration and tuning human immunologic and developmental processes.
© 2018 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  E-selectin ligand; Lewis-X; fucosyltransferase; glycobiology; glycoengineering; mRNA; mass spectrometry (MS); mesenchymal stem cells (MSCs); modified mRNA; sialyl Lewis-X

Mesh:

Substances:

Year:  2018        PMID: 29593094      PMCID: PMC5950021          DOI: 10.1074/jbc.RA117.000775

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  72 in total

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5.  Distinct substrate specificities of five human alpha-1,3-fucosyltransferases for in vivo synthesis of the sialyl Lewis x and Lewis x epitopes.

Authors:  H Kimura; N Shinya; S Nishihara; M Kaneko; T Irimura; H Narimatsu
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9.  Glycoengineering of E-Selectin Ligands by Intracellular versus Extracellular Fucosylation Differentially Affects Osteotropism of Human Mesenchymal Stem Cells.

Authors:  Brad Dykstra; Jungmin Lee; Luke J Mortensen; Haixiao Yu; Zhengliang L Wu; Charles P Lin; Derrick J Rossi; Robert Sackstein
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10.  LEC12 and LEC29 gain-of-function Chinese hamster ovary mutants reveal mechanisms for regulating VIM-2 antigen synthesis and E-selectin binding.

Authors:  Santosh K Patnaik; Barry Potvin; Pamela Stanley
Journal:  J Biol Chem       Date:  2004-09-13       Impact factor: 5.157

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Review 6.  Mammalian sugar-binding receptors: known functions and unexplored roles.

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10.  Major differences in glycosylation and fucosyltransferase expression in low-grade versus high-grade bladder cancer cell lines.

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